Psychiatric Times. Vol. 27 No. 5

Undue Pharmaceutical Influence on Psychiatric Practice

Steps That Can Reduce the Ethical Risk

By Lisa Cosgrove, PhD and Harold J. Bursztajn, MD | May 18, 2010

Dr Cosgrove is associate professor and clinical psychologist and mental health graduate program director at the University of Massachusetts in Boston. Dr Bursztajn is cofounder of the Program in Psychiatry and the Law at the Beth Israel Deaconess Hospital Department of Psychiatry of Harvard Medical School, Boston. Dr Cosgrove reports no conflicts of interest concerning the subject matter of this article. Dr Bursztajn reports that he has been retained by both plaintiff and defense attorneys to serve as a consultant and testifying expert in pharmaceutical and medical devise liability lawsuits.

Within the past few years, increasing concerns have arisen about the ways in which corporate sponsorship of clinical trials and continuing medical education activities may bias the information that is published and disseminated about the benefits and risks of medications. ^1,2Questions have also been raised about the extent of industry influence on the American Psychiatric Association’s diagnostic and treatment guidelines—namely, its DSM and Clinical Practice Guidelines.^3,4

Clinicians are not the only ones concerned about the effect of financial conflicts of interest on health care. As controversy over the current revision of DSM has spread to the popular media, patients may also have questions—regardless of whether they articulate them.

Clearly, there exists the potential for bias and misinformation in an industry-dominated climate. However, a psychiatrist’s treatment of patients need not be undermined by public controversy over the actions of corporations or professional organizations.

This article explores some of the ethical dilemmas that can arise in today’s challenging climate. In addition, psychiatrists’ responses to the growing distrust of patients are discussed.

Randomized clinical controlled trials

Randomized clinical trials are described as the gold standard for evaluating the efficacy and safety of medications. However, this gold standard is sometimes compromised because of inadequate methodological design and outcome measures; use of effect sizes that are not clinically meaningful; failure to report adverse effects; and violation of equipoise, which lead to the approval of “me-too” drugs that are not safer, less expensive, or more effective than medications already on the market.^5-8 The brief duration of some clinical trials (often 6 to 8 weeks) does not permit sound judgments about long-term efficacy and safety. Industry sponsorship tends to be associated with proindustry conclusions, even when those conclusions are not necessarily warranted^.5,6 Thus, convergent validity, ie, the use of different methods, including challenge/dechallenge case reports, is vital in considering pharmaceutical safety.

Physicians employed by industry as clinical trial and safety directors have an obligation—per universal principles of medical ethics as well as the AMA code of ethics—to design, implement, and report clinical trials in a scientifically responsible manner.^9,10 Nonetheless, the actions of some pharmaceutical companies have raised the question about whether the benefits of antidepressants and atypical antipsychotics are overemphasized and the risks underreported. One study of clinical trials of psychiatric medications found that “among the 162 randomized, double-blind, placebo-controlled studies examined, those that reported conflict of interest were 4.9 times more likely to report positive results.”¹¹

Antidepressants and atypical antipsychotics

A recently published meta-analysis of the efficacy of antidepressants found that “the magnitude of benefit of antidepressant medication compared with placebo increases with severity of depression symptoms and may be minimal or nonexistent, on average, in patients with mild or moderate symptoms.”¹² A research team that previously conducted a meta-analysis drew an even stronger conclusion: “the relationship between initial severity and antidepressant efficacy is attributable to decreased responsiveness to placebo among very depressed patients rather than increased responsiveness to medication [authors’ italics].”¹³ Moreover, pharmaceutical manufacturers do not have an incentive to ask whether the drugs they produce may have adverse effects.¹⁴

Similarly, the assumed superiority of atypical antipsychotics has been called into question. Several large multicenter studies in both the United States and the United Kingdom, as well as meta-analyses, have raised questions about the validity of differentiating between typical and atypical antipsychotics because no “differences in quality of life or effectiveness measures” between the 2 classes of drugs were found.¹⁵ Indeed, there is growing evidence that atypical antidepressants and antipsychotics are not advantageous for many patients (although they are properly prescribed for some), and there is increasing evidence of the persistence of adverse effects (eg, sexual dysfunction, type 2 diabetes mellitus) even after the medications are discontinued. The fact that prescription patterns have not changed reflects not only a triumph of marketing but also the strength of decision-making biases.^15,16

CHECKPOINTS

■ Clinicians are not the only ones concerned about the effect of financial conflicts of interest on health care—patients may also have questions, regardless of whether they articulate them.

■ It is in patients’ and clinicians’ best interest to maintain a healthy dose of skepticism when reviewing any data on the efficacy and safety of
psychotropic medications, however prestigious the source.

■ Practitioners who read and later recall guidelines typically remember the general recommendations but forget the detailed exceptions and qualifications—indications and benefits are more likely to be remembered than warnings and contraindications buried in the adverse events section.

DSM and Clinical Practice Guidelines are not immune to industry influence

DSM is often mischaracterized as the bible of psychiatric disorders because of its enormous influence on clinical practice. As with previous editions of DSM, the proposed revisions for DSM5 give little attention to adverse effects. Only 2 of more than 700 pages of text of the main body of DSM-IV-TR deal with diagnosing adverse effects of psychotropic medications, and there the focus is on movement disorders. Neuroleptic malignant syndrome is given short shrift (1 paragraph). A discussion of life-threatening adverse effects such as diabetes and other metabolic conditions is entirely absent. A review of the recently proposed changes to DSM (www.dsm5.org) indicates that these omissions will remain in the next edition. Approximately 68% of the DSM5 task force report having ties to the pharmaceutical industry.¹⁷ This represents an increase of 20% over the proportion of DSM-IV task force members with such ties.^17,18

Clinical Practice Guidelines, which are used by primary care physicians as well as mental health clinicians, exert enormous influence on psychiatric treatment. It is thus imperative that the recommendations be balanced and accurate, and that they give adequate consideration to informed consent, alternatives to medications, and information about when to discontinue medications. However, all of the authors of the Clinical Practice Guidelines for bipolar disorder, for example, had financial relationships with companies whose drugs were identified as “first-line pharmacological treatment.”³ Not surprisingly, there is little discussion of how to inform patients of the risks and benefits of medications, when to discontinue medications, or how to monitor patients for withdrawal symptoms in the Clinical Practice Guidelines.

Deeper implications for psychiatric practice

People being treated for serious mental illness are often highly vulnerable to distrust. The fear of psychosis and the hopelessness and helplessness of severe depression can diminish a patient’s ability to weigh treatment risks, benefits, and alternatives. Such challenges do not mean that patients cannot navigate complex decision-making processes and that psychiatrists must resort to a paternalistic model of care.^19,20 Patients who believe that their prescribing clinician has their best interests at heart are better able to engage in shared decision making. A therapeutic alliance grounded in trust is essential in bringing strength and hope to the lives of individuals with psychiatric disabilities. When a patient has been informed about the potential adverse effects of a medication, there is a better chance that he or she will trust the clinician, will adhere to the medication regimen, and will be receptive to other treatment trials than will a patient for whom a bad outcome is a devastating surprise.

Beyond the biases that influence the formulation of treatment guidelines, practitioners who read and later recall those guidelines typically remember the general recommendations but forget the detailed exceptions and qualifications.²¹ Warnings and contraindications buried in the adverse events section of the labeling of a pharmaceutical product are not likely to be as well-remembered as the indications and benefits that are prominently noted. The consequences of automated thinking and the irrational persistence in belief may be reinforced by delays in disclosing adverse effects of medications.^21,22 Once clinicians have internalized the mindset that a particular drug is the treatment of choice for a particular condition, the automatic prescribing habit sets in and becomes difficult to dislodge. As a result, a pharmaceutical company that engages in such tactics of habituation gains an unfair competitive advantage over a competitor that makes full and timely disclosures of adverse findings.

Recommendations

Although practicing evidence-based medicine can be a useful corrective to uncritical prescribing, it is no panacea. Unavoidably, we practice under conditions of uncertainty, where every patient exists in a unique life context, every patient-clinician relationship is in some ways unique, and the next clinical outcome cannot be known until it occurs.²³ Yet this very complexity, to which potential or real financial conflicts of interests contribute, presents an opportunity to enhance and strengthen the therapeutic alliance through a mix of clinical wisdom and humility.

The suggestions given in the Table were developed by soliciting feedback from individuals who represented a range of disciplines and perspectives. For example, some were social scientists who have publicly questioned the ethics of industry-funded research, while others were clinicians and academicians who received honoraria for talks sponsored by pharmaceutical companies, or who received funding for their research. Incorporating feedback from a wide variety of individuals—both critics of financial conflicts of interest and those with industry ties—may serve as a model for how professional orga-nizations such as the American Psychiatric Association can better manage collaborations between industry and academic institutions and medical schools. Specifically, the goal should be to achieve a meaningful system of checks and balances. Thus, rather than a ban on individuals with industry ties serving on panels of diagnostic and treatment guidelines, perhaps a more helpful solution would be to invite critics of industry to serve alongside individuals who have connections to pharmaceutical companies.

by Alto Strata | May 29, 2010 12:18 PM EDT

It is indeed unfortunate that, because of ethical compromises in research and clinical psychiatry, the clinician cannot trust the medical literature, even the Cochrane Database.

It's a problem of garbage in, garbage out. Reviews and meta-analyses of the literature, much of which is disguised promotional material for pharma marketing, can only result in a tautological result favoring pharma. Also, reviews and meta-analyses cannot take into account studies with negative findings that have been suppressed by pharmaceutical company sponsors and influence.

For example, although in the literature of antidepressant withdrawal syndrome it is found to be fairly frequent -- an incidence of at least 20% -- not a single case of antidepressant withdrawal syndrome is reported in studies of antidepressant efficacy, including the execrable STAR*D study, which switched thousands of patients on and off drugs.

In all these studies, even challenge-rechallenge reports, it is highly likely that some number of patients identified as "relapsed"after discontinuation of medication -- thereby "proving" antidepressant efficacy -- were in fact suffering from antidepressant withdrawal reactions.

(You may read thousands of patient reports of withdrawal syndrome on the Web site paxilprogress.org. Withdrawal syndrome can last months or even years.)

Indeed, any study that discusses a rate of relapse or "recurrence of depression" but does not provide statistics for antidepressant withdrawal reactions is suspect. Because of small sample size, even a few withdrawal cases misdiagnosed as relapse would throw evidence of efficacy into statistical insignificance.

This flaw affects ALL studies of antidepressant efficacy -- the ENTIRE history.

(One also wonders about the unreported frequency of adverse effects -- surely a reflection of a lack of efficacy -- among the very large number of dropouts in these trials and whether they suffered withdrawal symptoms.)

The short duration of almost all antidepressant efficacy studies probably vastly underestimates the prevalence of antidepressant withdrawal syndrome in actual practice, as doctors are encouraged to persuade patients to take antidepressants for much longer periods of time, likely enhancing the frequency and severity of withdrawal syndrome.

Even the recent study Am J Psychiatry. 2010 May 17, Baldessarini et al, Illness Risk Following Rapid Versus Gradual Discontinuation of Antidepressants. (which indicates simply discontinuing an antidepressant increases rate of relapse beyond unmedicated rates) misstates the issue, as it probably also counted prolonged withdrawal syndrome as relapse.

The study does conclude (as most studies on withdrawal syndrome do) "These findings have implications for both clinical management and the design and interpretation of clinical trials."

You can say that again.

by Alto Strata | May 28, 2010 4:49 PM EDT

"...As with previous editions of DSM, the proposed revisions for DSM5 give little attention to adverse effects. Only 2 of more than 700 pages of text of the main body of DSM-IV-TR deal with diagnosing adverse effects of psychotropic medications, and there the focus is on movement disorders. Neuroleptic malignant syndrome is given short shrift (1 paragraph). A discussion of life-threatening adverse effects such as diabetes and other metabolic conditions is entirely absent. A review of the recently proposed changes to DSM (www.dsm5.org) indicates that these omissions will remain in the next edition.,,"

To comment on the DSM revisions, write DSM@psych.org and the head of the subcommittee looking at including adverse effects:

Charles P. O'Brien, MD, PhD
Kenneth Appel Professor
Department of Psychiatry
University of Pennsylvania
obrien@mail.trc.upenn.edu

Psychiatrists with ethical concerns must speak up to reform psychiatry. God knows they won't listen to patients.

by Adele Framer | May 28, 2010 2:20 PM EDT

Unfortunately, the horse has been out of the barn for a long, long time, and extensive patient injury has resulted from psychiatry's compromised ethics.

Read Anatomy of an Epidemic by Robert Whitaker, and see paxilprogress.org, a non-commercial patient support site for withdrawal from all psychiatric drugs, not just Paxil. Patients support each other because this support cannot be found in medicine. There are thousands of heart-rending case histories of injury posted on the site. With about 10% of the adult US population taking these drugs, we can assume this is just the tip of the iceberg. Psychiatric drugs have made millions worse, not better.

As to informed consent, the myth of medications correcting a neurotransmitter balance has as much currency among clinicians as a general public educated by TV advertising. There is no evidence whatsoever that mood disorders are caused by a lack or imbalance of serotonin or any other neurotransmitter, and promulgating this myth -- a common practice of psychiatry -- makes a mockery of both informed consent and evidence-based medicine.

Aside from misrepresenting the issue of neurotransmitter balance -- which is nothing but a manipulation to persuade patients they need to be medicated -- doctors fail to inform patients about common side effects of antidepressants, such as sexual dysfunction, affecting at least 50% of patients, or withdrawal syndrome, both with an incidence of at least 20%. They fail to discuss non-drug treatment before risking medication and its side effects.

By what ethical standard do psychiatrists misrepresent drug safety and elide the discussion of side effects, precluding patients' being able to make informed decisions about their treatment? Is disenfranchising patients in the best interest of treating them? Does a doctor who does this deserve a patient's trust? Does he or she even deserve to practice medicine?

At its root, psychiatry believes the doctor knows the patient's mind better than the patient does. The psychiatrist has license to ignore the patient's subjective experience, even to complaints of adverse effects from medication -- the drugs can do no wrong. This is why side effects and adverse events are given short shrift in the DSM.

With this fundamental contempt for the patient, psychiatry may be the medical discipline least capable of dealing with human emotional issues. It is better thought of as a branch of pharmaceutical marketing and distribution rather than medicine.

All of this is part and parcel of the intellectual dishonesty, the eagerness to sell drugs, that pervades both research and clinical psychiatry and certainly the hocus-pocus of psychopharmacology. The other medical specialties are led by psychiatry in this and should resist it to save their credibility.

by Ron Pies | May 26, 2010 1:02 AM EDT

Very useful and important issues raised here, Prof. Cosgrove and Dr. Bursztajn--many thanks!

Ron Pies MD
Editor in Chief

Also in this Special Report

Introduction: Ethical Dilemmas Old and New

Undue Pharmaceutical Influence on Psychiatric Practice

Ethical Aspects of Self-Disclosure in Psychotherapy

Ethics, Psychiatry, and End-of-Life Issues

Ethics and Child and Adolescent Psychiatry

Psychiatry in the Era of Neuroethics

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Undue Pharmaceutical Influence on Psychiatric Practice

Steps That Can Reduce the Ethical Risk

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