The May 31 British Medical Journal  focused on the relationship between
physicians and drug companies. One of the aspects of this relationship
reviewed was the frequency of pharmaceutical company rep visits to
physicians. How do you think weekly visits from a pharmaceutical company rep
affect physicians' prescribing habits of that company's drugs?
http://www.medscape.com/px/instantpollservlet/result?PollID=821&WebLogicSess
ion=PuYKEDKsbSQ5OzwI2ETVvpKRz7TdAAf19360w2Z5RbARpCpv6vFK|-356169868323148936
8/184161392/6/7001/7001/7002/7002/7001/-1

Increases prescribing.   78%  (1045)
Decreases prescribing.   2%  (38)
No effect on prescribing.   18%  (246)
Total Responses: 1329
Poll conducted 31-May-2003 - 08-Jun-2003

Related Medscape news article
http://www.medscape.com/viewarticle/456554





BMJ: Pharmaceutical Industry-Physician "Entanglement" Affects Research, Care


Laurie Barclay, MD


June 3, 2003 - A special issue of the British Medical Journal explores the
"entangled" relationship between pharmaceutical companies and physicians,
reporting that industry-supported trials are biased toward the drugs for
which the companies seek marketing approval, saying industry "largesse" is
undermining clinical decision-making, and suggesting that doctors share the
blame if they don't wean themselves from industry influence.

Systematic reviews in the May 30 issue conclude that there is selective
reporting from industry-supported studies used to support new drug
applications, and the reviews discuss the effect of industry sponsorship on
research outcomes and study balance. A third report ties regular physician
contact with drug company representatives to unnecessary prescribing.
Finally, two commentaries discuss efforts to promote the "disentanglement"
of physicians and industry.

Industry representatives quoted in the BMJ reports and interviewed by
Medscape argue that pharmaceutical companies have a valid role to play in
educating physicians and point to a year-old, voluntary industry code of
conduct that bars many once-common marketing practices. They also argue that
government regulators, at least in the U.S., closely watch for evidence of
bias in the research underlying the drug approval process.

In the issue's lead editorial, BMJ Editor Richard Smith and Deputy Editor
Kamran Abbasi say they're not anti-industry. Virtually all new drugs
developed in the past 60 years - "drugs that have transformed medicine" -
were developed or made by pharmaceutical firms, they note, and their own
employer gets "substantial net income" from the industry. They also agree
that "it takes two to entangle.

"Doctors...are perhaps more to blame in coming to depend on drug company
largesse," they say. "Doctors and drug companies must work together, but
doctors do not need to be banqueted, transported in luxury, put up in the
best hotels, and educated by drug companies. The result is bias in the
decisions made about patient care."

Nor are medical journals necessarily exempt from industry influence, they
argue. "Journals are caught between publishing the most relevant and valid
research and being used as vehicles for drug company propaganda," they note.

Because publication of research findings occurs relatively late in the
process of study design, execution, data analysis, and interpretation,
safeguards against undue corporate influence on trials planning is
essential, the editors write. They cite two reviews in the theme issue
delineating potential bias in published trials.

One report, a review of 30 studies, based on a MEDLINE search from January
1966 to December 2002 and an EMBASE search from January 1980 to December
2002, found that trials sponsored by a pharmaceutical company were four
times more likely to show positive results for that company's drug than were
studies funded by other supporters (odds ratio, 4.05; 95% confidence
interval, 2.98 - 5.51). The study, by Joel Lexchin, MD, associate professor
of health policy and management at York University in Toronto, Ontario,
Canada, and colleagues, also found that company-funded research is less
likely to be published than research funded by other sources. But none of
the 13 studies that analyzed methods found industry-funded studies of poorer
quality than others.

"The bias that we see in studies sponsored by pharmaceutical companies is
not confined to any single group of drugs or diseases, and it has taken
place for over two decades," Dr. Lexchin told Medscape. "From my point of
view, these findings are not very surprising, because the drug companies
would have many problems if they had negative trials for their products and
if these trials were published."

"It's not that the drug companies deliberately deceive, but some decisions
they make regarding study design do tend to create bias," Dr. Lexchin says,
explaining that one potential source of bias is the choice of comparator, or
the comparison for the study drug. "Of course, these potential mechanisms
are just my hypothesis - you can't really prove it." Testing the drug
against placebo rather than against another active drug enhances the
likelihood of getting a positive result, Dr. Lexchin noted. Using too high a
dose for the comparison drug could lead to more adverse events while using
too low a dose could make the comparator look less effective than the test
drug.

Alan Goldhammer, PhD, associate vice president of regulatory affairs for the
Pharmaceutical Research and Manufacturers of America (PhRMA), the U.S.
industry's Washington, D.C.-based trade group, said in an interview that any
arguments about bias, at least from a U.S. perspective, "call into question
the role of the FDA [Food and Drug Administration], which is supposed to be
an unbiased regulatory agency.

"Regarding the allegation that drug companies choose comparators to be
favorable to their product, it's up to the FDA to say that additional or
different comparators are needed. So there are many checks and balances
here," Dr. Goldhammer said.

However, Dr. Smith points out in a separate article that medical journals
and pharmaceutical companies are "uneasy bedfellows," and that as long as
journals gain financially from publishing industry-sponsored studies,
negative trials are less likely to be published than positive ones.
Additionally, he says, "if the sponsors controlled publication and didn't
like the results, the papers won't be sent to these journals for
publication."

To counteract any potential bias from nonpublication of negative studies,
Dr. Lexchin's group proposes a registry of all trials. That way, they say,
when authors of reviews look at published reports, they would also know
about other, still-unpublished trials.

The author of another review in the theme issue, Hans Melander, PhLic, a
senior biostatistician with Sweden's Medical Products Agency, agreed that
anyone making a decision about drug treatment should not just rely on
published data. Dr. Melander is the lead author of a review of 42 studies
submitted to the agency to secure marketing approval for five selective
serotonin reuptake inhibitors. Comparing these studies with those actually
published between 1983 and 1999, the authors identified three potential
sources of bias: duplicate publication, selective publication, and selective
reporting.

Examples of duplicate publication included 21 studies reported in at least
two publications each, and three studies reported in five publications.
Studies showing significant benefits of a drug were published more often
than studies with insignificant or unfavorable results, the review found.
Many articles ignored the results of intention-to-treat analyses and
reported only the more favorable per-protocol analyses, Dr. Melander said.
However, he told Medscape, such publication bias is not a problem in drug
approval because regulatory agencies have access to all studies and all
alternative analyses and also can perform their own analyses.

Dr. Goldhammer said he didn't see how Dr. Melander's analysis applied in the
U.S., "where all clinical trials are reviewed by the FDA.

"Drug companies can promote their products based only on what the FDA allows
on the drug label," he added. "If there is a claim of superiority to another
drug, that data has to be generated and submitted to the FDA for review."

But while regulators may look at all data, physicians may rely on what's
published. Acknowledging that his study may not necessarily be generalizable
to all drugs, Dr. Melander urges physicians to seek out independent sources
of drug information, such as that available on the FDA Web site (Summary
Basis of Approval) and the European Agency for the Evaluation of Medicinal
Products (EMEA) Web site (European Public Assessment Report), as well as on
the Web sites of some national European agencies.

Dr. Lexchin points out that journal editors also have a responsibility to
ensure that study funding and potential conflicts of interest - from any
source - are declared. "Government-funded studies may have biases too; for
example, their bias might be to show that the least expensive drug for a
given indication is as good as the most expensive," he says. "If an article
doesn't state the source of funding, it should be regarded more skeptically
than those that do report it."

One information source not likely to be unbiased, however, is the industry
representative, found a systematic review by Christopher Watkins, MB, BS,
PhD, FRCGP, a general practitioner with the Backwell and Nailsea Medical
Group in Bristol, U.K.

"[Among] British general practitioners, high levels of contact with drug
industry representatives are associated with factors that indicate
professional isolation, a lack of involvement with training future general
practitioners, and a preference for educational support provided by the drug
industry," Dr. Watkins told Medscape. "These characteristics provide a major
challenge to those who wish to develop acceptable educational
interventions."

In his study of more than 1,000 general practitioners randomly selected from
200 practices in England, Dr. Watkins found that those "detailed" by drug
industry representatives at least once weekly were more likely to express
views leading to unnecessary prescribing, as indicated by a set of component
characteristics outlined in the study. These included greater willingness to
prescribe new drugs, acquiescence to patients' requests to prescribe drugs
not clinically indicated, dissatisfaction with consultations ending in
advice only, and "receptiveness to drug company advertisements and
promotional literature."

"High levels of contact with drug industry representatives is also
associated with general practitioner attitudes and behaviors that discourage
critical attitudes towards prescribing practice, encourage unrealistic
healthcare-seeking behavior in patients and thus increase the workload of
[clinicians]," Dr. Watkins said.

He encourages physicians to be aware of these influences and to examine them
critically to facilitate cost-effective prescribing. Future research, he
argued, should focus on alternative, more appropriate educational
interventions for those clinicians who now rely heavily on drug industry
representatives.

Ray Moynihan, a journalist in Washington, D.C., and a guest editor for the
BMJ special issue, agreed, telling Medscape that "the challenge facing
physicians is how to get quality, unbiased information about drugs quickly."
Company representatives are not that source, he argued. A better approach,
he said, might be to have "academic detailers" sponsored by public funding
who essentially do what industry representatives do, without any financial
incentive to promote a particular product. The U.K. has Pharmacy Advisors to
fulfill this function, and Australia has the National Prescribing Service.
In the U.S., Mr. Moynihan acknowledges, such programs "are in their
infancy."

He also argues that pharmaceutical companies' efforts to influence
physicians include supporting hundreds of thousands of continuing medical
education (CME) conferences and other events annually. Some associations and
academic centers are now declining or considering saying no to such support,
as well as contemplating closing the door to pharmaceutical representatives
out of concern about efforts to inappropriately influence physicians or
students.

PhRMA representatives noted that the industry, concerned about some of the
same issues, implemented a voluntary, self-regulatory code last year that
explicitly outlined the proper - and improper - ways industry
representatives could interact with physicians. The PhRMA code, one of a
number of new or proposed regulatory initiatives aimed at the industry,
rejects as improper several once-common perks - including travel and
entertainment - that had more to do with marketing than education or
scientific discussion.

John Kelly, MD, PhRMA's senior vice president for scientific and regulatory
affairs, was quoted in one of the BMJ articles as saying that the new code
benefits patients. He also told the BMJ that numerous organizations
representing practicing physicians continue to acknowledge the important
role industry plays in underwriting educational activities for physicians.
Supported CME also benefits patients, Dr. Kelly told the BMJ, because it
facilitates physicians' access to the "best available information."

However, several of the BMJ articles express concern that patients'
interests may actually be compromised by industry involvement. Drs. Abbasi
and Smith note that drug companies often fund patient organizations and
public relations companies but that the extent of that support is not always
disclosed.

None of the reviews or studies in the BMJ theme issue was supported by
industry or other interest groups. Drs. Lexchin, Melander, and Watkins
reported no pertinent financial conflicts of interest. Mr. Moynihan is an
independent journalist.

BMJ. 2003;326:1167-1170, 1171-1173, 1178-1179, 1189-1196, 1208-1210


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