Affiliations
Center for Research in the Implementation of Innovative Strategies in Practice (CRIISP) at the Iowa City Veterans Affairs (VA) Healthcare System, Iowa City, Iowa
Division of General Internal Medicine, Department of Internal Medicine, University of Iowa Carver College of Medicine, Iowa City, Iowa
Given name(s)
Connie
Family name
Chen
Degrees
PharmD

UGIB vs. LGIB

Article Type
Article
Changed
Sun, 05/28/2017 - 20:29
Display Headline
Upper versus lower gastrointestinal bleeding: A direct comparison of clinical presentation, outcomes, and resource utilization
Author(s)
Chad T. Whelan, MD
Connie Chen, PharmD
Peter Kaboli, MD, MS
Juned Siddique, DrPH
Micah Prochaska, BA
David O. Meltzer, MD, PhD

Gastrointestinal bleeding (GIB) is a frequent reason for acute hospitalization, with estimated rates of hospitalization at 375 per 100,000 per year in the United States.1 GIB is not a specific disease but rather a diverse set of conditions that lead to the clinical manifestations associated with bleeding into the gastrointestinal tract. One of the most commonly used organizing frameworks in gastrointestinal bleeding is the differentiation between upper gastrointestinal bleeding (UGIB) and lower gastrointestinal bleeding (LGIB). There are important differences in the etiologies between the 2 sources. For example, acid‐related disease is a common etiology in UGIB but does not occur in LGIB. While some aspects of the acute management are shared between UGIB and LGIB, important differences exist in the management, including initial endoscopy and medication choice. There have been few direct comparisons of rates, resource use, and clinical outcomes between UGIB and LGIB.

Historically, rates of UGIB have been reported to exceed those of LGIB by 2‐fold to 8‐fold.25 Protocols, clinical practice guidelines, and policy decisions reflect this emphasis on UGIB.68 Among 9 guidelines hosted by National Guideline Clearinghouse addressing GIB, 6 were focused on UGIB, 2 on both UGIB and LGIB, and only 1 on LGIB.9 There are several reasons to believe that these relative incidence rates may not be accurate. First, recent advances in therapy and prevention of UGIB, such as the treatment of Helicobacter pylori infection; proton pump inhibitors (PPIs); and selective cyclooxygenase‐2 (COX‐2) inhibitors, may have affected the epidemiology of gastrointestinal bleeding.1016 Among these therapies, only COX‐2 inhibitors may also reduce the incidence of LGIB.14, 1618 Therefore, these advances may result in a disproportionate drop in UGIB relative to LGIB. In addition, known risk factors for both LGIB and UGIB, including advancing age and renal failure, are increasing in the general population.5, 19, 20 Finally, given the recent increased recommendations for aspirin therapy and systemic anticoagulation, exposure to aspirin and warfarin have increased, both risk factors for LGIB and UGIB.2124 Indeed, recent studies in the epidemiology of UGIB do suggest a changing pattern of etiologies of UGIB reflecting these advances.25 One study examining rates of both UGIB and LGIB demonstrate a decrease in hospitalizations overall for GIB driven by a reduction in UGIB while at the same time reporting an increase in the incidence of hospitalization for LGIB.1

In addition to a changing epidemiology, a second reason for a potential underestimation of LGIB incidence is one of methodology. There are well‐recognized limitations with using purely administrative data due to difficulties in accurately identifying patients with LGIB.26

Studies using large administrative databases may not accurately identify LGIB because of the poor sensitivity and specificity of International Classification of Diseases, Ninth revision, Clinical Modification (ICD‐9) codes for LGIB.5 While there are standard methods of identifying patients with UGIB using ICD‐9 codes,19 there is not an accepted standard for LGIB. Thus, estimates using only ICD‐9 codes may overidentify or underidentify patients with LGIB. Prior studies that have most accurately identified patients with LGIB used a 2‐step method to address this issue. The initial ICD‐9 identification included a high sensitivity/low specificity approach. These identified patient charts undergo chart review to confirm the presence of an LGIB.5 This method is labor intensive and cannot be done using administrative databases. No direct comparison of UGIB to LGIB among hospitalized patients using this 2‐step method has been done recently.

The current emphasis on UGIB as seen in the published guidelines could also be supported if patients with UGIB had greater resource utilization or worse clinical outcomes. Limited direct comparisons for these outcomes are available. However, 1 administrative database study reported similar mortality rates for UGIB (2.7%) and LGIB (2.9%) in 2006.1 No direct comparisons of other clinical outcomes or resource use outcomes are available. Therefore, the emphasis on UGIB in publications and guidelines is best supported by the incidence rates that are, as has already been discussed, problematic.

We conducted a retrospective cohort study to examine the incidences of UGIB and LGIB among patients admitted to an academic medical center over 2 years using methods designed to optimally identify patients with either UGIB or LGIB. Our study also examined differences in clinical outcomes and resource utilization between subjects with UGIB and LGIB to examine the relative severity of these 2 clinical entities. These results may be useful in determining the need to reconsider clinical approaches as well as protocols and guidelines among patients with gastrointestinal bleeding.

Patients and Methods

Patients

This retrospective cohort study evaluated all patients who were admitted with GIB to a large urban academic medical center from July 1, 2001 to June 30, 2003 and who consented to a larger study examining the effects of hospitalists on patient care. Subjects unable to provide consent due to death or lack of decisional capacity were consented via proxy. To identify patients with GIB, all patients were screened for a primary or secondary diagnosis of GIB using ICD 9 codes. These codes were selected for a very high sensitivity threshold to assure that all potential subjects with GIB were identified. All subjects identified using these codes underwent chart abstraction to determine if they met criteria for GIB. These inclusion criteria required documentation in any portion of the chart (including emergency department [ED] clinician documentation, admission note, nursing intake note, etc.) of signs or symptoms of GI hemorrhage upon admission, including: hematemesis, coffee ground emesis, gastrooccult‐positive emesis, melena, hematochezia, maroon stools, and hemoccult‐positive stools interpreted by the treating physician team as an acute GIB. Subjects identified using the ICD‐9 codes and confirmed to have an acute GIB by chart review were included in the study and underwent additional chart abstraction and administrative data analysis.

ICD‐9 codes for GIB included: esophageal varices with hemorrhage (456.0, 456.20), Mallory‐Weiss syndrome (530.7), gastric ulcer with hemorrhage (531.00531.61), duodenal ulcer with hemorrhage (532.00532.61), peptic ulcer, site unspecified, with hemorrhage (533.00533.61), gastrojejunal ulcer with hemorrhage (534.00534.61), gastritis with hemorrhage (535.61), angiodysplasia of stomach/duodenum with hemorrhage (537.83), hematemesis (578.0578.9), diverticular disease (562.00562.9), other disorders of the intestine (569.00569.9), congenital anomalies of the digestive system (751.00), proctocolitis (556.00), hemorrhoids (455.00455.6), nondysenteric colitis (006.2), noninfectious gastroenteritis and colitis (558.0558.9), salmonella gastroenteritis (003.3), malignant neoplasm of colon (153), familial adenomatous polyposis (211.3), and gastric varices (456.8).

Data

Trained research assistants performed chart abstraction with validation by the principal investigators (PIs) of the first 15 charts to ensure accuracy. Subsequently, research assistants consulted with PIs with any questions during abstracting with final decisions being made by PIs. Detailed chart abstraction collected admission medication lists as obtained by the admitting physician team, including the use of PPIs, histamine‐2 (H‐2) blockers, COX‐2 inhibitors, and medications known to increase the risk of GIB, such as nonselective NSAIDs (nsNSAIDs), aspirin, and other anticoagulants. Other clinical data including risk factors, comorbid illnesses, laboratory tests, and vital signs were also abstracted from subjects' charts.

The source (UGIB vs. LGIB) and etiology (peptic ulcer disease [PUD], varices, diverticula, etc.) of bleeding were assessed using endoscopic reports as the primary source. When no clear source was identified on endoscopy or no endoscopy was done, the abstracter would review all progress notes, discharge summaries, and other diagnostic test results such as angiography in order to identify the source of bleeding (UGIB vs. LGIB). Endoscopic reports that identified a patient as having a UGIB or LGIB but no confirmed etiology were classified as undetermined etiology unless review of the other clinical documentation provided a specific etiology.

Tachycardia was defined as pulse greater than 100 beats per minute. Orthostasis was defined by either a drop in systolic blood pressure of 20 mmHg or an increase in pulse of 10 beats per minute. Hospital administrative databases were utilized to obtain resource utilization (ie, length of stay [LOS], total cost of care, intensive care transfers), Charlson comorbidity index,27 30‐day readmission rate, and in‐hospital mortality. Hospital costs were determined using TSI cost accounting software (Transition Systems Incorporated [now Eclypsis Corporation], Boston, MA), a validated system to assess actual direct and indirect costs of care.

Statistical Analysis

Descriptive statistics (means and proportions) were calculated by location of GIB for all variables describing patient characteristics, clinical presentation, clinical outcomes, and resource utilization. Differences in age and Charlson comorbidity index by GIB location were evaluated using t tests. Differences in gender, race, and medication use were evaluated using chi‐squared tests of independence.

We fit generalized linear models to investigate differences by location of bleed for those variables measuring clinical outcomes (inpatient mortality, intensive care unit [ICU] transfer, emergency surgery, 30‐day readmission, change in hemoglobin) and those variables measuring resource outcomes (total cost, LOS, number of procedures, number of correct scopes, repeat scope indicator, incorrect scope indicator, number of red blood cell [RBC] transfusions). The repeat scope indicator was used to denote a repeat scope (either esophagogastroduodenoscopy [EGD] or colonoscopy) and the incorrect scope indicator was used to denote when the initial scope was negative and a follow‐up scope from the other direction was positive (negative EGD followed by positive colonoscopy or negative colonoscopy followed by positive EGD). For each variable we fit 2 regression models, the first model (unadjusted effect) only included location of bleed as a covariate. The second model (adjusted effect) included location of bleed, age, gender, race (black/not black) and Charlson comorbidity index as covariates. Binary outcomes were modeled using logistic regressions. For continuous variables, we determined the distribution and link of the outcome variable using residual diagnostics and by comparing the log likelihood and information criteria of competing models. All analyses were performed using STATA SE Version 9.0 (StataCorp, College Station, TX)

This study was approved by the University of Chicago Institutional Review Board.

Results

During the 2 years of observation, a total of 7741 subjects were admitted to the internal medicine service and enrolled in the hospitalist study. Of these, 1014 had a primary or secondary ICD‐9 code that may be consistent with UGIB or LGIB and underwent chart review to determine if they had an acute GIB. Out of 1014 subjects, 647 were determined not to have an acute GI hemorrhage and were excluded from the remaining analyses; 367 of the 1104 subjects identified by ICD‐9 codes were found to have a clinical presentation consistent with GIB and were included in this study. A total of 180 of these 367 had UGIB and 187 had LGIB. The mean age was 62.4 years, 56.7% were female, 82.6% were African American, 12.7% were Caucasian, and the mean Charlson index was 1.5. (Table 1) Among baseline characteristics, both gender and age were statistically associated with a difference in rates of upper vs. lower source bleeding, with LGIB patients more likely to be female (P = 0.01) and older (P < 0.001). Etiologies of UGIB include erosive disease, peptic ulcer disease, variceal bleeding, arteriovenous malformation, and malignancy. Etiologies of LGIB include: diverticulosis, colitis, arteriovenous malformation, cancer, ischemic colitis, polyp, hemorrhoidal bleed, ulcer, inflammatory bowel disease, other, and not determined (Table 2).

Baseline Characteristics Among All Subjects Admitted for GI Hemorrhage
 Upper and Lower GI Bleeding (n = 367)Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)P Value

  • Abbreviations: GI, gastrointestinal; SD, standard deviation.

Age (years), mean (SD)62.4 (18.0)58.6 (18.2)66.0 (17.1)<0.001
Female gender (%)56.750.063.10.01
Race (%)    
African American82.685.380.10.43
White12.710.714.5 
Other4.74.05.4 
Charlson comorbidity index, mean (SD)1.5 (1.5)1.6 (1.6)1.4 (1.5)0.44
GI Bleeding Etiologies
Lower GI Bleed (n = 187)Upper GI Bleed (n = 180)
EtiologyFrequencyPercent of Total (%)EtiologyFrequencyPercent of Total (%)

  • NOTE: n = 367. Totals add up to >100% for upper GI bleed as some patients had more than 1 source identified.

  • Abbreviations: AVM, arteriovenous malformation; GI, gastrointestinal; IBD, inflammatory bowel disease; NOS, not otherwise specified.

Diverticulosis7641Erosive disease8648
Not identified3820Peptic ulcer5128
Colitis, NOS147Not identified2614
AVM137Mallory Weiss179
Cancer116Varices84
Ischemic colitis95AVMs53
Polyp95Mass/cancer53
Hemorrhoid84   
Ulcer53   
Other31   
IBD1<1   

Baseline use of medications known to be associated with either increased or decreased risk of GIB was common. Approximately one‐third of subjects with both LGIB and UGIB used aspirin and 10% used warfarin. LGIB subjects were less likely to use an nsNSAID (P < 0.001), but more likely to use a proton pump inhibitor (PPI) (P = 0.06) (Table 3).

Baseline Medication Use Among All Subjects Admitted for Gastrointestinal Hemorrhage
 Upper and Lower GI Bleeding (%) (n = 367)Upper GI Bleeding (%) (n = 180)Lower GI Bleeding (%) (n = 187)P Value*

  • Abbreviations: COX‐2, cyclooxygenase 2; GI, gastrointestinal; nsNSAID, nonselective nonsteroidal antiinflammatory drug; PPI, proton pump inhibitor.

  • P value comparing upper GI bleeding to lower GI bleeding.

Aspirin34.931.837.40.28
nsNSAID12.920.86.4< 0.001
COX‐2 selective inhibitor8.26.59.60.29
Warfarin10.98.412.80.19
PPI24.319.528.30.06
nsNSAID + PPI1.81.32.10.56
COX‐2 + PPI2.91.34.30.11

Key initial clinical presentation findings included vital sign abnormalities and admission hemoglobin levels. While hypotension was not common (4.7%), resting tachycardia (37%) and orthostasis (16%) were seen frequently. Subjects with LGIB were significantly less likely than those with UGIB to present with orthostasis (8.8% vs. 21.0%, respectively; P = 0.006) and resting tachycardia (32.3% vs. 42.5%, respectively; P = 0.04). Subjects with LGIB had a higher admission hemoglobin than those with UGIB (10.7 vs. 9.7, respectively; P < 0.001) (Table 4).

Admission Clinical Findings Among All Subjects Admitted for Gastrointestinal Hemorrhage
Clinical FindingUpper and Lower GI Bleeding (n = 367)Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)P Value*

  • Abbreviations: GI, gastrointestinal; SD, standard deviation.

  • P value comparing upper GI bleeding to lower GI bleeding.

Hypotension (%)4.75.73.80.39
Resting tachycardia (%)37.342.532.30.04
Orthostatic hypotension (%)16.221.08.80.006
Admission hemoglobin (g/dL), mean (SD)10.2 (2.6)9.7 (2.7)10.7 (2.5)<0.001

We also examined several clinical outcomes. When comparing LGIB to UGIB patients for these clinical outcomes using bivariate and multivariate statistics, there was no difference for in‐hospital mortality (1.1% vs. 1.1%), transfer to ICU (16.0% vs. 13.9%), 30‐day readmission (5.9% vs.7.8%), number of red blood cell (RBC) transfusions (2.7 vs. 2.4), or need for GI surgery (1.1% vs. 0.0%). The mean drop in hemoglobin was greater among subjects with LGIB compared to UGIB (1.9 g/dL vs. 1.5 g/dL, respectively) by both bivariate (P = 0.01) and multivariate (P = 0.003) analyses (Table 5).

Comparison of In‐hospital Clinical Outcomes Among All Subjects Admitted for GI Hemorrhage Using Bivariate and Multivariate Analyses
 Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)Bivariate P ValueMultivariate P Value

  • NOTE: Multivariate analyses control for age, gender, race (black/not black), and Charlson index.

  • Abbreviations: GI, gastrointestinal; ICU, intensive care unit; OLS, ordinary least squares; RBC, red blood cell; SD, standard deviation.

  • Modeled using logistic regression.

  • Modeled using OLS regression.

In‐hospital mortality (%)*1.11.10.970.74
Transfer to ICU (%)*13.916.00.560.44
Drop in hemoglobin (g/dL), mean (SD)1.5 (1.5)1.9 (1.6)0.010.003
Packed RBC transfusions required (units), mean (SD)*2.4 (2.9)2.7 (3.7)0.360.33
Surgery for GI bleeding (%)0.0%1.1  
30‐day readmission rate (%)*7.85.90.490.45

Mean costs were $11,892 for LGIB and $14,301 for UGIB and median costs were $7,890 for LGIB and $9,548 for UGIB, but were not statistically different. LOS was also similar between subjects with LGIB (5.1 days) and UGIB (5.7 days). In bivariate and multivariate analyses, UGIB subjects had a similar mean number of endoscopic procedures (1.3) compared to LGIB subjects (1.2). Thirteen percent of subjects with UGIB required a second EGD while only 8% of subjects with LGIB required 2 colonoscopies. In addition, 29% of subjects with LGIB received an EGD while only 16% of subjects with an UGIB received a colonoscopy (P = 0.001) (Table 6).

Comparison of Resource Utilization Among All Subjects Admitted for GI Hemorrhage Using Bivariate and Multivariate Analyses
 Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)Bivariate P ValueMultivariate P Value

  • NOTE: Multivariate analyses control for age, gender, race (black/not black), and Charlson index.

  • Abbreviations: GI, gastrointestinal; GLM, generalized linear model; OLS, ordinary least squares; SD, standard deviation.

  • Modeled using a GLM with a gamma distribution and log link.

  • Modeled using OLS regression.

Cost ($), mean (SD)*14,301 (17,196)11,892 (13,100)0.130.21
Cost ($), median$9,548$7,890  
Length of stay (days), mean (SD)*5.7 (7.0)5.1 (5.3)0.370.72
Number of endoscopies/ patient, mean (SD)1.3 (0.5)1.2 (0.9)0.180.20

Conclusions

This study represents one of the largest direct comparisons of LGIB to UGIB not based on administrative databases. The most striking finding was the nearly equal rates of LGIB and UGIB. There are 2 likely explanations for this surprising result. First, there may be methodological reasons that we identified a greater proportion of true LGIBs; our study used a highly sensitive search strategy of ICD‐9 coding with confirmatory chart abstraction to ensure that as many LGIB and UGIB cases would be identified as possible while also excluding cases not meeting accepted criteria for GIB. The second possibility is that there is an actual change in epidemiology of GIB. Known risk factors for LGIB are increasing such as advancing age, increased use of chronic aspirin therapy, and renal disease. At the same time, significant advances in the treatment and prevention of UGIB have been made. Recent studies have demonstrated similar trends in admissions for upper and lower GI complications, suggesting that there may be a changing epidemiology due primarily to reductions in upper GI complications.1, 16

Either explanation would have implications for the care of patients with GIB. Clinical decision‐making based on prior literature would support that in ambiguous clinical situations and initial evaluation for an UGIB is appropriate. Most risk stratification literature and clinical guidelines focus on UGIB. If rates of LGIB and UGIB are similar, then existing clinical decision protocols may need to be reevaluated to incorporate the higher likelihood of LGIB. This reevaluation would be less important if the clinical outcomes or resource utilization of UGIB was significantly greater than that for LGIB, but we did not find this was the case. Similarly, if the ability to distinguish between LGIB and UGIB were robust on clinical signs and symptoms, then a reevaluation would be less important. However, we found fairly similar numbers of patients initially receiving evaluation for UGIB then being evaluated for LGIB as we found patients initially receiving evaluation for LGIB then being evaluated for UGIB. This suggests the potential benefit of clinical decision protocols that could better distinguish between UGIB and LGIB and account for the potentially higher incidence of LGIB than previously thought.

In addition to affecting the attention paid to LGIB for acute management, a changed understanding of incidence could also affect the attention paid to prevention of LGIB. Of the recent nonendoscopic advances in the treatment and prevention of GIB, only the use of COX‐2s (when used in place of traditional nsNSAIDs) reduces the risk of both LGIB and UGIB;14, 1618 H .pylori treatment and PPIs only prevent UGIB. Therefore, if the clinical and financial burdens of LGIB are similar to those seen in UGIB, more attention may need to be focused on preventing LGIB.

Baseline medication use was notable primarily for the similarities between UGIB and LGIB. Agents known to affect the rates of GIB were common in both groups. Over one‐third of the population was using aspirin and 10% were taking warfarin. Over 20% of subjects were taking an nsNSAID or a COX‐2 inhibitor. Almost one‐quarter of subjects were taking a PPI, agents known to decrease rates of UGIB and potentially increase LGIB through the risk of C. difficile colitis. Notably, the only statistically significant difference in baseline medication use between subjects with UGIB and LGIB was the more than 3‐fold higher use of nsNSAIDs in patients with UGIB as compared to LGIB. While current guidelines are not clear and consistent about which populations of at‐risk patients should receive GI prophylaxis,2830 these results suggest that patients admitted with GIB are very likely to be taking medications which impact the risk of GIB.

In terms of disease severity, the clinical presentation at admission suggests a greater degree of hemodynamic instability among subjects with UGIB. Rates of orthostatic hypotension and resting tachycardia are higher in UGIB subjects, as well as having a lower mean hemoglobin levels at presentation. However, despite the more severe clinical presentation, clinical outcomes did not differ significantly between the 2 bleeding sources. Thus, the most relevant clinical outcomes suggest that the severity of both LGIB and UGIB are similar. This similarity again suggest that the clinical burden of LGIB is not significantly different than UGIB.

Our results concerning resource utilization demonstrate a similar pattern. While the point estimates for costs and LOS suggest that UGIB may be associated with higher resource utilization, these differences were not significant in either bivariate or multivariate analyses. Those subjects with UGIB did receive more total endoscopic procedures than subjects with LGIB. More interesting though was that 24% of all subjects received an endoscopy of the opposite site (LGIB with EGD and UGIB with colonoscopy). These results suggest that the site of bleeding is not clear in a significant proportion of patients who present with GIB. These additional endoscopies are associated with increased risk, costs, LOS, and discomfort to patients. Improving our ability to accurately predict the source (upper vs. lower) of bleeding would allow us to reduce the number of these excess endoscopies. Additionally, it is interesting that despite the almost universal use of endoscopies, 20% of LGIB and 14% of UGIB subjects could not have a specific etiology identified during endoscopy or subsequent workup.

There are some important limitations to this study. While the sample size is among the largest of its type involving chart abstraction, it may be underpowered to detect some differences. Additionally, our results are from a single urban academic medical center with a patient population that is predominantly African American, which may limit generalizability. This study required consent and therefore only examines a subset of patients admitted to the medical center with GIB, which could potentially introduce bias into the sample. However, it is not clear why there would be systematic differences in subjects who choose to consent vs. those who decide not to consent that would affect the results of this study in substantive ways.

Despite significant efforts at identifying all subjects with GIB admitted during this time period, there were potential methodological reasons that may have resulted in some cases being missed. Only subjects admitted to a medicine service were approached for consent. All subjects in this medical center with GIB are admitted to a medicine service. We captured all subjects who were initially admitted to a medicine service as well as those admitted initially to an ICU and then transferred to the floor at any point prior to discharge. It is possible, though, that a subject would be admitted to an ICU for GIB and die prior to being transferred to the floor. While it is the impression of the director of the ICU that this would be a very unusual event, as most of the patients would be discharged to the floor prior to death (personal communication), given the very low mortality rate seen in this study, small numbers of missed events could have a significant impact on the interpretation of in‐hospital mortality results. It is also important to note that this medical center did not have the ability to perform endoscopy prior to admission for patients with GIB at the time of the study; all patients who presented with GIB would have been admitted and identified for this study. Finally, we were unable to routinely identify the rationale for obtaining an endoscopic exam. We assumed that all endoscopic exams were done for the purpose of evaluating and/or treating the GIB for which the subject was admitted. It is possible that some subjects had additional endoscopies for other reasons, which would have led to our overestimating the rates of additional endoscopies for GIB.

This study highlights the similarities between LGIB and UGIB rather than the differences. There were few significant differences between the 2 bleeding sources in terms of incidence, clinical outcomes, and resource utilization. In fact, the study also suggests that determining the source of bleeding may not be clear, given the high rates of opposite site endoscopies. While this study did reveal several similarities between UGIB and LGIB, it also highlights the need to identify improved strategies to improve the sensitivity and specificity of identification of LGIB compared to UGIB, both for clinical purposes and for research. The value of such improved clinical algorithms have the potential to improve both the cost and outcomes of care, while better algorithms for separating UGIB and LGIB using administrative data might help produce more precise estimates of costs and clinical outcomes, and aid in the development of risk stratification models.

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Article PDF
606_ftp.pdf
Issue
Journal of Hospital Medicine - 5(3)
Publications
Journal of Hospital Medicine
Page Number
141-147
Legacy Keywords
cost effectiveness, endoscopy, epidemiology, gastrointestinal hemorrhage
Sections
Original Research
Author(s)
Chad T. Whelan, MD
Connie Chen, PharmD
Peter Kaboli, MD, MS
Juned Siddique, DrPH
Micah Prochaska, BA
David O. Meltzer, MD, PhD
Author(s)
Chad T. Whelan, MD
Connie Chen, PharmD
Peter Kaboli, MD, MS
Juned Siddique, DrPH
Micah Prochaska, BA
David O. Meltzer, MD, PhD
Article PDF
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Article PDF
606_ftp.pdf

Gastrointestinal bleeding (GIB) is a frequent reason for acute hospitalization, with estimated rates of hospitalization at 375 per 100,000 per year in the United States.1 GIB is not a specific disease but rather a diverse set of conditions that lead to the clinical manifestations associated with bleeding into the gastrointestinal tract. One of the most commonly used organizing frameworks in gastrointestinal bleeding is the differentiation between upper gastrointestinal bleeding (UGIB) and lower gastrointestinal bleeding (LGIB). There are important differences in the etiologies between the 2 sources. For example, acid‐related disease is a common etiology in UGIB but does not occur in LGIB. While some aspects of the acute management are shared between UGIB and LGIB, important differences exist in the management, including initial endoscopy and medication choice. There have been few direct comparisons of rates, resource use, and clinical outcomes between UGIB and LGIB.

Historically, rates of UGIB have been reported to exceed those of LGIB by 2‐fold to 8‐fold.25 Protocols, clinical practice guidelines, and policy decisions reflect this emphasis on UGIB.68 Among 9 guidelines hosted by National Guideline Clearinghouse addressing GIB, 6 were focused on UGIB, 2 on both UGIB and LGIB, and only 1 on LGIB.9 There are several reasons to believe that these relative incidence rates may not be accurate. First, recent advances in therapy and prevention of UGIB, such as the treatment of Helicobacter pylori infection; proton pump inhibitors (PPIs); and selective cyclooxygenase‐2 (COX‐2) inhibitors, may have affected the epidemiology of gastrointestinal bleeding.1016 Among these therapies, only COX‐2 inhibitors may also reduce the incidence of LGIB.14, 1618 Therefore, these advances may result in a disproportionate drop in UGIB relative to LGIB. In addition, known risk factors for both LGIB and UGIB, including advancing age and renal failure, are increasing in the general population.5, 19, 20 Finally, given the recent increased recommendations for aspirin therapy and systemic anticoagulation, exposure to aspirin and warfarin have increased, both risk factors for LGIB and UGIB.2124 Indeed, recent studies in the epidemiology of UGIB do suggest a changing pattern of etiologies of UGIB reflecting these advances.25 One study examining rates of both UGIB and LGIB demonstrate a decrease in hospitalizations overall for GIB driven by a reduction in UGIB while at the same time reporting an increase in the incidence of hospitalization for LGIB.1

In addition to a changing epidemiology, a second reason for a potential underestimation of LGIB incidence is one of methodology. There are well‐recognized limitations with using purely administrative data due to difficulties in accurately identifying patients with LGIB.26

Studies using large administrative databases may not accurately identify LGIB because of the poor sensitivity and specificity of International Classification of Diseases, Ninth revision, Clinical Modification (ICD‐9) codes for LGIB.5 While there are standard methods of identifying patients with UGIB using ICD‐9 codes,19 there is not an accepted standard for LGIB. Thus, estimates using only ICD‐9 codes may overidentify or underidentify patients with LGIB. Prior studies that have most accurately identified patients with LGIB used a 2‐step method to address this issue. The initial ICD‐9 identification included a high sensitivity/low specificity approach. These identified patient charts undergo chart review to confirm the presence of an LGIB.5 This method is labor intensive and cannot be done using administrative databases. No direct comparison of UGIB to LGIB among hospitalized patients using this 2‐step method has been done recently.

The current emphasis on UGIB as seen in the published guidelines could also be supported if patients with UGIB had greater resource utilization or worse clinical outcomes. Limited direct comparisons for these outcomes are available. However, 1 administrative database study reported similar mortality rates for UGIB (2.7%) and LGIB (2.9%) in 2006.1 No direct comparisons of other clinical outcomes or resource use outcomes are available. Therefore, the emphasis on UGIB in publications and guidelines is best supported by the incidence rates that are, as has already been discussed, problematic.

We conducted a retrospective cohort study to examine the incidences of UGIB and LGIB among patients admitted to an academic medical center over 2 years using methods designed to optimally identify patients with either UGIB or LGIB. Our study also examined differences in clinical outcomes and resource utilization between subjects with UGIB and LGIB to examine the relative severity of these 2 clinical entities. These results may be useful in determining the need to reconsider clinical approaches as well as protocols and guidelines among patients with gastrointestinal bleeding.

Patients and Methods

Patients

This retrospective cohort study evaluated all patients who were admitted with GIB to a large urban academic medical center from July 1, 2001 to June 30, 2003 and who consented to a larger study examining the effects of hospitalists on patient care. Subjects unable to provide consent due to death or lack of decisional capacity were consented via proxy. To identify patients with GIB, all patients were screened for a primary or secondary diagnosis of GIB using ICD 9 codes. These codes were selected for a very high sensitivity threshold to assure that all potential subjects with GIB were identified. All subjects identified using these codes underwent chart abstraction to determine if they met criteria for GIB. These inclusion criteria required documentation in any portion of the chart (including emergency department [ED] clinician documentation, admission note, nursing intake note, etc.) of signs or symptoms of GI hemorrhage upon admission, including: hematemesis, coffee ground emesis, gastrooccult‐positive emesis, melena, hematochezia, maroon stools, and hemoccult‐positive stools interpreted by the treating physician team as an acute GIB. Subjects identified using the ICD‐9 codes and confirmed to have an acute GIB by chart review were included in the study and underwent additional chart abstraction and administrative data analysis.

ICD‐9 codes for GIB included: esophageal varices with hemorrhage (456.0, 456.20), Mallory‐Weiss syndrome (530.7), gastric ulcer with hemorrhage (531.00531.61), duodenal ulcer with hemorrhage (532.00532.61), peptic ulcer, site unspecified, with hemorrhage (533.00533.61), gastrojejunal ulcer with hemorrhage (534.00534.61), gastritis with hemorrhage (535.61), angiodysplasia of stomach/duodenum with hemorrhage (537.83), hematemesis (578.0578.9), diverticular disease (562.00562.9), other disorders of the intestine (569.00569.9), congenital anomalies of the digestive system (751.00), proctocolitis (556.00), hemorrhoids (455.00455.6), nondysenteric colitis (006.2), noninfectious gastroenteritis and colitis (558.0558.9), salmonella gastroenteritis (003.3), malignant neoplasm of colon (153), familial adenomatous polyposis (211.3), and gastric varices (456.8).

Data

Trained research assistants performed chart abstraction with validation by the principal investigators (PIs) of the first 15 charts to ensure accuracy. Subsequently, research assistants consulted with PIs with any questions during abstracting with final decisions being made by PIs. Detailed chart abstraction collected admission medication lists as obtained by the admitting physician team, including the use of PPIs, histamine‐2 (H‐2) blockers, COX‐2 inhibitors, and medications known to increase the risk of GIB, such as nonselective NSAIDs (nsNSAIDs), aspirin, and other anticoagulants. Other clinical data including risk factors, comorbid illnesses, laboratory tests, and vital signs were also abstracted from subjects' charts.

The source (UGIB vs. LGIB) and etiology (peptic ulcer disease [PUD], varices, diverticula, etc.) of bleeding were assessed using endoscopic reports as the primary source. When no clear source was identified on endoscopy or no endoscopy was done, the abstracter would review all progress notes, discharge summaries, and other diagnostic test results such as angiography in order to identify the source of bleeding (UGIB vs. LGIB). Endoscopic reports that identified a patient as having a UGIB or LGIB but no confirmed etiology were classified as undetermined etiology unless review of the other clinical documentation provided a specific etiology.

Tachycardia was defined as pulse greater than 100 beats per minute. Orthostasis was defined by either a drop in systolic blood pressure of 20 mmHg or an increase in pulse of 10 beats per minute. Hospital administrative databases were utilized to obtain resource utilization (ie, length of stay [LOS], total cost of care, intensive care transfers), Charlson comorbidity index,27 30‐day readmission rate, and in‐hospital mortality. Hospital costs were determined using TSI cost accounting software (Transition Systems Incorporated [now Eclypsis Corporation], Boston, MA), a validated system to assess actual direct and indirect costs of care.

Statistical Analysis

Descriptive statistics (means and proportions) were calculated by location of GIB for all variables describing patient characteristics, clinical presentation, clinical outcomes, and resource utilization. Differences in age and Charlson comorbidity index by GIB location were evaluated using t tests. Differences in gender, race, and medication use were evaluated using chi‐squared tests of independence.

We fit generalized linear models to investigate differences by location of bleed for those variables measuring clinical outcomes (inpatient mortality, intensive care unit [ICU] transfer, emergency surgery, 30‐day readmission, change in hemoglobin) and those variables measuring resource outcomes (total cost, LOS, number of procedures, number of correct scopes, repeat scope indicator, incorrect scope indicator, number of red blood cell [RBC] transfusions). The repeat scope indicator was used to denote a repeat scope (either esophagogastroduodenoscopy [EGD] or colonoscopy) and the incorrect scope indicator was used to denote when the initial scope was negative and a follow‐up scope from the other direction was positive (negative EGD followed by positive colonoscopy or negative colonoscopy followed by positive EGD). For each variable we fit 2 regression models, the first model (unadjusted effect) only included location of bleed as a covariate. The second model (adjusted effect) included location of bleed, age, gender, race (black/not black) and Charlson comorbidity index as covariates. Binary outcomes were modeled using logistic regressions. For continuous variables, we determined the distribution and link of the outcome variable using residual diagnostics and by comparing the log likelihood and information criteria of competing models. All analyses were performed using STATA SE Version 9.0 (StataCorp, College Station, TX)

This study was approved by the University of Chicago Institutional Review Board.

Results

During the 2 years of observation, a total of 7741 subjects were admitted to the internal medicine service and enrolled in the hospitalist study. Of these, 1014 had a primary or secondary ICD‐9 code that may be consistent with UGIB or LGIB and underwent chart review to determine if they had an acute GIB. Out of 1014 subjects, 647 were determined not to have an acute GI hemorrhage and were excluded from the remaining analyses; 367 of the 1104 subjects identified by ICD‐9 codes were found to have a clinical presentation consistent with GIB and were included in this study. A total of 180 of these 367 had UGIB and 187 had LGIB. The mean age was 62.4 years, 56.7% were female, 82.6% were African American, 12.7% were Caucasian, and the mean Charlson index was 1.5. (Table 1) Among baseline characteristics, both gender and age were statistically associated with a difference in rates of upper vs. lower source bleeding, with LGIB patients more likely to be female (P = 0.01) and older (P < 0.001). Etiologies of UGIB include erosive disease, peptic ulcer disease, variceal bleeding, arteriovenous malformation, and malignancy. Etiologies of LGIB include: diverticulosis, colitis, arteriovenous malformation, cancer, ischemic colitis, polyp, hemorrhoidal bleed, ulcer, inflammatory bowel disease, other, and not determined (Table 2).

Baseline Characteristics Among All Subjects Admitted for GI Hemorrhage
 Upper and Lower GI Bleeding (n = 367)Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)P Value

  • Abbreviations: GI, gastrointestinal; SD, standard deviation.

Age (years), mean (SD)62.4 (18.0)58.6 (18.2)66.0 (17.1)<0.001
Female gender (%)56.750.063.10.01
Race (%)    
African American82.685.380.10.43
White12.710.714.5 
Other4.74.05.4 
Charlson comorbidity index, mean (SD)1.5 (1.5)1.6 (1.6)1.4 (1.5)0.44
GI Bleeding Etiologies
Lower GI Bleed (n = 187)Upper GI Bleed (n = 180)
EtiologyFrequencyPercent of Total (%)EtiologyFrequencyPercent of Total (%)

  • NOTE: n = 367. Totals add up to >100% for upper GI bleed as some patients had more than 1 source identified.

  • Abbreviations: AVM, arteriovenous malformation; GI, gastrointestinal; IBD, inflammatory bowel disease; NOS, not otherwise specified.

Diverticulosis7641Erosive disease8648
Not identified3820Peptic ulcer5128
Colitis, NOS147Not identified2614
AVM137Mallory Weiss179
Cancer116Varices84
Ischemic colitis95AVMs53
Polyp95Mass/cancer53
Hemorrhoid84   
Ulcer53   
Other31   
IBD1<1   

Baseline use of medications known to be associated with either increased or decreased risk of GIB was common. Approximately one‐third of subjects with both LGIB and UGIB used aspirin and 10% used warfarin. LGIB subjects were less likely to use an nsNSAID (P < 0.001), but more likely to use a proton pump inhibitor (PPI) (P = 0.06) (Table 3).

Baseline Medication Use Among All Subjects Admitted for Gastrointestinal Hemorrhage
 Upper and Lower GI Bleeding (%) (n = 367)Upper GI Bleeding (%) (n = 180)Lower GI Bleeding (%) (n = 187)P Value*

  • Abbreviations: COX‐2, cyclooxygenase 2; GI, gastrointestinal; nsNSAID, nonselective nonsteroidal antiinflammatory drug; PPI, proton pump inhibitor.

  • P value comparing upper GI bleeding to lower GI bleeding.

Aspirin34.931.837.40.28
nsNSAID12.920.86.4< 0.001
COX‐2 selective inhibitor8.26.59.60.29
Warfarin10.98.412.80.19
PPI24.319.528.30.06
nsNSAID + PPI1.81.32.10.56
COX‐2 + PPI2.91.34.30.11

Key initial clinical presentation findings included vital sign abnormalities and admission hemoglobin levels. While hypotension was not common (4.7%), resting tachycardia (37%) and orthostasis (16%) were seen frequently. Subjects with LGIB were significantly less likely than those with UGIB to present with orthostasis (8.8% vs. 21.0%, respectively; P = 0.006) and resting tachycardia (32.3% vs. 42.5%, respectively; P = 0.04). Subjects with LGIB had a higher admission hemoglobin than those with UGIB (10.7 vs. 9.7, respectively; P < 0.001) (Table 4).

Admission Clinical Findings Among All Subjects Admitted for Gastrointestinal Hemorrhage
Clinical FindingUpper and Lower GI Bleeding (n = 367)Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)P Value*

  • Abbreviations: GI, gastrointestinal; SD, standard deviation.

  • P value comparing upper GI bleeding to lower GI bleeding.

Hypotension (%)4.75.73.80.39
Resting tachycardia (%)37.342.532.30.04
Orthostatic hypotension (%)16.221.08.80.006
Admission hemoglobin (g/dL), mean (SD)10.2 (2.6)9.7 (2.7)10.7 (2.5)<0.001

We also examined several clinical outcomes. When comparing LGIB to UGIB patients for these clinical outcomes using bivariate and multivariate statistics, there was no difference for in‐hospital mortality (1.1% vs. 1.1%), transfer to ICU (16.0% vs. 13.9%), 30‐day readmission (5.9% vs.7.8%), number of red blood cell (RBC) transfusions (2.7 vs. 2.4), or need for GI surgery (1.1% vs. 0.0%). The mean drop in hemoglobin was greater among subjects with LGIB compared to UGIB (1.9 g/dL vs. 1.5 g/dL, respectively) by both bivariate (P = 0.01) and multivariate (P = 0.003) analyses (Table 5).

Comparison of In‐hospital Clinical Outcomes Among All Subjects Admitted for GI Hemorrhage Using Bivariate and Multivariate Analyses
 Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)Bivariate P ValueMultivariate P Value

  • NOTE: Multivariate analyses control for age, gender, race (black/not black), and Charlson index.

  • Abbreviations: GI, gastrointestinal; ICU, intensive care unit; OLS, ordinary least squares; RBC, red blood cell; SD, standard deviation.

  • Modeled using logistic regression.

  • Modeled using OLS regression.

In‐hospital mortality (%)*1.11.10.970.74
Transfer to ICU (%)*13.916.00.560.44
Drop in hemoglobin (g/dL), mean (SD)1.5 (1.5)1.9 (1.6)0.010.003
Packed RBC transfusions required (units), mean (SD)*2.4 (2.9)2.7 (3.7)0.360.33
Surgery for GI bleeding (%)0.0%1.1  
30‐day readmission rate (%)*7.85.90.490.45

Mean costs were $11,892 for LGIB and $14,301 for UGIB and median costs were $7,890 for LGIB and $9,548 for UGIB, but were not statistically different. LOS was also similar between subjects with LGIB (5.1 days) and UGIB (5.7 days). In bivariate and multivariate analyses, UGIB subjects had a similar mean number of endoscopic procedures (1.3) compared to LGIB subjects (1.2). Thirteen percent of subjects with UGIB required a second EGD while only 8% of subjects with LGIB required 2 colonoscopies. In addition, 29% of subjects with LGIB received an EGD while only 16% of subjects with an UGIB received a colonoscopy (P = 0.001) (Table 6).

Comparison of Resource Utilization Among All Subjects Admitted for GI Hemorrhage Using Bivariate and Multivariate Analyses
 Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)Bivariate P ValueMultivariate P Value

  • NOTE: Multivariate analyses control for age, gender, race (black/not black), and Charlson index.

  • Abbreviations: GI, gastrointestinal; GLM, generalized linear model; OLS, ordinary least squares; SD, standard deviation.

  • Modeled using a GLM with a gamma distribution and log link.

  • Modeled using OLS regression.

Cost ($), mean (SD)*14,301 (17,196)11,892 (13,100)0.130.21
Cost ($), median$9,548$7,890  
Length of stay (days), mean (SD)*5.7 (7.0)5.1 (5.3)0.370.72
Number of endoscopies/ patient, mean (SD)1.3 (0.5)1.2 (0.9)0.180.20

Conclusions

This study represents one of the largest direct comparisons of LGIB to UGIB not based on administrative databases. The most striking finding was the nearly equal rates of LGIB and UGIB. There are 2 likely explanations for this surprising result. First, there may be methodological reasons that we identified a greater proportion of true LGIBs; our study used a highly sensitive search strategy of ICD‐9 coding with confirmatory chart abstraction to ensure that as many LGIB and UGIB cases would be identified as possible while also excluding cases not meeting accepted criteria for GIB. The second possibility is that there is an actual change in epidemiology of GIB. Known risk factors for LGIB are increasing such as advancing age, increased use of chronic aspirin therapy, and renal disease. At the same time, significant advances in the treatment and prevention of UGIB have been made. Recent studies have demonstrated similar trends in admissions for upper and lower GI complications, suggesting that there may be a changing epidemiology due primarily to reductions in upper GI complications.1, 16

Either explanation would have implications for the care of patients with GIB. Clinical decision‐making based on prior literature would support that in ambiguous clinical situations and initial evaluation for an UGIB is appropriate. Most risk stratification literature and clinical guidelines focus on UGIB. If rates of LGIB and UGIB are similar, then existing clinical decision protocols may need to be reevaluated to incorporate the higher likelihood of LGIB. This reevaluation would be less important if the clinical outcomes or resource utilization of UGIB was significantly greater than that for LGIB, but we did not find this was the case. Similarly, if the ability to distinguish between LGIB and UGIB were robust on clinical signs and symptoms, then a reevaluation would be less important. However, we found fairly similar numbers of patients initially receiving evaluation for UGIB then being evaluated for LGIB as we found patients initially receiving evaluation for LGIB then being evaluated for UGIB. This suggests the potential benefit of clinical decision protocols that could better distinguish between UGIB and LGIB and account for the potentially higher incidence of LGIB than previously thought.

In addition to affecting the attention paid to LGIB for acute management, a changed understanding of incidence could also affect the attention paid to prevention of LGIB. Of the recent nonendoscopic advances in the treatment and prevention of GIB, only the use of COX‐2s (when used in place of traditional nsNSAIDs) reduces the risk of both LGIB and UGIB;14, 1618 H .pylori treatment and PPIs only prevent UGIB. Therefore, if the clinical and financial burdens of LGIB are similar to those seen in UGIB, more attention may need to be focused on preventing LGIB.

Baseline medication use was notable primarily for the similarities between UGIB and LGIB. Agents known to affect the rates of GIB were common in both groups. Over one‐third of the population was using aspirin and 10% were taking warfarin. Over 20% of subjects were taking an nsNSAID or a COX‐2 inhibitor. Almost one‐quarter of subjects were taking a PPI, agents known to decrease rates of UGIB and potentially increase LGIB through the risk of C. difficile colitis. Notably, the only statistically significant difference in baseline medication use between subjects with UGIB and LGIB was the more than 3‐fold higher use of nsNSAIDs in patients with UGIB as compared to LGIB. While current guidelines are not clear and consistent about which populations of at‐risk patients should receive GI prophylaxis,2830 these results suggest that patients admitted with GIB are very likely to be taking medications which impact the risk of GIB.

In terms of disease severity, the clinical presentation at admission suggests a greater degree of hemodynamic instability among subjects with UGIB. Rates of orthostatic hypotension and resting tachycardia are higher in UGIB subjects, as well as having a lower mean hemoglobin levels at presentation. However, despite the more severe clinical presentation, clinical outcomes did not differ significantly between the 2 bleeding sources. Thus, the most relevant clinical outcomes suggest that the severity of both LGIB and UGIB are similar. This similarity again suggest that the clinical burden of LGIB is not significantly different than UGIB.

Our results concerning resource utilization demonstrate a similar pattern. While the point estimates for costs and LOS suggest that UGIB may be associated with higher resource utilization, these differences were not significant in either bivariate or multivariate analyses. Those subjects with UGIB did receive more total endoscopic procedures than subjects with LGIB. More interesting though was that 24% of all subjects received an endoscopy of the opposite site (LGIB with EGD and UGIB with colonoscopy). These results suggest that the site of bleeding is not clear in a significant proportion of patients who present with GIB. These additional endoscopies are associated with increased risk, costs, LOS, and discomfort to patients. Improving our ability to accurately predict the source (upper vs. lower) of bleeding would allow us to reduce the number of these excess endoscopies. Additionally, it is interesting that despite the almost universal use of endoscopies, 20% of LGIB and 14% of UGIB subjects could not have a specific etiology identified during endoscopy or subsequent workup.

There are some important limitations to this study. While the sample size is among the largest of its type involving chart abstraction, it may be underpowered to detect some differences. Additionally, our results are from a single urban academic medical center with a patient population that is predominantly African American, which may limit generalizability. This study required consent and therefore only examines a subset of patients admitted to the medical center with GIB, which could potentially introduce bias into the sample. However, it is not clear why there would be systematic differences in subjects who choose to consent vs. those who decide not to consent that would affect the results of this study in substantive ways.

Despite significant efforts at identifying all subjects with GIB admitted during this time period, there were potential methodological reasons that may have resulted in some cases being missed. Only subjects admitted to a medicine service were approached for consent. All subjects in this medical center with GIB are admitted to a medicine service. We captured all subjects who were initially admitted to a medicine service as well as those admitted initially to an ICU and then transferred to the floor at any point prior to discharge. It is possible, though, that a subject would be admitted to an ICU for GIB and die prior to being transferred to the floor. While it is the impression of the director of the ICU that this would be a very unusual event, as most of the patients would be discharged to the floor prior to death (personal communication), given the very low mortality rate seen in this study, small numbers of missed events could have a significant impact on the interpretation of in‐hospital mortality results. It is also important to note that this medical center did not have the ability to perform endoscopy prior to admission for patients with GIB at the time of the study; all patients who presented with GIB would have been admitted and identified for this study. Finally, we were unable to routinely identify the rationale for obtaining an endoscopic exam. We assumed that all endoscopic exams were done for the purpose of evaluating and/or treating the GIB for which the subject was admitted. It is possible that some subjects had additional endoscopies for other reasons, which would have led to our overestimating the rates of additional endoscopies for GIB.

This study highlights the similarities between LGIB and UGIB rather than the differences. There were few significant differences between the 2 bleeding sources in terms of incidence, clinical outcomes, and resource utilization. In fact, the study also suggests that determining the source of bleeding may not be clear, given the high rates of opposite site endoscopies. While this study did reveal several similarities between UGIB and LGIB, it also highlights the need to identify improved strategies to improve the sensitivity and specificity of identification of LGIB compared to UGIB, both for clinical purposes and for research. The value of such improved clinical algorithms have the potential to improve both the cost and outcomes of care, while better algorithms for separating UGIB and LGIB using administrative data might help produce more precise estimates of costs and clinical outcomes, and aid in the development of risk stratification models.

Gastrointestinal bleeding (GIB) is a frequent reason for acute hospitalization, with estimated rates of hospitalization at 375 per 100,000 per year in the United States.1 GIB is not a specific disease but rather a diverse set of conditions that lead to the clinical manifestations associated with bleeding into the gastrointestinal tract. One of the most commonly used organizing frameworks in gastrointestinal bleeding is the differentiation between upper gastrointestinal bleeding (UGIB) and lower gastrointestinal bleeding (LGIB). There are important differences in the etiologies between the 2 sources. For example, acid‐related disease is a common etiology in UGIB but does not occur in LGIB. While some aspects of the acute management are shared between UGIB and LGIB, important differences exist in the management, including initial endoscopy and medication choice. There have been few direct comparisons of rates, resource use, and clinical outcomes between UGIB and LGIB.

Historically, rates of UGIB have been reported to exceed those of LGIB by 2‐fold to 8‐fold.25 Protocols, clinical practice guidelines, and policy decisions reflect this emphasis on UGIB.68 Among 9 guidelines hosted by National Guideline Clearinghouse addressing GIB, 6 were focused on UGIB, 2 on both UGIB and LGIB, and only 1 on LGIB.9 There are several reasons to believe that these relative incidence rates may not be accurate. First, recent advances in therapy and prevention of UGIB, such as the treatment of Helicobacter pylori infection; proton pump inhibitors (PPIs); and selective cyclooxygenase‐2 (COX‐2) inhibitors, may have affected the epidemiology of gastrointestinal bleeding.1016 Among these therapies, only COX‐2 inhibitors may also reduce the incidence of LGIB.14, 1618 Therefore, these advances may result in a disproportionate drop in UGIB relative to LGIB. In addition, known risk factors for both LGIB and UGIB, including advancing age and renal failure, are increasing in the general population.5, 19, 20 Finally, given the recent increased recommendations for aspirin therapy and systemic anticoagulation, exposure to aspirin and warfarin have increased, both risk factors for LGIB and UGIB.2124 Indeed, recent studies in the epidemiology of UGIB do suggest a changing pattern of etiologies of UGIB reflecting these advances.25 One study examining rates of both UGIB and LGIB demonstrate a decrease in hospitalizations overall for GIB driven by a reduction in UGIB while at the same time reporting an increase in the incidence of hospitalization for LGIB.1

In addition to a changing epidemiology, a second reason for a potential underestimation of LGIB incidence is one of methodology. There are well‐recognized limitations with using purely administrative data due to difficulties in accurately identifying patients with LGIB.26

Studies using large administrative databases may not accurately identify LGIB because of the poor sensitivity and specificity of International Classification of Diseases, Ninth revision, Clinical Modification (ICD‐9) codes for LGIB.5 While there are standard methods of identifying patients with UGIB using ICD‐9 codes,19 there is not an accepted standard for LGIB. Thus, estimates using only ICD‐9 codes may overidentify or underidentify patients with LGIB. Prior studies that have most accurately identified patients with LGIB used a 2‐step method to address this issue. The initial ICD‐9 identification included a high sensitivity/low specificity approach. These identified patient charts undergo chart review to confirm the presence of an LGIB.5 This method is labor intensive and cannot be done using administrative databases. No direct comparison of UGIB to LGIB among hospitalized patients using this 2‐step method has been done recently.

The current emphasis on UGIB as seen in the published guidelines could also be supported if patients with UGIB had greater resource utilization or worse clinical outcomes. Limited direct comparisons for these outcomes are available. However, 1 administrative database study reported similar mortality rates for UGIB (2.7%) and LGIB (2.9%) in 2006.1 No direct comparisons of other clinical outcomes or resource use outcomes are available. Therefore, the emphasis on UGIB in publications and guidelines is best supported by the incidence rates that are, as has already been discussed, problematic.

We conducted a retrospective cohort study to examine the incidences of UGIB and LGIB among patients admitted to an academic medical center over 2 years using methods designed to optimally identify patients with either UGIB or LGIB. Our study also examined differences in clinical outcomes and resource utilization between subjects with UGIB and LGIB to examine the relative severity of these 2 clinical entities. These results may be useful in determining the need to reconsider clinical approaches as well as protocols and guidelines among patients with gastrointestinal bleeding.

Patients and Methods

Patients

This retrospective cohort study evaluated all patients who were admitted with GIB to a large urban academic medical center from July 1, 2001 to June 30, 2003 and who consented to a larger study examining the effects of hospitalists on patient care. Subjects unable to provide consent due to death or lack of decisional capacity were consented via proxy. To identify patients with GIB, all patients were screened for a primary or secondary diagnosis of GIB using ICD 9 codes. These codes were selected for a very high sensitivity threshold to assure that all potential subjects with GIB were identified. All subjects identified using these codes underwent chart abstraction to determine if they met criteria for GIB. These inclusion criteria required documentation in any portion of the chart (including emergency department [ED] clinician documentation, admission note, nursing intake note, etc.) of signs or symptoms of GI hemorrhage upon admission, including: hematemesis, coffee ground emesis, gastrooccult‐positive emesis, melena, hematochezia, maroon stools, and hemoccult‐positive stools interpreted by the treating physician team as an acute GIB. Subjects identified using the ICD‐9 codes and confirmed to have an acute GIB by chart review were included in the study and underwent additional chart abstraction and administrative data analysis.

ICD‐9 codes for GIB included: esophageal varices with hemorrhage (456.0, 456.20), Mallory‐Weiss syndrome (530.7), gastric ulcer with hemorrhage (531.00531.61), duodenal ulcer with hemorrhage (532.00532.61), peptic ulcer, site unspecified, with hemorrhage (533.00533.61), gastrojejunal ulcer with hemorrhage (534.00534.61), gastritis with hemorrhage (535.61), angiodysplasia of stomach/duodenum with hemorrhage (537.83), hematemesis (578.0578.9), diverticular disease (562.00562.9), other disorders of the intestine (569.00569.9), congenital anomalies of the digestive system (751.00), proctocolitis (556.00), hemorrhoids (455.00455.6), nondysenteric colitis (006.2), noninfectious gastroenteritis and colitis (558.0558.9), salmonella gastroenteritis (003.3), malignant neoplasm of colon (153), familial adenomatous polyposis (211.3), and gastric varices (456.8).

Data

Trained research assistants performed chart abstraction with validation by the principal investigators (PIs) of the first 15 charts to ensure accuracy. Subsequently, research assistants consulted with PIs with any questions during abstracting with final decisions being made by PIs. Detailed chart abstraction collected admission medication lists as obtained by the admitting physician team, including the use of PPIs, histamine‐2 (H‐2) blockers, COX‐2 inhibitors, and medications known to increase the risk of GIB, such as nonselective NSAIDs (nsNSAIDs), aspirin, and other anticoagulants. Other clinical data including risk factors, comorbid illnesses, laboratory tests, and vital signs were also abstracted from subjects' charts.

The source (UGIB vs. LGIB) and etiology (peptic ulcer disease [PUD], varices, diverticula, etc.) of bleeding were assessed using endoscopic reports as the primary source. When no clear source was identified on endoscopy or no endoscopy was done, the abstracter would review all progress notes, discharge summaries, and other diagnostic test results such as angiography in order to identify the source of bleeding (UGIB vs. LGIB). Endoscopic reports that identified a patient as having a UGIB or LGIB but no confirmed etiology were classified as undetermined etiology unless review of the other clinical documentation provided a specific etiology.

Tachycardia was defined as pulse greater than 100 beats per minute. Orthostasis was defined by either a drop in systolic blood pressure of 20 mmHg or an increase in pulse of 10 beats per minute. Hospital administrative databases were utilized to obtain resource utilization (ie, length of stay [LOS], total cost of care, intensive care transfers), Charlson comorbidity index,27 30‐day readmission rate, and in‐hospital mortality. Hospital costs were determined using TSI cost accounting software (Transition Systems Incorporated [now Eclypsis Corporation], Boston, MA), a validated system to assess actual direct and indirect costs of care.

Statistical Analysis

Descriptive statistics (means and proportions) were calculated by location of GIB for all variables describing patient characteristics, clinical presentation, clinical outcomes, and resource utilization. Differences in age and Charlson comorbidity index by GIB location were evaluated using t tests. Differences in gender, race, and medication use were evaluated using chi‐squared tests of independence.

We fit generalized linear models to investigate differences by location of bleed for those variables measuring clinical outcomes (inpatient mortality, intensive care unit [ICU] transfer, emergency surgery, 30‐day readmission, change in hemoglobin) and those variables measuring resource outcomes (total cost, LOS, number of procedures, number of correct scopes, repeat scope indicator, incorrect scope indicator, number of red blood cell [RBC] transfusions). The repeat scope indicator was used to denote a repeat scope (either esophagogastroduodenoscopy [EGD] or colonoscopy) and the incorrect scope indicator was used to denote when the initial scope was negative and a follow‐up scope from the other direction was positive (negative EGD followed by positive colonoscopy or negative colonoscopy followed by positive EGD). For each variable we fit 2 regression models, the first model (unadjusted effect) only included location of bleed as a covariate. The second model (adjusted effect) included location of bleed, age, gender, race (black/not black) and Charlson comorbidity index as covariates. Binary outcomes were modeled using logistic regressions. For continuous variables, we determined the distribution and link of the outcome variable using residual diagnostics and by comparing the log likelihood and information criteria of competing models. All analyses were performed using STATA SE Version 9.0 (StataCorp, College Station, TX)

This study was approved by the University of Chicago Institutional Review Board.

Results

During the 2 years of observation, a total of 7741 subjects were admitted to the internal medicine service and enrolled in the hospitalist study. Of these, 1014 had a primary or secondary ICD‐9 code that may be consistent with UGIB or LGIB and underwent chart review to determine if they had an acute GIB. Out of 1014 subjects, 647 were determined not to have an acute GI hemorrhage and were excluded from the remaining analyses; 367 of the 1104 subjects identified by ICD‐9 codes were found to have a clinical presentation consistent with GIB and were included in this study. A total of 180 of these 367 had UGIB and 187 had LGIB. The mean age was 62.4 years, 56.7% were female, 82.6% were African American, 12.7% were Caucasian, and the mean Charlson index was 1.5. (Table 1) Among baseline characteristics, both gender and age were statistically associated with a difference in rates of upper vs. lower source bleeding, with LGIB patients more likely to be female (P = 0.01) and older (P < 0.001). Etiologies of UGIB include erosive disease, peptic ulcer disease, variceal bleeding, arteriovenous malformation, and malignancy. Etiologies of LGIB include: diverticulosis, colitis, arteriovenous malformation, cancer, ischemic colitis, polyp, hemorrhoidal bleed, ulcer, inflammatory bowel disease, other, and not determined (Table 2).

Baseline Characteristics Among All Subjects Admitted for GI Hemorrhage
 Upper and Lower GI Bleeding (n = 367)Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)P Value

  • Abbreviations: GI, gastrointestinal; SD, standard deviation.

Age (years), mean (SD)62.4 (18.0)58.6 (18.2)66.0 (17.1)<0.001
Female gender (%)56.750.063.10.01
Race (%)    
African American82.685.380.10.43
White12.710.714.5 
Other4.74.05.4 
Charlson comorbidity index, mean (SD)1.5 (1.5)1.6 (1.6)1.4 (1.5)0.44
GI Bleeding Etiologies
Lower GI Bleed (n = 187)Upper GI Bleed (n = 180)
EtiologyFrequencyPercent of Total (%)EtiologyFrequencyPercent of Total (%)

  • NOTE: n = 367. Totals add up to >100% for upper GI bleed as some patients had more than 1 source identified.

  • Abbreviations: AVM, arteriovenous malformation; GI, gastrointestinal; IBD, inflammatory bowel disease; NOS, not otherwise specified.

Diverticulosis7641Erosive disease8648
Not identified3820Peptic ulcer5128
Colitis, NOS147Not identified2614
AVM137Mallory Weiss179
Cancer116Varices84
Ischemic colitis95AVMs53
Polyp95Mass/cancer53
Hemorrhoid84   
Ulcer53   
Other31   
IBD1<1   

Baseline use of medications known to be associated with either increased or decreased risk of GIB was common. Approximately one‐third of subjects with both LGIB and UGIB used aspirin and 10% used warfarin. LGIB subjects were less likely to use an nsNSAID (P < 0.001), but more likely to use a proton pump inhibitor (PPI) (P = 0.06) (Table 3).

Baseline Medication Use Among All Subjects Admitted for Gastrointestinal Hemorrhage
 Upper and Lower GI Bleeding (%) (n = 367)Upper GI Bleeding (%) (n = 180)Lower GI Bleeding (%) (n = 187)P Value*

  • Abbreviations: COX‐2, cyclooxygenase 2; GI, gastrointestinal; nsNSAID, nonselective nonsteroidal antiinflammatory drug; PPI, proton pump inhibitor.

  • P value comparing upper GI bleeding to lower GI bleeding.

Aspirin34.931.837.40.28
nsNSAID12.920.86.4< 0.001
COX‐2 selective inhibitor8.26.59.60.29
Warfarin10.98.412.80.19
PPI24.319.528.30.06
nsNSAID + PPI1.81.32.10.56
COX‐2 + PPI2.91.34.30.11

Key initial clinical presentation findings included vital sign abnormalities and admission hemoglobin levels. While hypotension was not common (4.7%), resting tachycardia (37%) and orthostasis (16%) were seen frequently. Subjects with LGIB were significantly less likely than those with UGIB to present with orthostasis (8.8% vs. 21.0%, respectively; P = 0.006) and resting tachycardia (32.3% vs. 42.5%, respectively; P = 0.04). Subjects with LGIB had a higher admission hemoglobin than those with UGIB (10.7 vs. 9.7, respectively; P < 0.001) (Table 4).

Admission Clinical Findings Among All Subjects Admitted for Gastrointestinal Hemorrhage
Clinical FindingUpper and Lower GI Bleeding (n = 367)Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)P Value*

  • Abbreviations: GI, gastrointestinal; SD, standard deviation.

  • P value comparing upper GI bleeding to lower GI bleeding.

Hypotension (%)4.75.73.80.39
Resting tachycardia (%)37.342.532.30.04
Orthostatic hypotension (%)16.221.08.80.006
Admission hemoglobin (g/dL), mean (SD)10.2 (2.6)9.7 (2.7)10.7 (2.5)<0.001

We also examined several clinical outcomes. When comparing LGIB to UGIB patients for these clinical outcomes using bivariate and multivariate statistics, there was no difference for in‐hospital mortality (1.1% vs. 1.1%), transfer to ICU (16.0% vs. 13.9%), 30‐day readmission (5.9% vs.7.8%), number of red blood cell (RBC) transfusions (2.7 vs. 2.4), or need for GI surgery (1.1% vs. 0.0%). The mean drop in hemoglobin was greater among subjects with LGIB compared to UGIB (1.9 g/dL vs. 1.5 g/dL, respectively) by both bivariate (P = 0.01) and multivariate (P = 0.003) analyses (Table 5).

Comparison of In‐hospital Clinical Outcomes Among All Subjects Admitted for GI Hemorrhage Using Bivariate and Multivariate Analyses
 Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)Bivariate P ValueMultivariate P Value

  • NOTE: Multivariate analyses control for age, gender, race (black/not black), and Charlson index.

  • Abbreviations: GI, gastrointestinal; ICU, intensive care unit; OLS, ordinary least squares; RBC, red blood cell; SD, standard deviation.

  • Modeled using logistic regression.

  • Modeled using OLS regression.

In‐hospital mortality (%)*1.11.10.970.74
Transfer to ICU (%)*13.916.00.560.44
Drop in hemoglobin (g/dL), mean (SD)1.5 (1.5)1.9 (1.6)0.010.003
Packed RBC transfusions required (units), mean (SD)*2.4 (2.9)2.7 (3.7)0.360.33
Surgery for GI bleeding (%)0.0%1.1  
30‐day readmission rate (%)*7.85.90.490.45

Mean costs were $11,892 for LGIB and $14,301 for UGIB and median costs were $7,890 for LGIB and $9,548 for UGIB, but were not statistically different. LOS was also similar between subjects with LGIB (5.1 days) and UGIB (5.7 days). In bivariate and multivariate analyses, UGIB subjects had a similar mean number of endoscopic procedures (1.3) compared to LGIB subjects (1.2). Thirteen percent of subjects with UGIB required a second EGD while only 8% of subjects with LGIB required 2 colonoscopies. In addition, 29% of subjects with LGIB received an EGD while only 16% of subjects with an UGIB received a colonoscopy (P = 0.001) (Table 6).

Comparison of Resource Utilization Among All Subjects Admitted for GI Hemorrhage Using Bivariate and Multivariate Analyses
 Upper GI Bleeding (n = 180)Lower GI Bleeding (n = 187)Bivariate P ValueMultivariate P Value

  • NOTE: Multivariate analyses control for age, gender, race (black/not black), and Charlson index.

  • Abbreviations: GI, gastrointestinal; GLM, generalized linear model; OLS, ordinary least squares; SD, standard deviation.

  • Modeled using a GLM with a gamma distribution and log link.

  • Modeled using OLS regression.

Cost ($), mean (SD)*14,301 (17,196)11,892 (13,100)0.130.21
Cost ($), median$9,548$7,890  
Length of stay (days), mean (SD)*5.7 (7.0)5.1 (5.3)0.370.72
Number of endoscopies/ patient, mean (SD)1.3 (0.5)1.2 (0.9)0.180.20

Conclusions

This study represents one of the largest direct comparisons of LGIB to UGIB not based on administrative databases. The most striking finding was the nearly equal rates of LGIB and UGIB. There are 2 likely explanations for this surprising result. First, there may be methodological reasons that we identified a greater proportion of true LGIBs; our study used a highly sensitive search strategy of ICD‐9 coding with confirmatory chart abstraction to ensure that as many LGIB and UGIB cases would be identified as possible while also excluding cases not meeting accepted criteria for GIB. The second possibility is that there is an actual change in epidemiology of GIB. Known risk factors for LGIB are increasing such as advancing age, increased use of chronic aspirin therapy, and renal disease. At the same time, significant advances in the treatment and prevention of UGIB have been made. Recent studies have demonstrated similar trends in admissions for upper and lower GI complications, suggesting that there may be a changing epidemiology due primarily to reductions in upper GI complications.1, 16

Either explanation would have implications for the care of patients with GIB. Clinical decision‐making based on prior literature would support that in ambiguous clinical situations and initial evaluation for an UGIB is appropriate. Most risk stratification literature and clinical guidelines focus on UGIB. If rates of LGIB and UGIB are similar, then existing clinical decision protocols may need to be reevaluated to incorporate the higher likelihood of LGIB. This reevaluation would be less important if the clinical outcomes or resource utilization of UGIB was significantly greater than that for LGIB, but we did not find this was the case. Similarly, if the ability to distinguish between LGIB and UGIB were robust on clinical signs and symptoms, then a reevaluation would be less important. However, we found fairly similar numbers of patients initially receiving evaluation for UGIB then being evaluated for LGIB as we found patients initially receiving evaluation for LGIB then being evaluated for UGIB. This suggests the potential benefit of clinical decision protocols that could better distinguish between UGIB and LGIB and account for the potentially higher incidence of LGIB than previously thought.

In addition to affecting the attention paid to LGIB for acute management, a changed understanding of incidence could also affect the attention paid to prevention of LGIB. Of the recent nonendoscopic advances in the treatment and prevention of GIB, only the use of COX‐2s (when used in place of traditional nsNSAIDs) reduces the risk of both LGIB and UGIB;14, 1618 H .pylori treatment and PPIs only prevent UGIB. Therefore, if the clinical and financial burdens of LGIB are similar to those seen in UGIB, more attention may need to be focused on preventing LGIB.

Baseline medication use was notable primarily for the similarities between UGIB and LGIB. Agents known to affect the rates of GIB were common in both groups. Over one‐third of the population was using aspirin and 10% were taking warfarin. Over 20% of subjects were taking an nsNSAID or a COX‐2 inhibitor. Almost one‐quarter of subjects were taking a PPI, agents known to decrease rates of UGIB and potentially increase LGIB through the risk of C. difficile colitis. Notably, the only statistically significant difference in baseline medication use between subjects with UGIB and LGIB was the more than 3‐fold higher use of nsNSAIDs in patients with UGIB as compared to LGIB. While current guidelines are not clear and consistent about which populations of at‐risk patients should receive GI prophylaxis,2830 these results suggest that patients admitted with GIB are very likely to be taking medications which impact the risk of GIB.

In terms of disease severity, the clinical presentation at admission suggests a greater degree of hemodynamic instability among subjects with UGIB. Rates of orthostatic hypotension and resting tachycardia are higher in UGIB subjects, as well as having a lower mean hemoglobin levels at presentation. However, despite the more severe clinical presentation, clinical outcomes did not differ significantly between the 2 bleeding sources. Thus, the most relevant clinical outcomes suggest that the severity of both LGIB and UGIB are similar. This similarity again suggest that the clinical burden of LGIB is not significantly different than UGIB.

Our results concerning resource utilization demonstrate a similar pattern. While the point estimates for costs and LOS suggest that UGIB may be associated with higher resource utilization, these differences were not significant in either bivariate or multivariate analyses. Those subjects with UGIB did receive more total endoscopic procedures than subjects with LGIB. More interesting though was that 24% of all subjects received an endoscopy of the opposite site (LGIB with EGD and UGIB with colonoscopy). These results suggest that the site of bleeding is not clear in a significant proportion of patients who present with GIB. These additional endoscopies are associated with increased risk, costs, LOS, and discomfort to patients. Improving our ability to accurately predict the source (upper vs. lower) of bleeding would allow us to reduce the number of these excess endoscopies. Additionally, it is interesting that despite the almost universal use of endoscopies, 20% of LGIB and 14% of UGIB subjects could not have a specific etiology identified during endoscopy or subsequent workup.

There are some important limitations to this study. While the sample size is among the largest of its type involving chart abstraction, it may be underpowered to detect some differences. Additionally, our results are from a single urban academic medical center with a patient population that is predominantly African American, which may limit generalizability. This study required consent and therefore only examines a subset of patients admitted to the medical center with GIB, which could potentially introduce bias into the sample. However, it is not clear why there would be systematic differences in subjects who choose to consent vs. those who decide not to consent that would affect the results of this study in substantive ways.

Despite significant efforts at identifying all subjects with GIB admitted during this time period, there were potential methodological reasons that may have resulted in some cases being missed. Only subjects admitted to a medicine service were approached for consent. All subjects in this medical center with GIB are admitted to a medicine service. We captured all subjects who were initially admitted to a medicine service as well as those admitted initially to an ICU and then transferred to the floor at any point prior to discharge. It is possible, though, that a subject would be admitted to an ICU for GIB and die prior to being transferred to the floor. While it is the impression of the director of the ICU that this would be a very unusual event, as most of the patients would be discharged to the floor prior to death (personal communication), given the very low mortality rate seen in this study, small numbers of missed events could have a significant impact on the interpretation of in‐hospital mortality results. It is also important to note that this medical center did not have the ability to perform endoscopy prior to admission for patients with GIB at the time of the study; all patients who presented with GIB would have been admitted and identified for this study. Finally, we were unable to routinely identify the rationale for obtaining an endoscopic exam. We assumed that all endoscopic exams were done for the purpose of evaluating and/or treating the GIB for which the subject was admitted. It is possible that some subjects had additional endoscopies for other reasons, which would have led to our overestimating the rates of additional endoscopies for GIB.

This study highlights the similarities between LGIB and UGIB rather than the differences. There were few significant differences between the 2 bleeding sources in terms of incidence, clinical outcomes, and resource utilization. In fact, the study also suggests that determining the source of bleeding may not be clear, given the high rates of opposite site endoscopies. While this study did reveal several similarities between UGIB and LGIB, it also highlights the need to identify improved strategies to improve the sensitivity and specificity of identification of LGIB compared to UGIB, both for clinical purposes and for research. The value of such improved clinical algorithms have the potential to improve both the cost and outcomes of care, while better algorithms for separating UGIB and LGIB using administrative data might help produce more precise estimates of costs and clinical outcomes, and aid in the development of risk stratification models.

References
  1. Zhao Y,Encinosa W.Hospitalizations for Gastrointestinal Bleeding in 1998 and 2006. HCUP Statistical Brief #65, December 2008.Rockville, MD:Agency for Healthcare Research and Quality.
  2. Wilcox CM,Clark WS.Causes and outcome of upper and lower gastrointestinal bleeding: The Grady Hospital Experience.South Med J.1999;92(1):4450.
  3. Blatchford O,Davidson LA,Murray WR, et al.Acute upper gastrointestinal haemorrhage in west of Scotland: case ascertainment study.BMJ.1997;315:510540.
  4. Jiradek GC,Kozarek RA.A cost‐effective approach to the patient with peptic ulcer bleeding.Surg Clin North Am.1996;76:83103.
  5. Longstreth GF.Epidemiology and outcome of patients hospitalized with acute lower gastrointestinal hemorrhage: a population based study.Am J Gastroenterol.1997;92:419424.
  6. Barkun A,Bardou M,Marshall J.Consensus recommendations for managing patients with nonvariceal upper gastrointestinal bleeding.Ann Int Med.2003;139:843857.
  7. Gralnek IM,Dulai GS.Incremental value of upper endoscopy for triage of patients with acute non‐variceal upper‐GI hemorrhage.Gastrointest Endosc2004;60:914.
  8. Hay JA,Lyubashevsky E,Elashoff J, et al.Upper gastrointestinal hemorrhage clinical guideline‐determining the optimal hospital length of stay.Am J Med.1996;100:313322.
  9. National Guideline Clearinghouse. Available at: http://www.guideline.gov. Accessed August2009.
  10. van der Hulst RW,Rauws EA,Koycu B, et al.Prevention of ulcer recurrence after eradication of Helicobacter pylori: a prospective long‐term follow‐up study.Gastroenterology.1997;113:10821086.
  11. Lai KC,Hui WM,Wong WM, et al.Treatment of Helicobacter pylori in patients with duodenal ulcer hemorrhage‐a long‐term randomized, controlled study.Am J Gastroenterol.2000;95:22252232.
  12. Chan FK,Chung SC,Suen BY, et al.Preventing recurrent upper gastrointestinal bleeding in patients with Helicobacter pylori infection who are taking low‐dose aspirin or naproxen.N Engl J Med.2001;344:967973.
  13. Lai KC,Lam SK,Chu KM, et al.Lansoprazole for the prevention of recurrences of ulcer complications from long‐term low‐dose aspirin use.N Engl J Med.2002;346:20332038.
  14. Bombardier C,Laine L,Reicin A, et al.Comparison of upper gastrointestinal toxicity of rofecoxib and naproxen in patients with rheumatoid arthritis. VIGOR Study Group.N Engl J Med.2000;343:15201528.
  15. Silverstein FE,Faich G,Goldstein JL, et al.Gastrointestinal toxicity with celecoxib vs nonsteroidal anti‐inflammatory drugs for osteoarthritis and rheumatoid arthritis: the CLASS study: a randomized controlled trial. Celecoxib Long‐Term Arthritis Safety Study.JAMA.2000;284:12471255.
  16. Lanas A,Garcia‐Rodriguez LA,Rodrigo L, et al.Time trends and clinical impact of upper and lower gastrointestinal complications. Digestive Disease Week National Meeting,2008. San Diego, CA, May 17–22.
  17. Goldstein JL,Eisen GM,Lewis B, et al.Video capsule endoscopy to prospectively assess small bowel injury with celecoxib, naproxen plus omeprazole, and placebo.Clin Gastroenterol Hepatol.2005;3:133141.
  18. Laine L,Connors LG,Reicin A, et al.Serious lower gastrointestinal clinical events with nonselective NSAID or Coxib use.Gastroenterology.2003;124:288292.
  19. Wasse H,Gillen DL,Ball AM, et al.Risk factors for upper gastrointestinal bleeding among end‐stage renal disease patients.Kidney Int.2003;64:14551461.
  20. Kaplan RC,Heckbert SR,Koepsell TD, et al.Risk factors for hospitalized bleeding among older patients.J Am Geriatr Soc.2001;49:126133.
  21. Institute for Clinical Systems Improvement (ICSI). Preventive services in adults. Bloomington, MN: Institute for Clinical Systems Improvement (ICSI).2005. Available at http://www.isci.org/guidelines_and_more/guidelines_order_sets_protocol/for_patients_families/preventive_services_for_adults_for_patients_families_.html. Accessed Month year.
  22. Cryer B.NSAID‐associated deaths: the rise and fall of NSAID‐associated GI mortality.Am J Gastroenterol.2005;100:16941695.
  23. Cryer B,Feldman M.Effects of very low doses of daily long‐term aspirin therapy on gastric, duodenal, and rectal prostaglandins on mucosal injury in healthy humans.Gastroenterology. 199;117:1725.
  24. Lanas A,Perez‐Asia MA,Feu F, et al.A nationwide study of mortality associated with hospital admission due to severe gastrointestinal events and those associated with nonsteroidal antiinflammatory drug use.Am J Gastroenterol.2005;100:16851693.
  25. van Leerdam ME,Vreeburg EM,Rauws EA, et al.Acute upper GI bleeding: did anything change?Am J Gastroenterol.2003;98:14941499.
  26. Lingenfelser T,Ell C.Lower intestinal bleeding.Best Pract Res Clin Gastroenterol.2001;15:135153.
  27. Charlson ME,Pompei P,Ales KL,MacKenzie CR.A new method of classifying prognostic comorbidity in longitudinal studies: development and validation.J Chronic Dis.1987;40:373383.
  28. AGS Panel on Persistent Pain in Older Persons. The management of persistent pain in older persons.J Am Geriatr Soc.2002;50(6 suppl):S205S224.
  29. Simon LS,Lipman AG,Jacox AK, et al.Pain in Osteoarthritis, Rheumatoid Arthritis and Juvenile Chronic Arthritis.2nd ed.Clinical practice guideline no. 2.Glenview, IL:American Pain Society (APS);2002:179.
  30. American College of Rheumatology Subcommittee on Osteoarthritis Guidelines.Recommendations for the Medical Management of Osteoarthritis of the Hip and Knee.Arthritis Rheum.2000;43:19051915.
References
  1. Zhao Y,Encinosa W.Hospitalizations for Gastrointestinal Bleeding in 1998 and 2006. HCUP Statistical Brief #65, December 2008.Rockville, MD:Agency for Healthcare Research and Quality.
  2. Wilcox CM,Clark WS.Causes and outcome of upper and lower gastrointestinal bleeding: The Grady Hospital Experience.South Med J.1999;92(1):4450.
  3. Blatchford O,Davidson LA,Murray WR, et al.Acute upper gastrointestinal haemorrhage in west of Scotland: case ascertainment study.BMJ.1997;315:510540.
  4. Jiradek GC,Kozarek RA.A cost‐effective approach to the patient with peptic ulcer bleeding.Surg Clin North Am.1996;76:83103.
  5. Longstreth GF.Epidemiology and outcome of patients hospitalized with acute lower gastrointestinal hemorrhage: a population based study.Am J Gastroenterol.1997;92:419424.
  6. Barkun A,Bardou M,Marshall J.Consensus recommendations for managing patients with nonvariceal upper gastrointestinal bleeding.Ann Int Med.2003;139:843857.
  7. Gralnek IM,Dulai GS.Incremental value of upper endoscopy for triage of patients with acute non‐variceal upper‐GI hemorrhage.Gastrointest Endosc2004;60:914.
  8. Hay JA,Lyubashevsky E,Elashoff J, et al.Upper gastrointestinal hemorrhage clinical guideline‐determining the optimal hospital length of stay.Am J Med.1996;100:313322.
  9. National Guideline Clearinghouse. Available at: http://www.guideline.gov. Accessed August2009.
  10. van der Hulst RW,Rauws EA,Koycu B, et al.Prevention of ulcer recurrence after eradication of Helicobacter pylori: a prospective long‐term follow‐up study.Gastroenterology.1997;113:10821086.
  11. Lai KC,Hui WM,Wong WM, et al.Treatment of Helicobacter pylori in patients with duodenal ulcer hemorrhage‐a long‐term randomized, controlled study.Am J Gastroenterol.2000;95:22252232.
  12. Chan FK,Chung SC,Suen BY, et al.Preventing recurrent upper gastrointestinal bleeding in patients with Helicobacter pylori infection who are taking low‐dose aspirin or naproxen.N Engl J Med.2001;344:967973.
  13. Lai KC,Lam SK,Chu KM, et al.Lansoprazole for the prevention of recurrences of ulcer complications from long‐term low‐dose aspirin use.N Engl J Med.2002;346:20332038.
  14. Bombardier C,Laine L,Reicin A, et al.Comparison of upper gastrointestinal toxicity of rofecoxib and naproxen in patients with rheumatoid arthritis. VIGOR Study Group.N Engl J Med.2000;343:15201528.
  15. Silverstein FE,Faich G,Goldstein JL, et al.Gastrointestinal toxicity with celecoxib vs nonsteroidal anti‐inflammatory drugs for osteoarthritis and rheumatoid arthritis: the CLASS study: a randomized controlled trial. Celecoxib Long‐Term Arthritis Safety Study.JAMA.2000;284:12471255.
  16. Lanas A,Garcia‐Rodriguez LA,Rodrigo L, et al.Time trends and clinical impact of upper and lower gastrointestinal complications. Digestive Disease Week National Meeting,2008. San Diego, CA, May 17–22.
  17. Goldstein JL,Eisen GM,Lewis B, et al.Video capsule endoscopy to prospectively assess small bowel injury with celecoxib, naproxen plus omeprazole, and placebo.Clin Gastroenterol Hepatol.2005;3:133141.
  18. Laine L,Connors LG,Reicin A, et al.Serious lower gastrointestinal clinical events with nonselective NSAID or Coxib use.Gastroenterology.2003;124:288292.
  19. Wasse H,Gillen DL,Ball AM, et al.Risk factors for upper gastrointestinal bleeding among end‐stage renal disease patients.Kidney Int.2003;64:14551461.
  20. Kaplan RC,Heckbert SR,Koepsell TD, et al.Risk factors for hospitalized bleeding among older patients.J Am Geriatr Soc.2001;49:126133.
  21. Institute for Clinical Systems Improvement (ICSI). Preventive services in adults. Bloomington, MN: Institute for Clinical Systems Improvement (ICSI).2005. Available at http://www.isci.org/guidelines_and_more/guidelines_order_sets_protocol/for_patients_families/preventive_services_for_adults_for_patients_families_.html. Accessed Month year.
  22. Cryer B.NSAID‐associated deaths: the rise and fall of NSAID‐associated GI mortality.Am J Gastroenterol.2005;100:16941695.
  23. Cryer B,Feldman M.Effects of very low doses of daily long‐term aspirin therapy on gastric, duodenal, and rectal prostaglandins on mucosal injury in healthy humans.Gastroenterology. 199;117:1725.
  24. Lanas A,Perez‐Asia MA,Feu F, et al.A nationwide study of mortality associated with hospital admission due to severe gastrointestinal events and those associated with nonsteroidal antiinflammatory drug use.Am J Gastroenterol.2005;100:16851693.
  25. van Leerdam ME,Vreeburg EM,Rauws EA, et al.Acute upper GI bleeding: did anything change?Am J Gastroenterol.2003;98:14941499.
  26. Lingenfelser T,Ell C.Lower intestinal bleeding.Best Pract Res Clin Gastroenterol.2001;15:135153.
  27. Charlson ME,Pompei P,Ales KL,MacKenzie CR.A new method of classifying prognostic comorbidity in longitudinal studies: development and validation.J Chronic Dis.1987;40:373383.
  28. AGS Panel on Persistent Pain in Older Persons. The management of persistent pain in older persons.J Am Geriatr Soc.2002;50(6 suppl):S205S224.
  29. Simon LS,Lipman AG,Jacox AK, et al.Pain in Osteoarthritis, Rheumatoid Arthritis and Juvenile Chronic Arthritis.2nd ed.Clinical practice guideline no. 2.Glenview, IL:American Pain Society (APS);2002:179.
  30. American College of Rheumatology Subcommittee on Osteoarthritis Guidelines.Recommendations for the Medical Management of Osteoarthritis of the Hip and Knee.Arthritis Rheum.2000;43:19051915.
Issue
Journal of Hospital Medicine - 5(3)
Issue
Journal of Hospital Medicine - 5(3)
Page Number
141-147
Page Number
141-147
Publications
Journal of Hospital Medicine
Publications
Journal of Hospital Medicine
Article Type
Article
Display Headline
Upper versus lower gastrointestinal bleeding: A direct comparison of clinical presentation, outcomes, and resource utilization
Display Headline
Upper versus lower gastrointestinal bleeding: A direct comparison of clinical presentation, outcomes, and resource utilization
Legacy Keywords
cost effectiveness, endoscopy, epidemiology, gastrointestinal hemorrhage
Legacy Keywords
cost effectiveness, endoscopy, epidemiology, gastrointestinal hemorrhage
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Original Research
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Corresponding Author
Chad T. Whelan, MD
Correspondence Location
Division of Hospital Medicine, Department of Medicine, Loyola University Chicago Stritch School of Medicine, 2160 South First Avenue, Maywood, IL 60153
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Continuing Medical Education Program in

Article Type
Article
Changed
Mon, 01/02/2017 - 19:34
Display Headline
Continuing Medical Education Program in the Journal of Hospital Medicine
Author(s)
Thomas E. Baudendistel, MD, FACP
Chad T. Whelan, MD
Connie Chen, PharmD
Peter Kaboli, MD, MS
Juned Siddique, DrPH
Micah Prochaska, BA
David O. Meltzer, MD, PhD

If you wish to receive credit for this activity, which begins on the next page, please refer to the website: www. blackwellpublishing.com/cme.

Accreditation and Designation Statement

Blackwell Futura Media Services designates this educational activity for a 1 AMA PRA Category 1 Credit. Physicians should only claim credit commensurate with the extent of their participation in the activity.

Blackwell Futura Media Services is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians.

Educational Objectives

Continuous participation in the Journal of Hospital Medicine CME program will enable learners to be better able to:

  • Interpret clinical guidelines and their applications for higher quality and more efficient care for all hospitalized patients.

  • Describe the standard of care for common illnesses and conditions treated in the hospital; such as pneumonia, COPD exacerbation, acute coronary syndrome, HF exacerbation, glycemic control, venous thromboembolic disease, stroke, etc.

  • Discuss evidence‐based recommendations involving transitions of care, including the hospital discharge process.

  • Gain insights into the roles of hospitalists as medical educators, researchers, medical ethicists, palliative care providers, and hospital‐based geriatricians.

  • Incorporate best practices for hospitalist administration, including quality improvement, patient safety, practice management, leadership, and demonstrating hospitalist value.

  • Identify evidence‐based best practices and trends for both adult and pediatric hospital medicine.

Instructions on Receiving Credit

For information on applicability and acceptance of continuing medical education credit for this activity, please consult your professional licensing board.

This activity is designed to be completed within the time designated on the title page; physicians should claim only those credits that reflect the time actually spent in the activity. To successfully earn credit, participants must complete the activity during the valid credit period that is noted on the title page.

Follow these steps to earn credit:

  • Log on to www.blackwellpublishing.com/cme.

  • Read the target audience, learning objectives, and author disclosures.

  • Read the article in print or online format.

  • Reflect on the article.

  • Access the CME Exam, and choose the best answer to each question.

  • Complete the required evaluation component of the activity.

Article PDF
692_ftp.pdf
Issue
Journal of Hospital Medicine - 5(3)
Publications
Journal of Hospital Medicine
Page Number
140-140
Sections
CME
Author(s)
Thomas E. Baudendistel, MD, FACP
Chad T. Whelan, MD
Connie Chen, PharmD
Peter Kaboli, MD, MS
Juned Siddique, DrPH
Micah Prochaska, BA
David O. Meltzer, MD, PhD
Author(s)
Thomas E. Baudendistel, MD, FACP
Chad T. Whelan, MD
Connie Chen, PharmD
Peter Kaboli, MD, MS
Juned Siddique, DrPH
Micah Prochaska, BA
David O. Meltzer, MD, PhD
Article PDF
692_ftp.pdf
Article PDF
692_ftp.pdf

If you wish to receive credit for this activity, which begins on the next page, please refer to the website: www. blackwellpublishing.com/cme.

Accreditation and Designation Statement

Blackwell Futura Media Services designates this educational activity for a 1 AMA PRA Category 1 Credit. Physicians should only claim credit commensurate with the extent of their participation in the activity.

Blackwell Futura Media Services is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians.

Educational Objectives

Continuous participation in the Journal of Hospital Medicine CME program will enable learners to be better able to:

  • Interpret clinical guidelines and their applications for higher quality and more efficient care for all hospitalized patients.

  • Describe the standard of care for common illnesses and conditions treated in the hospital; such as pneumonia, COPD exacerbation, acute coronary syndrome, HF exacerbation, glycemic control, venous thromboembolic disease, stroke, etc.

  • Discuss evidence‐based recommendations involving transitions of care, including the hospital discharge process.

  • Gain insights into the roles of hospitalists as medical educators, researchers, medical ethicists, palliative care providers, and hospital‐based geriatricians.

  • Incorporate best practices for hospitalist administration, including quality improvement, patient safety, practice management, leadership, and demonstrating hospitalist value.

  • Identify evidence‐based best practices and trends for both adult and pediatric hospital medicine.

Instructions on Receiving Credit

For information on applicability and acceptance of continuing medical education credit for this activity, please consult your professional licensing board.

This activity is designed to be completed within the time designated on the title page; physicians should claim only those credits that reflect the time actually spent in the activity. To successfully earn credit, participants must complete the activity during the valid credit period that is noted on the title page.

Follow these steps to earn credit:

  • Log on to www.blackwellpublishing.com/cme.

  • Read the target audience, learning objectives, and author disclosures.

  • Read the article in print or online format.

  • Reflect on the article.

  • Access the CME Exam, and choose the best answer to each question.

  • Complete the required evaluation component of the activity.

If you wish to receive credit for this activity, which begins on the next page, please refer to the website: www. blackwellpublishing.com/cme.

Accreditation and Designation Statement

Blackwell Futura Media Services designates this educational activity for a 1 AMA PRA Category 1 Credit. Physicians should only claim credit commensurate with the extent of their participation in the activity.

Blackwell Futura Media Services is accredited by the Accreditation Council for Continuing Medical Education to provide continuing medical education for physicians.

Educational Objectives

Continuous participation in the Journal of Hospital Medicine CME program will enable learners to be better able to:

  • Interpret clinical guidelines and their applications for higher quality and more efficient care for all hospitalized patients.

  • Describe the standard of care for common illnesses and conditions treated in the hospital; such as pneumonia, COPD exacerbation, acute coronary syndrome, HF exacerbation, glycemic control, venous thromboembolic disease, stroke, etc.

  • Discuss evidence‐based recommendations involving transitions of care, including the hospital discharge process.

  • Gain insights into the roles of hospitalists as medical educators, researchers, medical ethicists, palliative care providers, and hospital‐based geriatricians.

  • Incorporate best practices for hospitalist administration, including quality improvement, patient safety, practice management, leadership, and demonstrating hospitalist value.

  • Identify evidence‐based best practices and trends for both adult and pediatric hospital medicine.

Instructions on Receiving Credit

For information on applicability and acceptance of continuing medical education credit for this activity, please consult your professional licensing board.

This activity is designed to be completed within the time designated on the title page; physicians should claim only those credits that reflect the time actually spent in the activity. To successfully earn credit, participants must complete the activity during the valid credit period that is noted on the title page.

Follow these steps to earn credit:

  • Log on to www.blackwellpublishing.com/cme.

  • Read the target audience, learning objectives, and author disclosures.

  • Read the article in print or online format.

  • Reflect on the article.

  • Access the CME Exam, and choose the best answer to each question.

  • Complete the required evaluation component of the activity.

Issue
Journal of Hospital Medicine - 5(3)
Issue
Journal of Hospital Medicine - 5(3)
Page Number
140-140
Page Number
140-140
Publications
Journal of Hospital Medicine
Publications
Journal of Hospital Medicine
Article Type
Article
Display Headline
Continuing Medical Education Program in the Journal of Hospital Medicine
Display Headline
Continuing Medical Education Program in the Journal of Hospital Medicine
Sections
CME
Article Source
Copyright © 2010 Society of Hospital Medicine
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