Fwd: Hard to swallow

[Guest guest]

Fri, 28 Mar 2003 16:50:00 -0500

WC Douglass

Hard to swallow

 

Daily Dose

March 28, 2003

 

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A conspiracy of greed?

 

Everyone's blue nowadays, it seems. In the last 15 years,

the number of people seeking treatment for depression in the

U.S has nearly doubled -- now 25 million per year. That's

bad news -- but what's worse is that according to recent

research, 90% of these people left their doctors' offices

with a prescription for antidepressants.

 

What we're dealing with here is a two-part problem: First, a

dramatic rise in the incidence of depression; and second,

the increasing reliance on drugs as the preferred treatment

option. Of course, I've got some theories about why

depression is running rampant these days, but I'll have to

tell you about them in the next Daily Dose. What I want to

talk about now is one reason why prescription drugs have

become the treatment of choice -- and it's downright

frightening...

 

In these days of HMOs and group health plans, if you have

insurance, your health care is usually funneled through

a " primary care physician " (PCP) whose responsibility it is

to diagnose the problem and -- if he can't treat it -- to

refer you to a specialist. But in the case of depression,

instead of referring patients to qualified therapists, the

PCP often dashes off a prescription for a month's worth of

antidepressant drugs. Sure, I'm skeptical of psychotherapy,

but it beats harmful drugs -- and the vicious cycle of

dependency they bring, with no real hope of a lasting cure.

 

This " band-aiding " of depression symptoms could be doctors

brainwashed by drug company propaganda into believing

antidepressants are the best course of action. Or it could

be that these PCPs are directed by the insurance companies

to prescribe expensive, addictive drugs in place of other

therapies.

 

Neither reality is best for the patient, but one can be

blamed on ignorance -- and the other only on a conspiracy.

In either event, large forces with much to gain financially

are influencing our doctors toward treatments that may not

be the best course of action for you. Makes you wonder

exactly what the drug company/insurance industry

relationship is, doesn't it? It certainly doesn't seem to

revolve around your good health...

 

And that's enough to make anyone depressed.

 

(I'll have more to say about antidepressants in the next

Daily Dose, about what works and what's worthless.)

 

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Statin drugs cause mental " static "

 

I know I've mentioned cholesterol drugs a lot in the last

year or so, both in Real Health and in the Daily Dose. But

new research findings keep cropping up almost daily, it

seems, that tell us new things about these harmful patent

medications -- and their " benefits. "

 

For instance, research unveiled at last fall's meeting of

the American Heart Association revealed that a commonly

prescribed " statin " drug for lowering cholesterol might

actually impair patients' brain function -- even so far as

to affect their ability to perform everyday tasks, like

drive a car. The study pinpointed measurable decreases in

attention span and psychomotor reflex speed among the

subject group when compared to the un-medicated control

group...

 

But here's the really incriminating part: Those patients who

experienced the greatest decreases in blood cholesterol also

suffered the greatest levels of impairment! Interesting,

huh?

 

I mention these findings to you now because I know the

mainstream press will never pick up the story -- but also

because some medical authorities estimate that in the very

near future, half of the adult U.S. population could be

taking cholesterol-lowering medications. That's right -- if

conventional doctors and the " drug thugs " have their way,

every other one of us will be stumbling around in a statin

stupor! But what's not clear is whether the impairment is

caused by the drugs themselves -- or the lack of

cholesterol...

 

I suspect it's the latter. Why? Because low cholesterol

levels have been linked to numerous other health issues

directly related to the brain -- things like violent

behavior, depression, mood swings, stroke risk and other

problems. Maybe now, we should add " impaired brain

functioning " to that list.

 

I've said it before, and I'll say it again now: Unless your

cholesterol climbs over 300, forget about it -- even

the " ratio " of LDL to HDL that so many conventional doctors

make such a fuss about. For heart health, concentrate

instead on DHEA, testosterone (for both men and women), and

homocysteine levels. And be sure to supplement with plenty

of folic acid, B vitamins, and CoQ10, too...

 

Just leave the statin drugs alone -- unless you're suffering

from an excess of IQ or terminal euphoria.

 

It's not easy being blue,

 

William Campbell Douglass II, MD

 

 

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[Guest guest]

SSRI-Research , JustSayNo wrote:

Hard to Swallow

 

Read the ads and you'll think relief from the black cloud of

depression is

just a pill away. But if you consult the scientific record and look

at the

medical trials the pills have gone through, you'll see a much scarier

story.

 

http://www.washingtonian.com/health/hardtoswallow.html

 

By Thomas J. Moore

 

Thomas J. Moore is the author of four books about health and medical

care.

His book, Prescription for Disaster, (published by Simon & Schuster,

1998)

focuses on the risks of the most widely used prescription drugs.

 

 

" Prozac seemed to give social confidence to the habitually timid, to

make

the sensitive brash, to lend the introvert the social skills of a

salesman. "

 

So writes psychiatrist Peter Kramer in his book Listening to Prozac.

Such

glowing accounts have helped make antidepressants such as Prozac,

Paxil,

Zoloft, Effexor, and Serzone among the best-selling drugs in the

world.

 

Yet here, in similar language, is how Johns Hopkins psychiatrist Kay

Redfield Jamison describes an episode of mania in An Unquiet Mind, a

memoir

of her long battle with mental illness:

 

" Shyness goes, the right words and gestures are suddenly there, the

power to

captivate others a felt certainty. There are interests found in

uninteresting people. "

 

These statements are so strikingly alike because both describe a

serious

mental illness, no matter how attractive Kramer makes it sound.

During manic

episodes, the habitually timid may attack a police officer; armed

with new

social confidence, an introverted woman may brazenly solicit men in a

bar. A

serious episode of mania typically ends in a locked psychiatric ward.

 

In fact, according to their manufacturers, Prozac, Paxil, Zoloft,

Effexor,

Serzone, and other antidepressants may trigger mania, or less severe

hypomania.

 

Fortunately, mania is an infrequent side effect of drugs for

depression.

What is distressingly common, though, is the tendency of both doctors

and

patients to overestimate the benefits of these drugs while ignoring

their

risks.

 

How does the hype about antidepressants compare to the scientific

record?

 

The drugs are touted as effective for the vast majority of depressed

patients. Yet they routinely fail to produce a measurable benefit in

clinical testing.

 

Prozac especially is claimed to be relatively free of side effects.

Yet in

reports to the Food and Drug Administration, Prozac has been linked

to more

serious adverse reactions than any other drug in America over the past

decade. And other antidepressants are little safer.

 

Antidepressants are said to be non-habit-forming. Yet in the first

large

study, more than one out of three patients experienced withdrawal

effects.

 

The safety of antidepressants is supposedly proven by the fact that

they

have been taken by more than 20 million Americans. Yet virtually no

meaningful research has been conducted on their long-term risks.

 

The danger of suicide is widely cited as a reason to treat depression

with

these drugs. Yet there is no evidence that antidepressants prevent

suicide--and dark hints that they may even encourage it.

 

With antidepressants, side effects are more common than success

stories.

Here is what a patient named Greg had to say about Zoloft:

 

" Side effects? Just about all of them. The ones that stick around? Dry

mouth, some hot flashes. I still get unusual cases where I'll wake up

at

three in the morning sweating. I have drowsiness and difficulty

focusing for

the first five hours after taking a dosage. " (Greg's comments and

those of

some of the other patients quoted in this article were obtained

through the

Internet. To protect privacy, last names have been omitted.)

 

The fact is that antidepressant drugs are overrated by many consumers

and

doctors, overprescribed because of aggressive marketing, and among

the most

toxic drugs in widespread use as measured by the number, variety, and

severity of adverse effects.

 

What's more, millions of Americans who think they can testify to the

benefits of antidepressants are being misled by their own feelings.

Doctors,

if they rely on their clinical experience, are similarly deceived.

 

Why? Because in the treatment of depression, the placebo effect is

very

large. Scientific testing shows that roughly two out of three people

who

report a " marked " improvement on an antidepressant drug would have

done

equally well on a harmless placebo--and they wouldn't have to suffer

such

side effects as sexual dysfunction, anxiety, insomnia, sweating, and

nausea.

 

An objective appraisal of antidepressants would be easier if global

pharmaceutical companies didn't depend so heavily on their sales.

Take Eli

Lilly: Last year, Prozac accounted for about 30 percent of its total

sales

and probably an even larger share of its profits.

 

Like tobacco and beer companies, the pharmaceutical industry spends

more for

advertising and promotion than for manufacturing or research. This

means

billions are available to polish the image of products--and to combat

critics.

 

For the facts about antidepressants, the best place to look is the

Food and

Drug Administration. By law, drugs have to be extensively tested

before

being marketed. The tests are evaluated by FDA doctors, chemists, and

statisticians.

 

This article focuses on two of the newest drugs for depression,

Serzone and

Effexor, because--as new drugs--they ought to be tested to high

standards

and might offer advantages over Prozac, now in its tenth year. But

what does

the record say?

 

An examination of the risks and benefits of a drug must begin with a

look at

the medical problem it is intended to combat. Those who have not

personally

experienced major depression should not underestimate the severity of

the

disorder. Few afflictions are so capable of causing suffering. Here's

how

Charlotte Brontë described an episode of depression in her novel

Villette:

 

" Indescribably was I torn, racked, and oppressed in mind: Galled was

my

innermost spirit with an unutterable sense of despair about the

future.

Motive there was none why I should try to recover or wish to live;

and yet

quite unendurable was the pitiless and haughty voice in which Death

challenged me to engage his unknown terrors. "

 

Modern psychiatry has reduced Brontë's poetic account of a dark cloud

over

the human spirit into a dry list. A " major depressive episode " is

defined as

a period of two weeks or longer in which a person loses pleasure in

all or

almost all activities. To this may be added fatigue, a feeling of

worthlessness, inappropriate guilt, anxiety, difficulty sleeping or

excessive sleeping, indecisiveness, inability to concentrate, or

thoughts of

suicide. By the medical criteria, just one of these episodes

justifies a

diagnosis of " major depressive disorder. "

 

The number of people who suffer from this mood disorder has been

poorly

studied and is often exaggerated, either to sell drugs or to advance

depression to a more prominent position on the list of disorders

worthy of

media attention, aggressive medical treatment, and public funds.

 

In a survey of 18,000 people funded by the National Institutes of

Health,

1.5 percent of the population was suffering from major depression when

interviewed, and 4.5 percent had experienced major depression at some

point.

At any time, about 4 million people in the United States suffer from

the

disorder. Millions more suffer less-severe episodes, often in

connection

with bereavement, divorce, or other life stresses.

 

The oppression of the human spirit that is called depression may be

measured

by a numerical scale of symptoms that ranges from 0 to 52. Called the

Hamilton Depression, or Ham-D, scale, it consists of 17 scored items.

A

person with a Ham-D score of less than 6 is roughly normal. A Ham-D

score of

20 or higher indicates major depression.

 

The strength of this approach is that psychiatrists everywhere can

use the

same protocol to evaluate patients and ought to get at least similar

results. Under controlled conditions, raters agreed on diagnoses

about 80

percent of the time. The scale isn't perfect, but Ham-D is a

reasonably

precise tool for diagnosing depression and measuring improvement or

deterioration.

 

 

Hard to Swallow

 

Page 2 of 6

 

Given that major depression is a mood disorder involving great human

suffering, the next question is whether antidepressants relieve this

psychic

burden. Some answers come from patients who have taken them.

 

Jeanne describes " the wonderful world of Prozac. To me it felt like

laying

back in a bed of rose petals and staying there all day. "

 

Sean said, " My daughter was on Prozac for three months, and it made

her

worse. "

 

Pauolo said, " I have found Prozac to be extremely helpful. I feel

perfectly

normal for the first time in my life. "

 

Jane said, " It was as though the color had gone out of my

personality. Once

I came off, I became myself again. "

 

Select a few glowing stories, and Prozac sounds like a drug that

helps many

people. That is what Peter Kramer did in Listening to Prozac. Fill a

book

with horror stories, and most of its readers wouldn't touch an

antidepressant. Such anecdotes, in short, tell us little about

whether these

drugs work.

 

Reliably observing the effects of a drug on something as ephemeral and

variable as depressed mood requires the most rigorous rules that

science can

devise.

 

We have no laboratory tests to measure mood. Mood can be transformed

in an

instant, and even the most compassionate observer still can never

know what

another person truly feels. Many depressed people have learned to

fool their

associates, perhaps sometimes even themselves.

 

Finally, the appraisal of drug effects has long been contaminated by

our

need to believe there is something available to relieve our suffering,

reduce our pain, hasten our return to health.

 

Why in the name of health did so many people once consume foul-tasting

concoctions, deadly arsenic, or violent purgatives? Because for

centuries

doctors and patients so hoped for a cure that they thought they

observed

people getting better after treatment. Somewhere deep in the human

spirit

people want to believe in medication, and it takes all the objectivity

modern science can muster to separate hopes and wishes from genuine

drug

effects.

 

The procedure for testing a drug for depression is something like a

courtroom jury trial. It is a drama played out according to detailed

rules

that take years of training to master. Like a prosecutor, the

researchers

must declare in advance exactly what they expect to prove. Every

participant

must consent in writing. The judges are the medical and statistical

experts

at the FDA, as well as outside experts drawn from medical schools and

research centers. The official record may be thousands of pages long.

 

The clinical trials of the antidepressant drug Serzone serve as an

example.

To win approval to market Serzone, Bristol-Myers Squibb had to

conduct at

least two successful trials with humans. To do that, the company

contracted

with outside research doctors who oversaw the trials at various

clinics,

doctors' offices, and medical centers throughout the United States and

Canada. The rules can change between clinical trials but must be

identical

for every patient within each trial. In all, more than 3,000 patients

took

part in the testing of Serzone.

 

More money is at stake in these clinical trials than in all but the

very

largest courtroom cases. A drug that fails will mean tens of millions

of

dollars wasted; a big success can bring billions of dollars in

profits,

enough to sustain a global pharmaceutical giant for years.

 

With so much at stake--including human lives--a modest amount of

checking

and double-checking occurs. The way the system works can be seen in

the

Serzone clinical trial known as CN104-002.

 

It began with a group of similar patients who had been diagnosed with

major

depression and consented to join this experiment. It was important to

make

sure that healthy patients were not accidentally included. No drug

works

when given to people who don't have a medical problem needing

treatment. The

most extremely ill--those openly suicidal--also were excluded.

 

A drug-research institute in Southern California recruited 180

patients with

depression so serious that, on the average, the participants rated 24

on the

Ham-D.

 

At random, the patients were assigned to receive either Serzone or a

seemingly identical placebo. Except for a group of safety monitors,

no one

in the experiment was supposed to know which patients were given

Serzone and

which were given the placebo. Random chance is the fairest way of

selecting

a jury to take the drug while maintaining a nearly identical

untreated group

for comparison purposes.

 

The experiment continued for six weeks with investigators evaluating

every

patient on a weekly basis and scoring the results. Bristol-Myers

hoped to

find " marked improvement " among those treated with Serzone. This was

defined

as a 50-percent drop in the Ham-D depression score. Since the average

depression score was 24, the company was hoping most patients' scores

would

drop by 12 or 13 points over six weeks. Although six weeks seems

brief for a

drug likely to be given for months, it is at least long enough to

detect an

initial effect.

 

What results did Serzone achieve?

 

Six weeks after the Serzone trial began, there was no difference, in

statistical terms, between the patients treated with Serzone and

those given

the placebo. The average patient on Serzone improved, but so did those

getting a placebo. The placebo group improved by 11 points on the Ham-

D

scale, the Serzone patients by 12 points--a difference so small that

it

might have occurred by chance.

 

In testing results submitted to the FDA, Serzone failed to show a

clear

benefit in six of the eight clinical trials. Three more clinical

trials were

discontinued before results were available. In some cases FDA

evaluators

thought they saw an explanation for the lack of effect. In three of

the

failures, the FDA was persuaded that the dose was too low. Since even

a

promising drug will have no useful effect at the wrong dose, Serzone

was

tested further at a higher dose. One of these high-dose trials failed

by

everyone's evaluation, and two more were borderline. However, two

other

trials were declared a success.

 

If six Serzone trials failed or were inconclusive, what results did

the two

claimed successes achieve? In one " successful " trial the placebo

patients

showed a dramatic improvement. Their depression scores dropped 17

points in

six weeks. Serzone patients didn't do as well, with average scores

improving

14 points.

 

On this data, a rational patient would choose to take the placebo

rather

than the drug. But as analysts pored over the details, they spotted an

interesting fact.

 

Overall, 88 percent of patients in the trial had been recruited at

one large

center in Canada and the remainder in three smaller centers, also in

Canada.

The largest placebo effects had been observed in the patients at the

three

smaller centers. When the results of these three smaller centers were

excluded, the patients in the test appeared to benefit from Serzone.

 

Excluding results unfavorable to Serzone after the fact was like

conducting

a jury trial and, if no guilty verdict resulted, allowing the

prosecution to

remove the jurors with doubts. But even when the most unfavorable

results

were excluded, Serzone patients' depression scores improved by 13

points,

the placebo patients' by 12.

 

Yes, Serzone was now slightly ahead, but again this small difference

could

easily be explained by chance. How then could anyone claim Serzone was

effective?

 

It turns out there is another way to score the results. A problem that

plagues clinical trials for depression is that patients drop out in

large

numbers because of toxic side effects or for other reasons. In this

trial,

one-third of the patients had quit before the six-week period ended.

Under

alternative statistical rules, it was permissible to pretend that

those who

dropped out had continued to the end of the trial. The final results

included all the scores, even for those who had quit after one week.

 

Suppose, for example, that a Serzone patient had improved

dramatically at

the third-week examination but was hospitalized the next week for

severe

adverse effects. The three-week score showing a great benefit still

would be

included--and there would be no penalty for the participant's not

continuing

to the end.

 

This is using statistical adjustments to try to prove an effect that

was not

detected by direct scientific observation. What's more, it makes the

test an

unrealistic estimate of what will be achieved in actual use.

Antidepressants

are prescribed for months and sometimes years.

 

Nonetheless, with these more lenient scoring rules, and after

eliminating

the centers where the results were poor, Serzone appeared to have a

beneficial effect. Scores for patients taking the drug improved by 11

points, while the placebo patients improved by just 7 points.

 

Yet another factor needs to be considered.

 

One of the most common adverse effects of antidepressant drugs is to

make

anxiety and insomnia worse--or to add these problems to the symptoms

already

present.

 

To combat this expected adverse effect, the patients were allowed to

take a

sedative called chloral hydrate. This is certainly humane, but if a

depressed patient is suddenly sleeping better and freed of the

terrors of

the night, do we credit Serzone or the sleeping pills?

 

In the " successful " clinical trial of Serzone, not only were patients

allowed to take sleeping pills; 14 of them also took other drugs,

including

tranquilizers and other antidepressants. Could it have been the other

medication that accounted for the small effect claimed for Serzone?

 

The second Serzone trial said to be a success required an even more

drastic

statistical adjustment. A single investigator supervised the trial in

six

psychiatric practices and seven family practices, all on the East

Coast.

When the overall results were scored, the trial was once again a

failure.

However, while the patients recruited from the family-practice sites

appeared to benefit, those recruited from the psychiatric sites did

not. The

solution? Exclude the psychiatric patients.

 

At the core of the scientific method is the requirement to produce, by

direct empirical observation, a result that can be replicated. Yet

Bristol-Myers could not replicate the results even using the identical

protocol, supervised by the same investigator.

 

The results for the second drug--Effexor--were not much more

impressive.

Manufacturer Wyeth-Ayerst conducted three clinical trials under a

special

protocol that allowed the investigators to individualize the dose for

each

patient. In two out of three trials, Effexor still failed to produce a

benefit as measured by Ham-D scores at six weeks.

 

Once again the FDA allowed the rules to be changed after the fact to

allow

Effexor to squeeze through. It counted as successful a clinical trial

that

had shown a benefit at four weeks--but these apparent benefits had

disappeared by the sixth week. As it had with Serzone, the FDA

provided a

generous interpretation of its own rules to " prove " Effexor effective

in two

clinical trials.

 

I challenged the quality of the scientific evidence for both drugs in

an

interview with Thomas P. Laughren, an FDA medical doctor who, as the

team

leader for evaluating psychiatric drugs, had reviewed both Serzone and

Effexor.

 

While conceding that the effects of these drugs were " modest, "

Laughren

noted that the drugs had been evaluated by the FDA's own statistical

specialists and then reviewed by an advisory panel of psychiatrists

and

drug-testing experts. All concluded the drugs were effective, he said.

 

It is revealing to observe these independent experts in action. On

July 19,

1993, 11 members of the Psychopharmacologic Drugs Advisory Committee

met to

deliberate on the fate of Serzone. Paul Leber, a medical doctor and

director

of the FDA division that evaluated the drug, led the discussion.

 

Very few drugs are sent to the committee unless approval is considered

likely. Still, one would think that Serzone faced an uphill battle.

By the

simplest box score, it had failed in six of eight tries.

 

After the committee got a briefing on the clinical testing, Leber

asked,

" [Does] the evidence as a whole [show] the drug has the effect

claimed for

it? So that gives you great latitude in interpreting the entire data

set. "

 

These words were scarcely out of Leber's mouth when it looked like

Serzone

might be in trouble. The final decision to approve or reject Serzone

would

be made by Leber's boss, an FDA doctor, Robert Temple, whose title was

director of the Office of Drug Evaluation I. Temple seemed to want to

emphasize a strict standard.

 

" It needn't be mindless, " Temple told the committee. " The only

limitation is

that we generally expect replication. But that doesn't mean that if

you get

two studies out of four that work, it is okay. "

 

This sounds like the death knell for Serzone. By the FDA's rules,

Serzone

produced no measurable benefit six times.

 

But this did not prove a fatal flaw to the chairman of the advisory

committee, Carol Tamminga, a professor of psychiatry at the

University of

Maryland. She found a distinction between studies that

were " negative " and

those that " failed. "

 

" There is only one negative study in this data set as I read it, "

Tamminga

told the panel. " The other failed studies are where there was no

difference

defined between placebo and the active control. "

 

Tamminga was referring to the fact that in some trials Serzone was

also

compared with another, older antidepressant as well as to a placebo

and that

neither drug proved effective. In effect, she seems to have assumed

that if

Bristol-Myers had done the experiment properly, at least the older

drug

would have looked beneficial.

 

Dennis S. Charney, a professor of psychiatry of Yale University,

agreed with

Tamminga: " It is that data that leads me to say it is an effective

drug. But

I do worry about the large number of failed studies. "

 

Next, Regina Casper, a professor of psychiatry at Stanford

University, noted

the obvious. " We do not have overwhelmingly strong support for this

drug

being a strongly effective antidepressant, " she said.

 

As happens in many committee meetings, the discussion meandered. But

in the

end, all but one member of the advisory committee voted to declare

the drug

effective.

 

Still, some of these drug experts seemed nervous about what they had

done.

Robert Temple, the FDA doctor who would later approve Serzone, was

concerned

about new risks now being discovered about antidepressants on the

market,

especially their capacity to interact with other drugs and food.

 

" It is very daunting, " Temple said. " The more you look, the more you

discover. And the limits of what we are going to discover are not

nearly

over. "

 

Temple had reason to feel daunted. Once approved, the risks of drugs

may

continue undetected for decades. A dramatic example came four years

after

Temple made this comment in 1993. The diet drugs Pon-dimin and Redux

were

hastily withdrawn after the FDA found evidence that more than 30

percent of

the patients checked had evidence of damage to their heart valves.

Pondimin

was approved in 1973, but no one noticed the capacity of the drug to

injure

heart valves until someone looked 21 years later. As Temple said, the

more

you look, the more you discover.

 

But that concern prevailed for only an instant. Soon the onus was on

consumers.

 

Temple said, " It seems that consumers need to start rethinking that

there is

a pill for every ill and that they are all safe. We are starting to

understand that things are more complicated than we once thought. "

 

Tamminga, the chairman, agreed: " That would be a superb message. "

 

The real message the FDA and the experts were sending was that the

efficacy

standards for approving drugs for depression were remarkably low. A

drug

that had a marginal effect at best, and by strict rules no beneficial

effect

at all, was deemed acceptable for aggressive marketing to doctors and

patients. Serzone's repeated failures to achieve the expected

benefits would

not be included in the information disclosed to doctors.

 

I asked Bristol-Myers to comment on Serzone's efficacy and was

granted an

interview with Darlene Jody, a psychiatrist and senior medical

director for

central-nervous-system drugs. It was clear that we both were looking

at the

same clinical-trials data. " Two studies of Serzone were positive, "

she said,

" and two were supportive. "

 

Asked about excluding the results of some centers and getting

different

results from different measurement methods, she said, " In

psychotropic drugs

it is not uncommon for all drugs to have these types of exceptions. "

 

Just one or two individual trials do not represent the whole body of

scientific evidence, she said. " There is an accumulation of data to

demonstrate that the drug has a positive effect on treatment outcome. "

 

Jody also said that since FDA approval, Bristol-Myers had completed

six more

trials comparing Serzone to Paxil, Prozac, and Zoloft: " In not one of

these

trials is Serzone less efficacious, and it is possibly more

efficacious. "

 

Wyeth-Ayerst Laboratories responded to questions about Effexor with

somewhat

similar points. Richard Rudolph, a physician who is senior director of

clinical research for the company, said, " You need to understand that

in the

history of submissions for psychoactive drugs, generally sponsors

have had

to submit multiple trials to get two positive results. "

 

There are many reasons why clinical trials fail, Rudolph said. " There

is a

high placebo-response rate. The sample size is inadequate. The patient

population is insensitive to the effects of the drug. "

 

Effexor, he said, also had been compared to Prozac and other

antidepressants

since FDA approval and had demonstrated comparable effects.

 

What these company representatives are in effect saying is that

patients do

very well on placebos. They are saying the expected effects are so

small and

unpredictable that every drug company has to plan for frequent

failures.

Finally, they are saying that all antidepressants are roughly the

same in

effectiveness. This is likely true, but it means all the similar

drugs have

the same limited benefit.

 

If antidepressant drugs had no adverse effects, harmed no one, and

never

spoiled a morning, a day, or a life, then turning loose the mighty

marketing

engine of the drug industry on such meager evidence might be an

acceptable

risk. The drugs might help some people. And many would be comforted

when a

doctor they respected prescribed a pill to relieve their suffering.

As one

observer put it, " False hope is better than no hope. "

 

However, antidepressant drugs are notable for a variety of adverse

effects

from which a large fraction of patients suffer.

 

When the participants in Effexor's clinical trials visited the

clinic, their

symptoms of depression were not the only item evaluated. They also

answered

a long series of questions intended to identify symptoms that might

signal a

dangerous adverse effect. Periodically, they would have their blood

and

urine tested and their heartbeat monitored. These medical tests might

provide the first evidence that a drug was injuring the liver,

damaging the

kidneys, or interfering with the operations of the heart.

 

If the doctor discontinued the drug because of an adverse effect,

this would

be noted. If a patient failed to appear for a scheduled appointment,

an

inquiry is supposed to be made. During the testing of antidepressant

drugs,

a few patients do not appear for appointments because they have shot

themselves, hanged themselves, or died of an intentional overdose. It

is

from this testing data that the safety profile of a new drug emerges.

 

This scrutiny also can prevent a promising new drug from becoming the

victim

of a bum rap. For example, 23 percent of the patients taking Effexor

reported having headaches. So does Effexor cause head-aches? Probably

not:

23 percent of those on placebo also reported headaches. The profile of

adverse effects that emerges from such data will not be perfect, but

it will

be more accurate than anecdotes.

 

When Effexor patients were asked about nausea, a genuine side effect

did

emerge. Thirty-six percent of the Effexor patients reported being

nauseated,

compared with 9 percent of the placebo group. When asked about sexual

impotence, 5 percent of men taking Effexor reported that problem, but

none

of the placebo patients.

 

When placebo effects are subtracted, the most common side effects can

be

accurately mapped.

 

Effexor had harmful effects on patients' appetites and on their

digestive

tracts. At least 27 percent experienced nausea, 8 percent reported

constipation, and 9 percent lost their appetite so completely that

they were

classified as having anorexia.

 

Effexor also had many adverse effects on the heart. On the average it

made

hearts beat faster by three beats a minute. It also raised blood

pressure.

Over a year's time, the FDA estimates suggest that about 8 percent of

Effexor patients might require treatment for high blood pressure.

Effexor

raised blood pressure in many patients by more than the typical

blood-pressure drug lowers it.

 

Overall about 11 percent of men reported sexual problems related to

Effexor,

divided equally among those who reported outright impotence and those

who

experienced abnormal or painful ejaculation. Another 2 percent of

both sexes

reported decreased sex drive. None of the placebo patients reported

any of

these sexual problems.

 

It was in the very system to which Effexor was targeted--the central

nervous

system--that the most unpredictable adverse effects could be observed.

Effexor made about 14 percent of the people who took it sleepy or

sedated.

 

Here is one experience: " I am taking 150 mg. of Effexor, " Donna

said. " I

have recently started back to work, and I can hardly keep my eyes

open. I

find that around 10:30 AM or so I start to get so tired and have

minimal

concentration. "

 

While Effexor made one in seven people sleepy or sedated, it made an

even

larger number nervous, anxious, or unable to sleep. Overall, 8 percent

reported insomnia, 8 percent nervousness, and another 2 percent

anxiety. Ten

percent reported breaking into abnormal sweats, and 11 percent

experienced

dry mouth.

 

Serzone's adverse effects were roughly similar but included possible

disruption of higher mental functions. After adjusting for placebo,

from 1

to 5 percent of those testing Serzone reported one or more of these

symptoms: confusion, impaired memory, abnormal dreams, decreased

concentration, lack of coordination, psychomotor retardation, and

tremors.

But Serzone appeared relatively free of adverse effects on sexual

activity--a key marketing point for the drug.

 

How severe are these problems? To obtain relief from major

depression, many

people might tolerate a little difficulty falling asleep or a dry

mouth some

of the time. But in 19 percent of the Effexor patients the problems

were so

severe that the drug had to be discontinued before the six-week trial

ended.

By this measure, the demonstrated toxicity of Effexor is above

average for

antidepressants: 15 percent had to discontinue Prozac and Zoloft

because of

adverse reactions; 16 percent discontinued Serzone; and 20 percent,

Paxil.

(Wyeth-Ayrest said it expects to market a sustained release version of

Effexor that will have a better side-effects profile.)

 

A drug so toxic that nearly one in five has to stop therapy would not

seem

to be a chemical that can be released to the public with confidence

that it

will at least do no harm. Nor is such toxicity typical of drugs

generally.

For example, the cholesterol-lowering drug Zocor was tested among

2,223

people for more than five years, with only 126 dropouts because of

adverse

effects. Fosamax was tested for two years to measure its effect on

osteoporosis with only 4 percent dropping out because of the

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