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Clinical Preventive Medicine: Primum Non Nocere?
The principle of “first, do no harm” comes from the oath of Hippocrates: “I will follow that method of treatment which, according to my ability and judgment, I consider for the benefit of my patients, and abstain from whatever is deleterious and mischievous.”
An assertion by Miller1 is consistent with this oath: “The ethical requirements for the introduction of screening are stringent” because of the “risks associated with screening, which extend beyond the risks of the test itself, to those associated with invitations for screening, false reassurance for false negatives, the diagnostic process and the problem of false positives, and the overtreatment of those with borderline abnormalities.” Tuohey,2 however, argues that avoidance of harm is not enough and that the Hippocratic oath also includes the principle of benefit. The United States Preventive Services Task Force (USPSTF)3 acknowledges this balance in its statement about preventive counseling:
Given the safety and generally low cost of advising patients about health-related behaviors, the USPSTF recommends routinely addressing some health behaviors even when the long-term effectiveness of such counseling has not yet been definitively proven. In their updated recommendations, however, the USPSTF explicitly distinguished between recommendations based on good evidence of the effectiveness of counseling per se (eg, smoking cessation) and recommendations made primarily on the basis of the strong link between behavior and disease (eg, sexually transmitted disease prevention).
Is prevention counseling safe?
A key assumption supporting these recommendations is the safety of counseling for primary prevention. Unfortunately, the work of Bowman and colleagues4 in this issue of the Journal challenges the benign nature of recommending behavioral change to patients. In that study, patients whose physicians recommended a behavioral change had lower self-esteem, worse mental and social health, and more dysfunction from anxiety, anxiety/depression, and depression 3 months after the visit than patients whose physicians had not recommended this type of change.
To its credit, the USPSTF explicitly considers the adverse effects of screening tests in its recommendations about secondary prevention. The paper by Mold and coworkers5 in this issue of the Journal adds to the literature cited in the USPSTF’s second report. These authors found an apparent adverse effect of labeling, with hypertensive patients estimating recovery time from an upper respiratory tract infection that was nearly twice as long as that estimated by patients who did not have hypertension.
These 2 studies bother me. I am an unabashed prevention enthusiast. I teach second-year medical students the USPSTF methodology and recommendations, and I lead a monthly clerkship seminar on helping people change problem behaviors. I hound residents about prevention at every turn: a session on the checkup visit for each stage in our lifecycle core curriculum, waxing on about prevention during precepting in the clinic, organizing the checkup visit by major categories of death and disability (cardiovascular disease, cancer, and so forth) instead of the traditional history and physical examination (history of present illness, past medical history, family history, social history), and a customized prevention template in our electronic medical record. For trauma prevention, I have even asked patients about handguns, despite the survey results from Shaughnessy and colleagues that state most patients believe gun safety should not be discussed during an office visit.6 But these 2 papers have led me to question whether my enthusiasm is misguided and may be a disservice to my patients. I wonder if the potential for an adverse effect of counseling or labeling is a widespread phenomenon. Is it a long-term problem? Can we do anything to minimize it?
What the literature shows
A quick search of the literature shows that the concern about possible adverse effects of screening and risk assessment cuts across all areas of prevention. In metabolic disease prevention, adults screened for carrier status in cystic fibrosis7-9 were anxious while awaiting the test results, but the anxiety resolved by 3 months and had no effect on perception of health. Individuals screened for risk of Huntington’s disease10-17 experienced anxiety and depression in the first 2 months after the test, which generally decreased in the following year, especially after a good test result. Those who had pessimistic risk perceptions or pretest depression responded more poorly to the information. Pregnant women having serum screening for congenital anomalies18 reported no adverse psychological effects at 24 weeks’ gestation. Those having false-positive screening results for gestational diabetes mellitus19 rated their health lower at 32 weeks’ gestation than those with negative results but did not differ on anxiety, depression, or concern levels about the health of their newborn.
Men screened for prostate cancer20 had high serum cortisol levels at the screening examination, that were back to normal in 2 weeks. The highest levels were from those getting biopsies, but they returned to normal when informed of the results, regardless of whether those results were abnormal. The authors suggested minimizing the interval between a test and informing the patient of the results to decrease the duration of stress. Breast cancer screening21-23 leads to short-term increases in anxiety, distress, and intrusive thoughts. In breast cancer susceptibility genetic testing,24-27 there was more distress if the person was tested first or if previously tested siblings were not carriers. In general, distress declined after testing, but women anticipated a negative psychologic impact of positive test results involving anxiety, depression, and impaired quality of life, while others still worried even with a negative test result. A false-positive screening result for ovarian cancer28 was associated with short-term distress but not severe or persistent distress. For cervical cancer,29 3 months after a positive Pap- anicolaou test result women had significant elevation in worries about cancer and impairments in mood, daily activities, sexual interest, and sleep patterns. These adverse effects were most pronounced in those who did not comply with colposcopy, for whom uncertainty was maintained by lack of compliance. Testing children for familial polyposis30 did not lead to adverse effects, as child and parent depression, anxiety, and behavioral problem scores remained normal 3 months after testing for children with both mutation-positive and mutation-negative results. Patients screened for colorectal cancer31 were distressed by an invitation letter, a positive test result, and delays in the process of screening (eg, wait of 10 days to colonoscopy), but reported that it was worthwhile to have had the test. In general cancer screening programs,32-34 anxiety, distress, and depression symptoms can be reduced by a brief orientation program at the clinic visit. It has been suggested that a moderate amount of anxiety about results may even be a motivating factor in getting subsequent checkups, but severe distress can interfere with adherence behavior.
In cardiovascular disease prevention, screening did not increase work absenteeism in the year after men were informed they had hypercholesterolemia and an elevated risk for myocardial infarction.35 Interestingly, half of the men denied having hypercholesterolemia 1 year after being informed and had no changes on psychological measures.36 In general screening for coronary artery disease risk (CAD), an “above average risk” label for CAD did not adversely affect psychological state if the individuals were prepared for risk labeling. However, communication of abnormal results without adequate preparation did cause short-term psychological harm. Nonspecific support from a familiar generalist physician reduced the risk of psychological ill health.37 There ere no changes in General Health Questionnaire scores before and 6 months after a screening examination,38 and no evidence of raised concerns about health or risk of heart attack.39 There has been a tendency to be bothered by intrusive thoughts, but not to the degree that patients were upset.40 There was no difference between the high-risk and reference populations in satisfaction with life or emotional well-being in the year after screening, but a substantial number of people reported distaste at being reminded of their risk of CAD.41 The authors of one study noted that psychological distress significantly increased 3 months after screening.42
In a review of DNA testing,43 those patients who were depressed before the test were more distressed after testing, but those who were anxious before the test were less distressed after the test, having fewer intrusive thoughts. In this area, the test result did not determine the amount of distress experienced by those tested. In another review44 of studies about cardiovascular risk, acquired immune deficiency syndrome, cancer, Huntington’s disease, diabetes mellitus, spinocerebellar ataxia, and osteoporosis, positive results were associated in the short term with depression, anxiety, poorer perceptions of health, and psychological distress. There was no distress in the longer term and little evidence of adverse psychological effects for those receiving unfavorable test results.
Conclusions
This scan of the literature allayed much of my initial concern about the psychological safety of primary and secondary prevention raised by the papers by Bowman and Mold and their colleagues. Yes, phenomena similar to their findings have been noted for many other conditions, but fortunately the adverse effects are neither long term nor particularly serious. In addition, this brief summary suggests ways to minimize the impact as well: (1) assess the patient’s pretest psychological state for depression or pessimism; (2) provide pretest orientation and preparation for risk stratification; (3) minimize delay between testing and informing the patient about the results; and (4) use an established physician-patient relationship to give the patient general support. The unexplored and provocative conclusion is that some distress or anxiety may be desirable because it may help motivate a patient to adhere to recommendations for further testing or to start behavioral change.
The oath of Maimonides states: “I have been appointed to watch over the life and death of my fellow human beings. Here I am ready for my vocation, and now I turn unto my calling.” Maybe we have to cause a little hurt to help even more.
1. Miller AB. The ethics, the risks and the benefits of screening. Biomed Pharmacother 1988;42:439-42.
2. Tuohey JF. Balancing benefit and burden: merely avoiding harm does not carry out the intent of the Hippocratic oath. Health Prog 1989;70:77-9.
3. US Preventive Services Task Force. Guide to clinical preventive services. 2nd ed. Baltimore, Md: Williams & Wilkins; 1996;lxxv-lxxvi.
4. Bowman MA, Dignan M, Crandall S, Baier M. Changes in functional status related to health maintenance visits to family physicians. J Fam Pract 2000;49:428-33.
5. Mold JW, Hamm R, Jafri B. The effect of labeling on perceived ability to recover from acute illnesses and injuries. J Fam Pract 2000;49:437-40.
6. Shaughnessy AF, Cincotta JA, Adelman A. Family practice patients’ attitudes toward firearm safety as a preventive medicine issue: a HARNET Study: Harrisburg Area Research Network. J Am Board Fam Pract 1999;12:354-9.
7. Mennie ME, Compton ME, Gilfillan A, et al. Prenatal screening for cystic fibrosis: psychological effects on carriers and their partners. J Med Genet 1993;30:543-8.
8. Clausen H, Brandt NJ, Schwartz M, Skovby F. Psychological and social impact of carrier screening for cystic fibrosis among pregnant woman-a pilot study. Clin Genet 1996;49:200-5.
9. Bekker H, Denniss G, Modell M, Bobrow M, Marteau T. The impact of population based screening for carriers of cystic fibrosis. J Med Genet 1994;31:364-8.
10. Decruyenaere M, Evers-Kiebooms G, Boogaerts A, et al. Psychological functioning before predictive testing for Huntington’s disease: the role of the parental disease, risk perception, and subjective proximity of the disease. J Med Genet 1999;36:897-905.
11. Wiggins S, Whyte P, Huggins M, Adam S, Theilmann J, Bloch M, Shep Schechter MT, Hayden MR. The psychological consequences of predictive testing for Huntington’s disease: Canadian Collaborative Study of Predictive Testing. N Engl J Med 1992;327:1401-5.
12. Codori AM, Brandt J. Psychological costs and benefits of predictive testing for Huntington’s disease. Am J Med Genet 1994;54:174-84.
13. Bloch M, Adam S, Wiggins S, Huggins M, Hayden MR. Predictive testing for Huntington disease in Canada: the experience of those receiving an increased risk. Am J Med Genet 1992;42:499-507.
14. Meissen GJ, Mastromauro CA, Kiely DK, McNamara DS, Myers RH. Understanding the decision to take the predictive test for Huntington disease. Am J Med Genet 1991;39:404-10.
15. Lawson K, Wiggins S, Green T, Adam S, Bloch M, Hayden MR. Adverse psychological events occurring in the first year after predictive testing for Huntington’s disease: the Canadian Collaborative Study Predictive Testing. J Med Genet 1996;33:856-62.
16. Decruyenaere M, Evers-Kiebooms G, Boogaerts A, et al. Prediction of psychological functioning one year after the predictive test for Huntington’s disease and impact of the test result on reproductive decision making. J Med Genet 1996;33:737-43.
17. Codori AM, Slavney PR, Young C, Miglioretti DL, Brandt J. Predictors of psychological adjustment to genetic testing for Huntington’s disease. Health Psychol 1997;161:36-50.
18. Goel V, Glazier R, Summers A, Holzapfel S. Psychological outcomes following maternal serum screening: a cohort study. CMAJ 1998;159:651-6.
19. Kerbel D, Glazier R, Holzapfel S, Yeung M, Lofsky S. Adverse effects of screening for gestational diabetes: a prospect cohort study in Toronto, Canada. J Med Screen 1997;4:128-32.
20. Gustafsson O, Theorell T, Normin U, Perski A, Ohstrom M, Nyman C. Psychological reactions in men screened for prostate cancer. Br J Urol 1995;75:631-61.
21. Ellman R, Angeli N, Christians A, Moss S, Chamberlain J, Maguire P. Psychiatric morbidity associated with screening for breast cancer. Br J Cancer 1989;60:781-4.
22. Gram IT, Lund E, Slenker SE. Quality of life following a false positive mammogram. Br J Cancer 1990;62:1018-22.
23. Rimer BK, Bluman LG. The psychosocial consequences of mammography. J Natl Cancer Inst Monogr 1997;22:131-8.
24. Lerman C, Seay J, Balshem A, Audrain J. Interest in genetic testing among first-degree relatives of breast cancer patients. Am J Med Genet 1995;57:385-92.
25. Croyle RT, Smith KR, Botkin JR, Baty B, Nash J. Psychological responses to BRCA1 mutation testing: preliminary findings. Health Psychol 1997;16:63-72.
26. Lerman C, Schwartz MD, Lin TH, Hughes C, Narod S, Lynch HT. The influence of psychological distress on use of genetic testing cancer risk. J Consult Clin Psychol 1997;65:414-20.
27. Smith KR, West JA, Croyle RT, Botkin JR. Familial context of genetic testing for cancer susceptibility: moderating effect of siblings’ test results on psychological distress one to two weeks after BRCA 1 mutation testing. Epidemiol Biomarkers Prev 1999;8:385-92.
28. Wardle FJ, Collins W, Pernet AL, Whitehead MI, Bourne TH, Campbell S. Psychological impact of screening for familial ovarian cancer. J Natl Cancer Inst 1993;85:653-7.
29. Lerman C, Miller SM, Scarborough R, Hanjani P, Nolte S, Smith D. Adverse psychologic consequences of positive cytologic cervical screening. Am J Obstet Gynecl 1991;165:658-22.
30. Codori AM, Petersen GM, Boyd PA, Brandt J, Giardiello FM. Genetic testing for cancer in children: short-term psychological effect. Arch Pediatr Adolesc Med 1996;150:1131-8.
31. Mant D, Fitzpatrick R, Hogg A, et al. Experiences of patients with false positive results from colorectal cancer screening. Br J Gen Pract 1990;40:423-5.
32. Lerman CE, Rimer BK. Psychosocial impact of cancer screening. Oncology 1993;7:67-72,75,79.
33. McQuellon RP, Wells M, Hoffman S, et al. Reducing distress in cancer patients with an orientation program. Psychooncology 1998;7:207-17.
34. Wardle J, Pope R. The psychological costs of screening for cancer. J Psychosom Res 1992;36:609-24.
35. Rastam L, Frick JO, Gullberg B. Work absenteeism in men who are labeled hypercholesterolaemic in screening. Eur Heart J 1991;12:1316-20.
36. Irvine MJ, Logan AG. Is knowing your cholesterol number harmful? J Clin Epidemiol 1994;47:131-45.
37. Connelly J, Cooper J, Mann A, Meade TW. The psychological impact of screening for risk of coronary heart disease in primary care settings. J Cardiovasc Risk 1998;5:185-91.
38. Christensen B. Psychological reactions to information about risk of ischaemic heart disease in general practice. Scand J Prim Health Care 1995;13:164-7.
39. Marteau TM, Kinmonth AL, Thompson S, Pyke S. The psychological impact of cardiovascular screening and intervention in primary care: a problem of false reassurance? British Family Heart Study Group. Br J Gen Pract 1996;46:577-82.
40. Horowitz MJ, Simon N, Holden M, et al. The stressful impact of news of risk for premature heart disease. Psychosom Med 1983;45:31-40.
41. Meland E, Laerum E, Maeland JG. Life style intervention in general practice: effects on psychological well-being and patient satisfaction. Qual Life Res 1996;5:348-54.
42. Stoate HG. Can health screening damage your health? J R Coll Gen Pract 1989;39:193-5.
43. DudokdeWit AC, Tibben A, Duivenvoorden HJ, Niermeijer MF, Passchier J. Predicting adaptation to presymptomatic DNA testing for late ovarian disorders: who will experience distress? Rotterdam Leiden Gen Workgroup. J Med Genet 1998;35:745-54.
44. Shaw C, Abrams, Marteau TM. Psychological impact of predicting individuals’ risks of illness: a systematic review. Soc Sci Med 1999;49:1571-98.-
The principle of “first, do no harm” comes from the oath of Hippocrates: “I will follow that method of treatment which, according to my ability and judgment, I consider for the benefit of my patients, and abstain from whatever is deleterious and mischievous.”
An assertion by Miller1 is consistent with this oath: “The ethical requirements for the introduction of screening are stringent” because of the “risks associated with screening, which extend beyond the risks of the test itself, to those associated with invitations for screening, false reassurance for false negatives, the diagnostic process and the problem of false positives, and the overtreatment of those with borderline abnormalities.” Tuohey,2 however, argues that avoidance of harm is not enough and that the Hippocratic oath also includes the principle of benefit. The United States Preventive Services Task Force (USPSTF)3 acknowledges this balance in its statement about preventive counseling:
Given the safety and generally low cost of advising patients about health-related behaviors, the USPSTF recommends routinely addressing some health behaviors even when the long-term effectiveness of such counseling has not yet been definitively proven. In their updated recommendations, however, the USPSTF explicitly distinguished between recommendations based on good evidence of the effectiveness of counseling per se (eg, smoking cessation) and recommendations made primarily on the basis of the strong link between behavior and disease (eg, sexually transmitted disease prevention).
Is prevention counseling safe?
A key assumption supporting these recommendations is the safety of counseling for primary prevention. Unfortunately, the work of Bowman and colleagues4 in this issue of the Journal challenges the benign nature of recommending behavioral change to patients. In that study, patients whose physicians recommended a behavioral change had lower self-esteem, worse mental and social health, and more dysfunction from anxiety, anxiety/depression, and depression 3 months after the visit than patients whose physicians had not recommended this type of change.
To its credit, the USPSTF explicitly considers the adverse effects of screening tests in its recommendations about secondary prevention. The paper by Mold and coworkers5 in this issue of the Journal adds to the literature cited in the USPSTF’s second report. These authors found an apparent adverse effect of labeling, with hypertensive patients estimating recovery time from an upper respiratory tract infection that was nearly twice as long as that estimated by patients who did not have hypertension.
These 2 studies bother me. I am an unabashed prevention enthusiast. I teach second-year medical students the USPSTF methodology and recommendations, and I lead a monthly clerkship seminar on helping people change problem behaviors. I hound residents about prevention at every turn: a session on the checkup visit for each stage in our lifecycle core curriculum, waxing on about prevention during precepting in the clinic, organizing the checkup visit by major categories of death and disability (cardiovascular disease, cancer, and so forth) instead of the traditional history and physical examination (history of present illness, past medical history, family history, social history), and a customized prevention template in our electronic medical record. For trauma prevention, I have even asked patients about handguns, despite the survey results from Shaughnessy and colleagues that state most patients believe gun safety should not be discussed during an office visit.6 But these 2 papers have led me to question whether my enthusiasm is misguided and may be a disservice to my patients. I wonder if the potential for an adverse effect of counseling or labeling is a widespread phenomenon. Is it a long-term problem? Can we do anything to minimize it?
What the literature shows
A quick search of the literature shows that the concern about possible adverse effects of screening and risk assessment cuts across all areas of prevention. In metabolic disease prevention, adults screened for carrier status in cystic fibrosis7-9 were anxious while awaiting the test results, but the anxiety resolved by 3 months and had no effect on perception of health. Individuals screened for risk of Huntington’s disease10-17 experienced anxiety and depression in the first 2 months after the test, which generally decreased in the following year, especially after a good test result. Those who had pessimistic risk perceptions or pretest depression responded more poorly to the information. Pregnant women having serum screening for congenital anomalies18 reported no adverse psychological effects at 24 weeks’ gestation. Those having false-positive screening results for gestational diabetes mellitus19 rated their health lower at 32 weeks’ gestation than those with negative results but did not differ on anxiety, depression, or concern levels about the health of their newborn.
Men screened for prostate cancer20 had high serum cortisol levels at the screening examination, that were back to normal in 2 weeks. The highest levels were from those getting biopsies, but they returned to normal when informed of the results, regardless of whether those results were abnormal. The authors suggested minimizing the interval between a test and informing the patient of the results to decrease the duration of stress. Breast cancer screening21-23 leads to short-term increases in anxiety, distress, and intrusive thoughts. In breast cancer susceptibility genetic testing,24-27 there was more distress if the person was tested first or if previously tested siblings were not carriers. In general, distress declined after testing, but women anticipated a negative psychologic impact of positive test results involving anxiety, depression, and impaired quality of life, while others still worried even with a negative test result. A false-positive screening result for ovarian cancer28 was associated with short-term distress but not severe or persistent distress. For cervical cancer,29 3 months after a positive Pap- anicolaou test result women had significant elevation in worries about cancer and impairments in mood, daily activities, sexual interest, and sleep patterns. These adverse effects were most pronounced in those who did not comply with colposcopy, for whom uncertainty was maintained by lack of compliance. Testing children for familial polyposis30 did not lead to adverse effects, as child and parent depression, anxiety, and behavioral problem scores remained normal 3 months after testing for children with both mutation-positive and mutation-negative results. Patients screened for colorectal cancer31 were distressed by an invitation letter, a positive test result, and delays in the process of screening (eg, wait of 10 days to colonoscopy), but reported that it was worthwhile to have had the test. In general cancer screening programs,32-34 anxiety, distress, and depression symptoms can be reduced by a brief orientation program at the clinic visit. It has been suggested that a moderate amount of anxiety about results may even be a motivating factor in getting subsequent checkups, but severe distress can interfere with adherence behavior.
In cardiovascular disease prevention, screening did not increase work absenteeism in the year after men were informed they had hypercholesterolemia and an elevated risk for myocardial infarction.35 Interestingly, half of the men denied having hypercholesterolemia 1 year after being informed and had no changes on psychological measures.36 In general screening for coronary artery disease risk (CAD), an “above average risk” label for CAD did not adversely affect psychological state if the individuals were prepared for risk labeling. However, communication of abnormal results without adequate preparation did cause short-term psychological harm. Nonspecific support from a familiar generalist physician reduced the risk of psychological ill health.37 There ere no changes in General Health Questionnaire scores before and 6 months after a screening examination,38 and no evidence of raised concerns about health or risk of heart attack.39 There has been a tendency to be bothered by intrusive thoughts, but not to the degree that patients were upset.40 There was no difference between the high-risk and reference populations in satisfaction with life or emotional well-being in the year after screening, but a substantial number of people reported distaste at being reminded of their risk of CAD.41 The authors of one study noted that psychological distress significantly increased 3 months after screening.42
In a review of DNA testing,43 those patients who were depressed before the test were more distressed after testing, but those who were anxious before the test were less distressed after the test, having fewer intrusive thoughts. In this area, the test result did not determine the amount of distress experienced by those tested. In another review44 of studies about cardiovascular risk, acquired immune deficiency syndrome, cancer, Huntington’s disease, diabetes mellitus, spinocerebellar ataxia, and osteoporosis, positive results were associated in the short term with depression, anxiety, poorer perceptions of health, and psychological distress. There was no distress in the longer term and little evidence of adverse psychological effects for those receiving unfavorable test results.
Conclusions
This scan of the literature allayed much of my initial concern about the psychological safety of primary and secondary prevention raised by the papers by Bowman and Mold and their colleagues. Yes, phenomena similar to their findings have been noted for many other conditions, but fortunately the adverse effects are neither long term nor particularly serious. In addition, this brief summary suggests ways to minimize the impact as well: (1) assess the patient’s pretest psychological state for depression or pessimism; (2) provide pretest orientation and preparation for risk stratification; (3) minimize delay between testing and informing the patient about the results; and (4) use an established physician-patient relationship to give the patient general support. The unexplored and provocative conclusion is that some distress or anxiety may be desirable because it may help motivate a patient to adhere to recommendations for further testing or to start behavioral change.
The oath of Maimonides states: “I have been appointed to watch over the life and death of my fellow human beings. Here I am ready for my vocation, and now I turn unto my calling.” Maybe we have to cause a little hurt to help even more.
The principle of “first, do no harm” comes from the oath of Hippocrates: “I will follow that method of treatment which, according to my ability and judgment, I consider for the benefit of my patients, and abstain from whatever is deleterious and mischievous.”
An assertion by Miller1 is consistent with this oath: “The ethical requirements for the introduction of screening are stringent” because of the “risks associated with screening, which extend beyond the risks of the test itself, to those associated with invitations for screening, false reassurance for false negatives, the diagnostic process and the problem of false positives, and the overtreatment of those with borderline abnormalities.” Tuohey,2 however, argues that avoidance of harm is not enough and that the Hippocratic oath also includes the principle of benefit. The United States Preventive Services Task Force (USPSTF)3 acknowledges this balance in its statement about preventive counseling:
Given the safety and generally low cost of advising patients about health-related behaviors, the USPSTF recommends routinely addressing some health behaviors even when the long-term effectiveness of such counseling has not yet been definitively proven. In their updated recommendations, however, the USPSTF explicitly distinguished between recommendations based on good evidence of the effectiveness of counseling per se (eg, smoking cessation) and recommendations made primarily on the basis of the strong link between behavior and disease (eg, sexually transmitted disease prevention).
Is prevention counseling safe?
A key assumption supporting these recommendations is the safety of counseling for primary prevention. Unfortunately, the work of Bowman and colleagues4 in this issue of the Journal challenges the benign nature of recommending behavioral change to patients. In that study, patients whose physicians recommended a behavioral change had lower self-esteem, worse mental and social health, and more dysfunction from anxiety, anxiety/depression, and depression 3 months after the visit than patients whose physicians had not recommended this type of change.
To its credit, the USPSTF explicitly considers the adverse effects of screening tests in its recommendations about secondary prevention. The paper by Mold and coworkers5 in this issue of the Journal adds to the literature cited in the USPSTF’s second report. These authors found an apparent adverse effect of labeling, with hypertensive patients estimating recovery time from an upper respiratory tract infection that was nearly twice as long as that estimated by patients who did not have hypertension.
These 2 studies bother me. I am an unabashed prevention enthusiast. I teach second-year medical students the USPSTF methodology and recommendations, and I lead a monthly clerkship seminar on helping people change problem behaviors. I hound residents about prevention at every turn: a session on the checkup visit for each stage in our lifecycle core curriculum, waxing on about prevention during precepting in the clinic, organizing the checkup visit by major categories of death and disability (cardiovascular disease, cancer, and so forth) instead of the traditional history and physical examination (history of present illness, past medical history, family history, social history), and a customized prevention template in our electronic medical record. For trauma prevention, I have even asked patients about handguns, despite the survey results from Shaughnessy and colleagues that state most patients believe gun safety should not be discussed during an office visit.6 But these 2 papers have led me to question whether my enthusiasm is misguided and may be a disservice to my patients. I wonder if the potential for an adverse effect of counseling or labeling is a widespread phenomenon. Is it a long-term problem? Can we do anything to minimize it?
What the literature shows
A quick search of the literature shows that the concern about possible adverse effects of screening and risk assessment cuts across all areas of prevention. In metabolic disease prevention, adults screened for carrier status in cystic fibrosis7-9 were anxious while awaiting the test results, but the anxiety resolved by 3 months and had no effect on perception of health. Individuals screened for risk of Huntington’s disease10-17 experienced anxiety and depression in the first 2 months after the test, which generally decreased in the following year, especially after a good test result. Those who had pessimistic risk perceptions or pretest depression responded more poorly to the information. Pregnant women having serum screening for congenital anomalies18 reported no adverse psychological effects at 24 weeks’ gestation. Those having false-positive screening results for gestational diabetes mellitus19 rated their health lower at 32 weeks’ gestation than those with negative results but did not differ on anxiety, depression, or concern levels about the health of their newborn.
Men screened for prostate cancer20 had high serum cortisol levels at the screening examination, that were back to normal in 2 weeks. The highest levels were from those getting biopsies, but they returned to normal when informed of the results, regardless of whether those results were abnormal. The authors suggested minimizing the interval between a test and informing the patient of the results to decrease the duration of stress. Breast cancer screening21-23 leads to short-term increases in anxiety, distress, and intrusive thoughts. In breast cancer susceptibility genetic testing,24-27 there was more distress if the person was tested first or if previously tested siblings were not carriers. In general, distress declined after testing, but women anticipated a negative psychologic impact of positive test results involving anxiety, depression, and impaired quality of life, while others still worried even with a negative test result. A false-positive screening result for ovarian cancer28 was associated with short-term distress but not severe or persistent distress. For cervical cancer,29 3 months after a positive Pap- anicolaou test result women had significant elevation in worries about cancer and impairments in mood, daily activities, sexual interest, and sleep patterns. These adverse effects were most pronounced in those who did not comply with colposcopy, for whom uncertainty was maintained by lack of compliance. Testing children for familial polyposis30 did not lead to adverse effects, as child and parent depression, anxiety, and behavioral problem scores remained normal 3 months after testing for children with both mutation-positive and mutation-negative results. Patients screened for colorectal cancer31 were distressed by an invitation letter, a positive test result, and delays in the process of screening (eg, wait of 10 days to colonoscopy), but reported that it was worthwhile to have had the test. In general cancer screening programs,32-34 anxiety, distress, and depression symptoms can be reduced by a brief orientation program at the clinic visit. It has been suggested that a moderate amount of anxiety about results may even be a motivating factor in getting subsequent checkups, but severe distress can interfere with adherence behavior.
In cardiovascular disease prevention, screening did not increase work absenteeism in the year after men were informed they had hypercholesterolemia and an elevated risk for myocardial infarction.35 Interestingly, half of the men denied having hypercholesterolemia 1 year after being informed and had no changes on psychological measures.36 In general screening for coronary artery disease risk (CAD), an “above average risk” label for CAD did not adversely affect psychological state if the individuals were prepared for risk labeling. However, communication of abnormal results without adequate preparation did cause short-term psychological harm. Nonspecific support from a familiar generalist physician reduced the risk of psychological ill health.37 There ere no changes in General Health Questionnaire scores before and 6 months after a screening examination,38 and no evidence of raised concerns about health or risk of heart attack.39 There has been a tendency to be bothered by intrusive thoughts, but not to the degree that patients were upset.40 There was no difference between the high-risk and reference populations in satisfaction with life or emotional well-being in the year after screening, but a substantial number of people reported distaste at being reminded of their risk of CAD.41 The authors of one study noted that psychological distress significantly increased 3 months after screening.42
In a review of DNA testing,43 those patients who were depressed before the test were more distressed after testing, but those who were anxious before the test were less distressed after the test, having fewer intrusive thoughts. In this area, the test result did not determine the amount of distress experienced by those tested. In another review44 of studies about cardiovascular risk, acquired immune deficiency syndrome, cancer, Huntington’s disease, diabetes mellitus, spinocerebellar ataxia, and osteoporosis, positive results were associated in the short term with depression, anxiety, poorer perceptions of health, and psychological distress. There was no distress in the longer term and little evidence of adverse psychological effects for those receiving unfavorable test results.
Conclusions
This scan of the literature allayed much of my initial concern about the psychological safety of primary and secondary prevention raised by the papers by Bowman and Mold and their colleagues. Yes, phenomena similar to their findings have been noted for many other conditions, but fortunately the adverse effects are neither long term nor particularly serious. In addition, this brief summary suggests ways to minimize the impact as well: (1) assess the patient’s pretest psychological state for depression or pessimism; (2) provide pretest orientation and preparation for risk stratification; (3) minimize delay between testing and informing the patient about the results; and (4) use an established physician-patient relationship to give the patient general support. The unexplored and provocative conclusion is that some distress or anxiety may be desirable because it may help motivate a patient to adhere to recommendations for further testing or to start behavioral change.
The oath of Maimonides states: “I have been appointed to watch over the life and death of my fellow human beings. Here I am ready for my vocation, and now I turn unto my calling.” Maybe we have to cause a little hurt to help even more.
1. Miller AB. The ethics, the risks and the benefits of screening. Biomed Pharmacother 1988;42:439-42.
2. Tuohey JF. Balancing benefit and burden: merely avoiding harm does not carry out the intent of the Hippocratic oath. Health Prog 1989;70:77-9.
3. US Preventive Services Task Force. Guide to clinical preventive services. 2nd ed. Baltimore, Md: Williams & Wilkins; 1996;lxxv-lxxvi.
4. Bowman MA, Dignan M, Crandall S, Baier M. Changes in functional status related to health maintenance visits to family physicians. J Fam Pract 2000;49:428-33.
5. Mold JW, Hamm R, Jafri B. The effect of labeling on perceived ability to recover from acute illnesses and injuries. J Fam Pract 2000;49:437-40.
6. Shaughnessy AF, Cincotta JA, Adelman A. Family practice patients’ attitudes toward firearm safety as a preventive medicine issue: a HARNET Study: Harrisburg Area Research Network. J Am Board Fam Pract 1999;12:354-9.
7. Mennie ME, Compton ME, Gilfillan A, et al. Prenatal screening for cystic fibrosis: psychological effects on carriers and their partners. J Med Genet 1993;30:543-8.
8. Clausen H, Brandt NJ, Schwartz M, Skovby F. Psychological and social impact of carrier screening for cystic fibrosis among pregnant woman-a pilot study. Clin Genet 1996;49:200-5.
9. Bekker H, Denniss G, Modell M, Bobrow M, Marteau T. The impact of population based screening for carriers of cystic fibrosis. J Med Genet 1994;31:364-8.
10. Decruyenaere M, Evers-Kiebooms G, Boogaerts A, et al. Psychological functioning before predictive testing for Huntington’s disease: the role of the parental disease, risk perception, and subjective proximity of the disease. J Med Genet 1999;36:897-905.
11. Wiggins S, Whyte P, Huggins M, Adam S, Theilmann J, Bloch M, Shep Schechter MT, Hayden MR. The psychological consequences of predictive testing for Huntington’s disease: Canadian Collaborative Study of Predictive Testing. N Engl J Med 1992;327:1401-5.
12. Codori AM, Brandt J. Psychological costs and benefits of predictive testing for Huntington’s disease. Am J Med Genet 1994;54:174-84.
13. Bloch M, Adam S, Wiggins S, Huggins M, Hayden MR. Predictive testing for Huntington disease in Canada: the experience of those receiving an increased risk. Am J Med Genet 1992;42:499-507.
14. Meissen GJ, Mastromauro CA, Kiely DK, McNamara DS, Myers RH. Understanding the decision to take the predictive test for Huntington disease. Am J Med Genet 1991;39:404-10.
15. Lawson K, Wiggins S, Green T, Adam S, Bloch M, Hayden MR. Adverse psychological events occurring in the first year after predictive testing for Huntington’s disease: the Canadian Collaborative Study Predictive Testing. J Med Genet 1996;33:856-62.
16. Decruyenaere M, Evers-Kiebooms G, Boogaerts A, et al. Prediction of psychological functioning one year after the predictive test for Huntington’s disease and impact of the test result on reproductive decision making. J Med Genet 1996;33:737-43.
17. Codori AM, Slavney PR, Young C, Miglioretti DL, Brandt J. Predictors of psychological adjustment to genetic testing for Huntington’s disease. Health Psychol 1997;161:36-50.
18. Goel V, Glazier R, Summers A, Holzapfel S. Psychological outcomes following maternal serum screening: a cohort study. CMAJ 1998;159:651-6.
19. Kerbel D, Glazier R, Holzapfel S, Yeung M, Lofsky S. Adverse effects of screening for gestational diabetes: a prospect cohort study in Toronto, Canada. J Med Screen 1997;4:128-32.
20. Gustafsson O, Theorell T, Normin U, Perski A, Ohstrom M, Nyman C. Psychological reactions in men screened for prostate cancer. Br J Urol 1995;75:631-61.
21. Ellman R, Angeli N, Christians A, Moss S, Chamberlain J, Maguire P. Psychiatric morbidity associated with screening for breast cancer. Br J Cancer 1989;60:781-4.
22. Gram IT, Lund E, Slenker SE. Quality of life following a false positive mammogram. Br J Cancer 1990;62:1018-22.
23. Rimer BK, Bluman LG. The psychosocial consequences of mammography. J Natl Cancer Inst Monogr 1997;22:131-8.
24. Lerman C, Seay J, Balshem A, Audrain J. Interest in genetic testing among first-degree relatives of breast cancer patients. Am J Med Genet 1995;57:385-92.
25. Croyle RT, Smith KR, Botkin JR, Baty B, Nash J. Psychological responses to BRCA1 mutation testing: preliminary findings. Health Psychol 1997;16:63-72.
26. Lerman C, Schwartz MD, Lin TH, Hughes C, Narod S, Lynch HT. The influence of psychological distress on use of genetic testing cancer risk. J Consult Clin Psychol 1997;65:414-20.
27. Smith KR, West JA, Croyle RT, Botkin JR. Familial context of genetic testing for cancer susceptibility: moderating effect of siblings’ test results on psychological distress one to two weeks after BRCA 1 mutation testing. Epidemiol Biomarkers Prev 1999;8:385-92.
28. Wardle FJ, Collins W, Pernet AL, Whitehead MI, Bourne TH, Campbell S. Psychological impact of screening for familial ovarian cancer. J Natl Cancer Inst 1993;85:653-7.
29. Lerman C, Miller SM, Scarborough R, Hanjani P, Nolte S, Smith D. Adverse psychologic consequences of positive cytologic cervical screening. Am J Obstet Gynecl 1991;165:658-22.
30. Codori AM, Petersen GM, Boyd PA, Brandt J, Giardiello FM. Genetic testing for cancer in children: short-term psychological effect. Arch Pediatr Adolesc Med 1996;150:1131-8.
31. Mant D, Fitzpatrick R, Hogg A, et al. Experiences of patients with false positive results from colorectal cancer screening. Br J Gen Pract 1990;40:423-5.
32. Lerman CE, Rimer BK. Psychosocial impact of cancer screening. Oncology 1993;7:67-72,75,79.
33. McQuellon RP, Wells M, Hoffman S, et al. Reducing distress in cancer patients with an orientation program. Psychooncology 1998;7:207-17.
34. Wardle J, Pope R. The psychological costs of screening for cancer. J Psychosom Res 1992;36:609-24.
35. Rastam L, Frick JO, Gullberg B. Work absenteeism in men who are labeled hypercholesterolaemic in screening. Eur Heart J 1991;12:1316-20.
36. Irvine MJ, Logan AG. Is knowing your cholesterol number harmful? J Clin Epidemiol 1994;47:131-45.
37. Connelly J, Cooper J, Mann A, Meade TW. The psychological impact of screening for risk of coronary heart disease in primary care settings. J Cardiovasc Risk 1998;5:185-91.
38. Christensen B. Psychological reactions to information about risk of ischaemic heart disease in general practice. Scand J Prim Health Care 1995;13:164-7.
39. Marteau TM, Kinmonth AL, Thompson S, Pyke S. The psychological impact of cardiovascular screening and intervention in primary care: a problem of false reassurance? British Family Heart Study Group. Br J Gen Pract 1996;46:577-82.
40. Horowitz MJ, Simon N, Holden M, et al. The stressful impact of news of risk for premature heart disease. Psychosom Med 1983;45:31-40.
41. Meland E, Laerum E, Maeland JG. Life style intervention in general practice: effects on psychological well-being and patient satisfaction. Qual Life Res 1996;5:348-54.
42. Stoate HG. Can health screening damage your health? J R Coll Gen Pract 1989;39:193-5.
43. DudokdeWit AC, Tibben A, Duivenvoorden HJ, Niermeijer MF, Passchier J. Predicting adaptation to presymptomatic DNA testing for late ovarian disorders: who will experience distress? Rotterdam Leiden Gen Workgroup. J Med Genet 1998;35:745-54.
44. Shaw C, Abrams, Marteau TM. Psychological impact of predicting individuals’ risks of illness: a systematic review. Soc Sci Med 1999;49:1571-98.-
1. Miller AB. The ethics, the risks and the benefits of screening. Biomed Pharmacother 1988;42:439-42.
2. Tuohey JF. Balancing benefit and burden: merely avoiding harm does not carry out the intent of the Hippocratic oath. Health Prog 1989;70:77-9.
3. US Preventive Services Task Force. Guide to clinical preventive services. 2nd ed. Baltimore, Md: Williams & Wilkins; 1996;lxxv-lxxvi.
4. Bowman MA, Dignan M, Crandall S, Baier M. Changes in functional status related to health maintenance visits to family physicians. J Fam Pract 2000;49:428-33.
5. Mold JW, Hamm R, Jafri B. The effect of labeling on perceived ability to recover from acute illnesses and injuries. J Fam Pract 2000;49:437-40.
6. Shaughnessy AF, Cincotta JA, Adelman A. Family practice patients’ attitudes toward firearm safety as a preventive medicine issue: a HARNET Study: Harrisburg Area Research Network. J Am Board Fam Pract 1999;12:354-9.
7. Mennie ME, Compton ME, Gilfillan A, et al. Prenatal screening for cystic fibrosis: psychological effects on carriers and their partners. J Med Genet 1993;30:543-8.
8. Clausen H, Brandt NJ, Schwartz M, Skovby F. Psychological and social impact of carrier screening for cystic fibrosis among pregnant woman-a pilot study. Clin Genet 1996;49:200-5.
9. Bekker H, Denniss G, Modell M, Bobrow M, Marteau T. The impact of population based screening for carriers of cystic fibrosis. J Med Genet 1994;31:364-8.
10. Decruyenaere M, Evers-Kiebooms G, Boogaerts A, et al. Psychological functioning before predictive testing for Huntington’s disease: the role of the parental disease, risk perception, and subjective proximity of the disease. J Med Genet 1999;36:897-905.
11. Wiggins S, Whyte P, Huggins M, Adam S, Theilmann J, Bloch M, Shep Schechter MT, Hayden MR. The psychological consequences of predictive testing for Huntington’s disease: Canadian Collaborative Study of Predictive Testing. N Engl J Med 1992;327:1401-5.
12. Codori AM, Brandt J. Psychological costs and benefits of predictive testing for Huntington’s disease. Am J Med Genet 1994;54:174-84.
13. Bloch M, Adam S, Wiggins S, Huggins M, Hayden MR. Predictive testing for Huntington disease in Canada: the experience of those receiving an increased risk. Am J Med Genet 1992;42:499-507.
14. Meissen GJ, Mastromauro CA, Kiely DK, McNamara DS, Myers RH. Understanding the decision to take the predictive test for Huntington disease. Am J Med Genet 1991;39:404-10.
15. Lawson K, Wiggins S, Green T, Adam S, Bloch M, Hayden MR. Adverse psychological events occurring in the first year after predictive testing for Huntington’s disease: the Canadian Collaborative Study Predictive Testing. J Med Genet 1996;33:856-62.
16. Decruyenaere M, Evers-Kiebooms G, Boogaerts A, et al. Prediction of psychological functioning one year after the predictive test for Huntington’s disease and impact of the test result on reproductive decision making. J Med Genet 1996;33:737-43.
17. Codori AM, Slavney PR, Young C, Miglioretti DL, Brandt J. Predictors of psychological adjustment to genetic testing for Huntington’s disease. Health Psychol 1997;161:36-50.
18. Goel V, Glazier R, Summers A, Holzapfel S. Psychological outcomes following maternal serum screening: a cohort study. CMAJ 1998;159:651-6.
19. Kerbel D, Glazier R, Holzapfel S, Yeung M, Lofsky S. Adverse effects of screening for gestational diabetes: a prospect cohort study in Toronto, Canada. J Med Screen 1997;4:128-32.
20. Gustafsson O, Theorell T, Normin U, Perski A, Ohstrom M, Nyman C. Psychological reactions in men screened for prostate cancer. Br J Urol 1995;75:631-61.
21. Ellman R, Angeli N, Christians A, Moss S, Chamberlain J, Maguire P. Psychiatric morbidity associated with screening for breast cancer. Br J Cancer 1989;60:781-4.
22. Gram IT, Lund E, Slenker SE. Quality of life following a false positive mammogram. Br J Cancer 1990;62:1018-22.
23. Rimer BK, Bluman LG. The psychosocial consequences of mammography. J Natl Cancer Inst Monogr 1997;22:131-8.
24. Lerman C, Seay J, Balshem A, Audrain J. Interest in genetic testing among first-degree relatives of breast cancer patients. Am J Med Genet 1995;57:385-92.
25. Croyle RT, Smith KR, Botkin JR, Baty B, Nash J. Psychological responses to BRCA1 mutation testing: preliminary findings. Health Psychol 1997;16:63-72.
26. Lerman C, Schwartz MD, Lin TH, Hughes C, Narod S, Lynch HT. The influence of psychological distress on use of genetic testing cancer risk. J Consult Clin Psychol 1997;65:414-20.
27. Smith KR, West JA, Croyle RT, Botkin JR. Familial context of genetic testing for cancer susceptibility: moderating effect of siblings’ test results on psychological distress one to two weeks after BRCA 1 mutation testing. Epidemiol Biomarkers Prev 1999;8:385-92.
28. Wardle FJ, Collins W, Pernet AL, Whitehead MI, Bourne TH, Campbell S. Psychological impact of screening for familial ovarian cancer. J Natl Cancer Inst 1993;85:653-7.
29. Lerman C, Miller SM, Scarborough R, Hanjani P, Nolte S, Smith D. Adverse psychologic consequences of positive cytologic cervical screening. Am J Obstet Gynecl 1991;165:658-22.
30. Codori AM, Petersen GM, Boyd PA, Brandt J, Giardiello FM. Genetic testing for cancer in children: short-term psychological effect. Arch Pediatr Adolesc Med 1996;150:1131-8.
31. Mant D, Fitzpatrick R, Hogg A, et al. Experiences of patients with false positive results from colorectal cancer screening. Br J Gen Pract 1990;40:423-5.
32. Lerman CE, Rimer BK. Psychosocial impact of cancer screening. Oncology 1993;7:67-72,75,79.
33. McQuellon RP, Wells M, Hoffman S, et al. Reducing distress in cancer patients with an orientation program. Psychooncology 1998;7:207-17.
34. Wardle J, Pope R. The psychological costs of screening for cancer. J Psychosom Res 1992;36:609-24.
35. Rastam L, Frick JO, Gullberg B. Work absenteeism in men who are labeled hypercholesterolaemic in screening. Eur Heart J 1991;12:1316-20.
36. Irvine MJ, Logan AG. Is knowing your cholesterol number harmful? J Clin Epidemiol 1994;47:131-45.
37. Connelly J, Cooper J, Mann A, Meade TW. The psychological impact of screening for risk of coronary heart disease in primary care settings. J Cardiovasc Risk 1998;5:185-91.
38. Christensen B. Psychological reactions to information about risk of ischaemic heart disease in general practice. Scand J Prim Health Care 1995;13:164-7.
39. Marteau TM, Kinmonth AL, Thompson S, Pyke S. The psychological impact of cardiovascular screening and intervention in primary care: a problem of false reassurance? British Family Heart Study Group. Br J Gen Pract 1996;46:577-82.
40. Horowitz MJ, Simon N, Holden M, et al. The stressful impact of news of risk for premature heart disease. Psychosom Med 1983;45:31-40.
41. Meland E, Laerum E, Maeland JG. Life style intervention in general practice: effects on psychological well-being and patient satisfaction. Qual Life Res 1996;5:348-54.
42. Stoate HG. Can health screening damage your health? J R Coll Gen Pract 1989;39:193-5.
43. DudokdeWit AC, Tibben A, Duivenvoorden HJ, Niermeijer MF, Passchier J. Predicting adaptation to presymptomatic DNA testing for late ovarian disorders: who will experience distress? Rotterdam Leiden Gen Workgroup. J Med Genet 1998;35:745-54.
44. Shaw C, Abrams, Marteau TM. Psychological impact of predicting individuals’ risks of illness: a systematic review. Soc Sci Med 1999;49:1571-98.-