From the AGA Journals

Duodenal bulb sampling barely increased celiac yield in low-probability cohort

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Extra pinches may not improve diagnostic recipe

Histologic diagnosis of celiac disease has traditionally relied upon endoscopic biopsies from the second and third portions of the duodenum. However, several recent studies indicate that duodenal bulb biopsies may show changes of celiac disease, despite normal histology in the more distal duodenum.

In their study, Dr. Stoven and her colleagues evaluated the diagnostic utility of endoscopic duodenal bulb biopsy in patients with a low probability for celiac disease. A new diagnosis of celiac disease was made in 16 of their 679 patients (2.4%). Only one patient showed villous atrophy of the duodenal bulb with normal histology of the more distal duodenum. Although a diagnosis of celiac disease was made, the case was atypical not only because distal duodenal biopsies were normal but also because multiple celiac serology tests were negative, raising the possibility of nonceliac villous atrophy. Thus, the added diagnostic yield of duodenal bulb biopsies in this low-risk population was extremely low (0.15% at most).

Dr. Ciaran P. Kelly

Dr. Ciaran P. Kelly

The extra biopsy will incur additional cost unless it is combined in the same sample container as the distal biopsies. However, combining the biopsies may pose diagnostic challenges for general, nonspecialized, pathologists. Incidental abnormalities, such as peptic duodenitis, are very common in the duodenal bulb; 35% of bulb samples were abnormal in this study. This can be a source of erroneous diagnoses to offset the very small increase in true diagnoses. Thus, for patients at low risk for celiac disease, extra pinches from the bulb may not improve the diagnostic recipe.

Ciaran P. Kelly, MD, AGAF, professor of medicine, Harvard Medical School, director Celiac Center, Beth Israel Deaconess Medical Center, Boston, has acted as a scientific adviser to companies including Celimmune, Cour Pharmaceuticals, ImmunogenX, and Takeda; he also acts as principal investigator on a research grant on celiac disease supported by Aptalis.


 

FROM CLINICAL GASTROENTEROLOGY AND HEPATOLOGY

Separate sampling of the duodenal bulb increased detection of celiac disease by only 0.1% when endoscopy patients had a low pretest probability of celiac disease, according to research published in the November issue of Clinical Gastroenterology and Hepatology.

Duodenal bulb histology did reveal other abnormal findings, such as chronic peptic duodenitis, gastric heterotopia, and Brunner gland hyperplasia, wrote Samantha Stoven, MD, of Mayo Clinic, Rochester, Minn., and her associates. These findings did not seem to impede the identification of celiac disease, but their clinical implications were unclear, the researchers noted.

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Most studies of the diagnostic yield of duodenal bulb specimens have been performed in patients with known celiac disease or positive serology. In past studies of these high-probability cohorts, duodenal bulb sampling increased the diagnostic yield of celiac disease anywhere from 1.8% to 18%, but whether and how that finding translates to low-probability cohorts is unclear, the researchers said. Therefore, they retrospectively analyzed data from 679 endoscopy patients who had both duodenal bulb and small bowel biopsies collected at three Mayo Clinic sites in 2011. These sites are “open access,” meaning that patients can be referred for endoscopy without the approval of a gastroenterologist.

The average age of the patients was 50 years, and 63% were female. They were most commonly referred for duodenal biopsy because of chronic dyspepsia (46% of patients), diarrhea (35%), or nausea (17%). Patients with either known celiac disease or positive serology were excluded from the study (Clin Gastroenterol Hepatol. 2016 Mar 7. doi: 10.1016/j.cgh.2016.02.026). A total of 265 patients (39%) had abnormal duodenal histology, which was most often diagnosed as chronic peptic duodenitis, the researchers said. Histologic abnormalities usually involved the duodenal bulb (36% of cases), not the distal duodenum (15%; P less than .0001). However, among the 16 patients (2%) found to have celiac disease, just one patient had disease only in the duodenal bulb. Thus, duodenal bulb sampling increased the diagnostic yield of celiac disease by only 0.1% when considering the overall cohort. The patient with celiac disease limited to the bulb was a 46-year-old female presenting with diarrhea and anemia who had normal serologies but a permissive human leukocyte antigen test. Her duodenal bulb had villous atrophy and more than 25 intraepithelial lymphocytes per 100 epithelial cells, while her distal duodenum was normal.

Among the 85% of patients who had normal distal duodenums, 28% had abnormal bulb histology, most often chronic peptic duodenitis, active chronic peptic duodenitis, or gastric heterotopia, the researchers said. Among the 59% of patients whose celiac serology before endoscopy was truly unknown, only two (0.5%) had histologic changes consistent with celiac disease, which in both cases were located in the distal duodenum.

SOURCE: American Gastroenterological Association

“Individual sampling of the duodenal bulb in patients with either negative or unknown celiac serologic status can be considered in practices where expert gastrointestinal pathologists are present and there is agreement that both samples can be submitted in the same bottle, or there is not a separate charge for the additional container. Further studies may be needed to assess the diagnostic yield of separate bulb biopsies for celiac detection in all comers.”

An American College of Gastroenterology Junior Faculty Development Award helped support the work. Senior author Joseph A. Murray, MD, disclosed ties to Alba Therapeutics, Alvine Pharmaceuticals, AMAG Pharmaceuticals, and several other corporate entities. The remaining authors had no disclosures.

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