International Center for the Study of Psychiatry and Psychology - Psychiatric Drugs: Chemical Warfare on Humans

Psychiatric Drugs: Chemical Warfare on Humans - interview with Robert Whitaker

From http://www.newstarget.com/011353.html
The following is a Street Spirit interview with Robert Whitaker, author of "Mad In America: Bad Science, Bad Medicine, and the Enduring Mistreatment of the Mentally Ill". The interview is conducted by Terry Messman, editor of Street Spirit. Investigative reporter Robert Whitaker, author of the groundbreaking book
Mad In America, is now pursuing a fascinating line of research into how the
mammoth psychiatric drug industry is endangering the American public by
covering up the untold cases of suffering, anguish and disease caused by
the most widely prescribed antidepressants and antipsychotic medications.

Whitaker exposes the massive lies and cover-ups that have corrupted the
Food and Drug Administration's drug review process, and co-opted research
trials in order to spin the results of drug tests and conceal the serious
hazards and even deadly side-effects of brand-name drugs like Prozac,
Zoloft, Paxil and Zyprexa.

The story becomes even more frightening when we look at the aggressive
tactics these giant drug companies have used to silence prominent critics
by defaming them in the press, and by using their money and power to have
widely respected scientists and eminent medical researchers fired for
daring to point out the hazards and risks of suicide and premature death
caused by these drugs.

Whitaker starts by debunking the effectiveness of these massively hyped
wonder drugs -- antidepressants like Prozac, Zoloft and Paxil, and the new
atypical antipsychotic drugs like Zyprexa. His research shows how they
often are barely more effective than placebos in treating mental disorder
and depression, despite the glowing adulation they have received in the
mainstream media.

But he goes on to make the startling claim that these new psychiatric drugs
have directly contributed to an alarming new epidemic of drug-induced
mental illness. The very drugs prescribed by physicians to stabilize mental
disorders in fact are inducing pathological changes in brain chemistry and
triggering suicide, manic and psychotic episodes, convulsions, violence,
diabetes, pancreatic failure, metabolic diseases, and premature death.

Whitaker originally was a highly regarded medical reporter at the Albany
Times Union and also wrote off and on for the Boston Globe. A series he
co-wrote for the Boston Globe on harmful psychiatric research was a
finalist for the Pulitzer Prize in 1998. When he began his investigative
research into psychiatric issues, Whitaker was still a believer in the
story of progress that psychiatry has been telling the public for decades.

He said, "I absolutely believed the common wisdom that these antipsychotic
drugs actually had improved things and that they had totally revolutionized
how we treated schizophrenia. People used to be locked away forever, and
now maybe things weren't great, but they were a lot better. It was a story
of progress."

That story of progress was fraudulent, as Whitaker soon found out when he
gained new insight from his research into torturous psychiatric practices
such as electroshock, lobotomy, insulin coma, and neuroleptic drugs.
Psychiatrists told the public that these techniques "cured" psychosis or
balanced the chemistry of the brain.

But, in reality, the common thread in all these different treatments was
the attempt to suppress "mental illness" by deliberately damaging the
higher functions of the brain. The stunning truth is that, behind closed
doors, the psychiatric establishment itself labeled these treatments as
"brain-damaging therapeutics."

The first generation of antipsychotic drugs created a drug-induced brain
pathology by blocking the neurotransmitter dopamine and essentially
shutting down many higher brain functions. In fact, when antipsychotics
such as Thorazine and Haldol were first introduced, psychiatrists
themselves said that these neuroleptic drugs were virtually
indistinguishable from a "chemical lobotomy."

In recent years, the media have heralded the arrival of so-called designer
drugs like Prozac, Paxil and Zyprexa that are supposed to be superior and
have fewer side effects than the old tricyclic antidepressants and the
first antipsychotics. Millions of Americans have believed this story and
have enriched drug companies like Eli Lilly by spending billions of dollars
annually to purchase these new medications.

Whitaker's research into the tragic cases of disease, suffering and early
deaths caused by these drugs shows that millions of consumers have been
misled by a massive campaign of lies, distortions, and bought-and-paid-for
drug trials. Eminent medical researchers who have tried to warn us of the
perils of these drugs have been silenced, intimidated and defamed. In the
process, the Food and Drug Administration has become the lapdog of the
giant pharmaceutical industry, not its watchdog.

Street Spirit interviewed Robert Whitaker about this new "epidemic" of
mental disorders, and how the giant drug companies have profited from
selling drugs that make us sicker.

Street Spirit: Your new line of research indicates that there has been an
enormous rise in the incidence of mental illness in the United States,
despite the seeming advances in a new generation of psychiatric drugs. Why
do you refer to this increase as an epidemic?

Robert Whitaker: Even people like the psychiatrist E. Fuller Torrey wrote a
book recently in which he said it looks like we're having an epidemic of
mental illness. When the National Institute of Mental Health publishes its
figures on the incidence of mental illness, you see these rising numbers of
mentally ill people. Some recent reports even say that 20 percent of
Americans now are mentally ill.

So what I wanted to do was two-fold. I wanted to look into exactly how
dramatic is this increase in mental illness, and particularly severe mental
illness. Part of this rise in the number of people said to be mentally ill
is just definitional. We draw a big wide boundary today and we throw all
sorts of people into that category of mentally ill. So children who are not
sitting neatly enough in their school rooms are said to have attention
deficit hyperactivity disorder (ADHD), and we created a new disorder called
social anxiety disorder.

SS: So what used to be called simply shyness or anxiety in relating to
people is now labeled a mental disorder and you supposedly need an
antidepressant like Paxil for social anxiety disorder.

RW: Exactly. And you need a stimulant like Ritalin for ADHD.

SS: This increases psychiatry's clients, but doesn't it also increase the
number of people that giant pharmaceutical companies can sell their
psychiatric drugs to?

RW: Absolutely. So part of what we're seeing is nothing more than the
creation of a larger market for drugs. If you think about it, as long as we
draw as big a circle as possible, and expand the boundaries of mental
illness, psychiatry can have more clients and sell more drugs. So there's a
built-in economic incentive to define mental illness in as broad terms as
possible, and to find ordinary, distressing emotions or behaviors that some
people may not like and label them as mental illness.

SS: Your research also shows that there is a real increase in people who
have a severe mental disorder. Now, this seems counterintuitive, but is it
true that you believe much of this increase is caused by the overuse of
some of the new generations of psychiatric drugs?

RW: Yes, exactly. I looked at the number of the so-called severely disabled
mentally ill -- people who aren't working or who are somehow dysfunctional
because of mental illness. So I wanted to chart through history the
percentage of the population who are considered the disabled mentally ill.

Now, by 1903, we see that roughly 1 out of every 500 people in the United
States is hospitalized for mental illness. By 1955, at the start of the
modern era of psychiatric drugs, roughly one out of every 300 people was
disabled by mental illness. Now, let's go to 1987, the end of the first
generation of antipsychotic drugs; and from 1987 forward we get the modern
psychiatric drugs. From 1955 to 1987, during this first era of psychiatric
drugs -- the antipsychotic drugs Thorazine and Haldol and the tricyclic
antidepressants (such as Elavil and Anafranil) -- we saw the number of
disabled mentally ill increase four-fold, to the point where roughly one
out of every 75 persons are deemed disabled mentally ill.

Now, there was a shift in how we cared for the disabled mentally ill
between 1955 and 1987. In 1955, we were hospitalizing them. Then, by 1987,
we had gone through social change, and we were now placing people in
shelters, nursing homes, and some sort of community care, and gave them
either SSI or SSDI payments for mental disability. In 1987, we started
getting these supposedly better, second-generation psychiatric drugs like
Prozac and the other selective serotonin re-uptake inhibitor (SSRI)
antidepressants. Shortly after that, we get the new, atypical antipsychotic
drugs like Zyprexa (olanzapine), Clozaril and Risperdal.

What's happened since 1987? Well, the disability rate has continued to
increase until it's now one in every 50 Americans. Think about that: One in
every 50 Americans disabled by mental illness today. And it's still
increasing. The number of mentally disabled people in the United States has
been increasing at the rate of 150,000 people per year since 1987. That's
an increase every day over the last 17 years of 410 people per day newly
disabled by mental illness.

SS: So that leads to the obvious question. If psychiatry has introduced
these so-called wonder drugs like Prozac and Zoloft and Zyprexa, why is the
incidence of mental illness going up dramatically?

RW: That's exactly it. This is a scientific question. We have a form of
care where we're using these drugs in an ever more expansive manner, and
supposedly we have better drugs and they're the cornerstone of our care, so
we should see decreasing disability rates. That's what your expectation
would be.

Instead, from 1987 until the present, we saw an increase in the number of
mentally disabled people from 3.3 million people to 5.7 million people in
the United States. In that time, our spending on psychiatric drugs
increased to an amazing degree. Combined spending on antipsychotic drugs
and antidepressants jumped from around $500 million in 1986 to nearly $20
billion in 2004. So we raise the question: Is the use of these drugs
somehow actually fueling this increase in the number of the disabled
mentally ill?

When you look at the research literature, you find a clear pattern of
outcomes with all these drugs -- you see it with the antipsychotics, the
antidepressants, the anti-anxiety drugs and the stimulants like Ritalin
used to treat ADHD. All these drugs may curb a target symptom slightly more
effectively than a placebo does for a short period of time, say six weeks.
An antidepressant may ameliorate the symptoms of depression better than a
placebo over the short term.

What you find with every class of these psychiatric drugs is a worsening of
the target symptom of depression or psychosis or anxiety over the long
term, compared to placebo-treated patients. So even on the target symptoms,
there's greater chronicity and greater severity of symptoms. And you see a
fairly significant percentage of patients where new and more severe
psychiatric symptoms are triggered by the drug itself.

SS: New psychiatric symptoms created by the very drugs people are told will
help them recover?

RW: Absolutely. The most obvious case is with the antidepressants. A
certain percentage of people placed on the SSRIs because they have some
form of depression will suffer either a manic or psychotic attack --
drug-induced. This is well recognized. So now, instead of just dealing with
depression, they're dealing with mania or psychotic symptoms. And once they
have a drug-induced manic episode, what happens? They go to an emergency
room, and at that point they're newly diagnosed. They're now said to be
bipolar and they're given an antipsychotic to go along with the
antidepressant; and, at that point, they're moving down the path to chronic
disability.

SS: Modern psychiatry claims that these psychiatric drugs correct
pathological brain chemistry. Is there any evidence to back up their claim
that abnormal brain chemistry is the culprit in schizophrenia and depression?

RW: This is the key thing everyone needs to understand. It really is the
answer that unlocks this mystery of why the drugs would have this long-term
problematic effect. Start with schizophrenia. They hypothesize that these
drugs work by correcting an imbalance of the neurotransmitter dopamine in
the brain.

The theory was that people with schizophrenia had overactive dopamine
systems; and these drugs, by blocking dopamine in the brain, fixed that
chemical imbalance. Therefore, you get the metaphor that they're like
insulin is for diabetes; they're fixing an abnormality. With the
antidepressants, the theory was that people with depression had too low
levels of serotonin; the drugs upped the levels of serotonin in the brain
and therefore they're balancing the brain chemistry.

First of all, those theories never arose from investigations into what was
actually happening to people. Rather, they would find out that
antipsychotics blocked dopamine and so they theorized that people had
overactive dopamine systems. Same with the antidepressants. They found that
antidepressants upped the levels of serotonin; therefore, they theorized
that people with depression must have low levels of serotonin.

But here is the thing that one wishes all of America would know and wishes
psychiatry would come clean on: They've never been able to find that people
with schizophrenia have overactive dopamine systems. They've never been
able to find that people with depression have underactive serotonin
systems. They've never found consistently that any of these disorders are
associated with any chemical imbalance in the brain. The story that people
with mental disorders have known chemical imbalances -- that's a lie. We
don't know that at all. It's just something that they say to help sell the
drugs and help sell the biological model of mental disorders.

But the kicker is this. We do know, in fact, that these drugs perturb how
these chemical messengers work in the brain. The real paradigm is: People
diagnosed with mental disorders have no known problem with their
neurotransmitter systems; and these drugs perturb the normal function of
neurotransmitters.

SS: So rather than fixing a chemical imbalance, these widely prescribed
drugs distort the brain chemistry and make it pathological.

RW: Absolutely. Stephen Hyman, a well-known neuroscientist and the former
director of the National Institute of Mental Health, wrote a paper in 1996
that looked at how psychiatric drugs affect the brain. He wrote that all
these drugs create perturbations in neurotransmitter functions. And he
notes that the brain, in response to this drug from the outside, alters its
normal functions and goes through a series of compensatory adaptations.

In other words, it tries to adapt to the fact that an antipsychotic drug is
blocking normal dopamine functions. Or in the case of antidepressants, it
tries to compensate for the fact that you're blocking a normal reuptake of
serotonin. The way it does this is to adapt in the opposite way. So, if
you're blocking dopamine in the brain, the brain tries to put out more
dopamine and it actually increases the number of dopamine receptors. So a
person placed on antipsychotic drugs will end up with an abnormally high
number of dopamine receptors in the brain.

If you give someone an antidepressant, and that tries to keep serotonin
levels too high in the brain, it does exactly the opposite. It stops
producing as much serotonin as it normally does and it reduces the number
of serotonin receptors in the brain. So someone who is on an
antidepressant, after a time ends up with an abnormally low level of
serotonin receptors in the brain. And here's what Hyman concluded about
this: After these changes happened, the patient's brain is functioning in a
way that is "qualitatively as well as quantitatively different from the
normal state." So what Stephen Hyman, former head of the NIMH, has done is
present a paradigm for how these drugs affect the brain that shows that
they're inducing a pathological state.

SS: So the paradox is there's no evidence for modern psychiatry's claim
that there is any pathological biochemical imbalance in the brain that
causes mental illness, but if you treat people with these new wonder drugs,
that is what creates a pathological imbalance?

RW: Yes, these drugs disrupt normal brain chemistry. That's the real
paradox here. And the real tragedy is, that even as we peddle these drugs
as chemical balancers, chemical fixers, in truth we're doing precisely the
opposite. We're taking a brain that has no known abnormal brain chemistry,
and by placing people on the drugs, we're perturbing that normal chemistry.
Here's how Barry Jacobs, a Princeton neuroscientist, describes what happens
to a person given an SSRI antidepressant. "These drugs," he said, "alter
the level of synaptic transmission beyond the physiologic range achieved
under normal environmental biological conditions. Thus, any behavioral or
physiologic change produced under these conditions might more appropriately
be considered pathologic rather than reflective of the normal biological
role of serotonin."

SS: One of the SSRI antidepressants that's widely believed to be a wonder
drug is Prozac. Yet your research found that the Food and Drug
Administration (FDA) received more adverse reports about Prozac than any
other drug. What sort of ill effects were people reporting?

RW: First of all, with Prozac and the SSRIs that followed, their level of
efficacy was always of a very minor sort. In all the clinical trials of the
antidepressants, roughly 41 percent of the patients got better in the short
term versus 31 percent of the patients on placebo. Now just one other
caveat on that. If you use an active placebo in these trials -- an active
placebo causes a physiologic change with no benefit, like a dry mouth --
any difference in outcome between the antidepressant and placebo virtually
disappears.

SS: Weren't the early drug tests of Prozac so unpromising that they had to
manipulate test results to get FDA approval at all?

RW: What happened with Prozac is a fascinating story. Right from the
beginning, they noticed only very marginal efficacy over placebo; and they
noticed that they had some problems with suicide. There were increased
suicidal responses compared to placebo. In other words, the drugs was
agitating people and making people suicidal who hadn't been suicidal
before. They were getting manic responses in people who hadn't been manic
before. They were getting psychotic episodes in people who hadn't been
psychotic before. So you were seeing these very problematic side effects
even at the same time that you were seeing very modest efficacy, if any,
over placebo in ameliorating depression.

Basically, what Eli Lilly (Prozac's manufacturer) had to do was cover up
the psychosis, cover up the mania; and, in that manner, it was able to get
these drugs approved. One FDA reviewer even warned that Prozac appeared to
be a dangerous drug, but it was approved anyway. We're seemingly finding
all this out only now: "Oh, Prozac can cause suicidal impulses and all
these SSRIs may increase the risk of suicide." The point is, that wasn't
anything new. That data was there from the very first trial. You had people
in Germany saying, "I think this is a dangerous drug."

SS: Even back in the late 1980s, they already knew?

RW: Before the late 1980s -- in the early '80s, before Prozac gets
approved. Basically what Eli Lilly had to do was cover up that risk of
mania and psychosis, cover up that some people were becoming suicidal
because they were getting this nervous agitation from Prozac. That's the
only way it got approved.

There were various ways they did the cover-up. One was just to simply
remove reports of psychosis from some of the data. They also went back and
recoded some of the trial results. Let's say someone had a manic episode or
a psychotic episode; instead of putting that down, they would just put down
a return of depression, and that sort of thing. So there was a basic need
to hide these risks right from the beginning, and that's what was done.

So Prozac gets approved in 1987, and it's launched in this amazing PR
campaign. The pill itself is featured on the cover of several magazines!
It's like the Pill of the Year [laughs]. And it's said to be so much safer:
a wonder drug. We have doctors saying, "Oh, the real problem with this drug
is that we can now create whatever personality we want. We're just so
skilled with these drugs that if you want to be happy all the time, take
your pill!"

That was complete nonsense. The drugs were barely better than placebo at
alleviating depressive symptoms over the short term. You had all these
problems; yet we were touting these drugs, saying, "Oh, the powers of
psychiatry are such that we can give you the mind you want -- a designer
personality!" It was absolutely obscene. Meanwhile, which drug, after being
launched, quickly became the most complained about drug in America? Prozac!

SS: What were the level of complaints when Prozac hit the market?

RW: In this county, we have Medwatch, a reporting system in which we report
adverse events about psychiatric drugs to the FDA. By the way, the FDA
tries to keep these adverse reports from the public. So, instead of the FDA
making these easily available to the public. so you can know about the
dangers of the drugs, it's very hard to get these reports.

Within one decade, there were 39,000 adverse reports about Prozac that were
sent to Medwatch. The number of adverse events sent to Medwatch is thought
to represent only one percent of the actual number of such events. So, if
we get 39,000 adverse event reports about Prozac, the number of people who
have actually suffered such problems is estimated to be 100 times as many,
or roughly four million people. This makes Prozac the most complained about
drug in America, by far. There were more adverse event reports received
about Prozac in its first two years on the market than had been reported on
the leading tricyclic antidepressant in 20 years.

Remember, Prozac is pitched to the American public as this wonderfully safe
drug, and yet what are people complaining about? Mania, psychotic
depression, nervousness, anxiety, agitation, hostility, hallucinations,
memory loss, tremors, impotence, convulsions, insomnia, nausea, suicidal
impulses. It's a wide range of serious symptoms.

And here's the kicker. It wasn't just Prozac. Once we got the other SSRIs
on the market, like Zoloft and Paxil, by 1994, four SSRI antidepressants
were among the top 20 most complained about drugs on the FDA's Medwatch
list. In other words, every one of these drugs brought to market started
triggering this range of adverse events. And these were not minor things.
When you talk about mania, hallucinations, psychotic depression, these are
serious adverse events.

Prozac was pitched to the American public as a wonder drug. It was featured
on the covers of magazines as so safe, and as a sign of our wonderful
ability to effect the brain just as we want it. In truth, the reports were
showing it could trigger a lot of dangerous events, including suicide and
psychosis.

The FDA was being warned about this. They were getting a flood of adverse
event reports, and the public was never told about this for the longest
period of time. It took a decade for the FDA to begin to acknowledge the
increased suicides and the violence it can trigger in some people. It just
shows how the FDA betrayed the American people. This is a classic example.
They betrayed their responsibility to act as a watchdog for the American
people. Instead they acted as an agency that covered up harm and risk with
these drugs.

SS: In light of the FDA's failure to warn us about Prozac, what about their
recent negligence on the issue of the risk of suicide in children given
antidepressants like Paxil? Weren't England's mental health officials far
better than their American counterparts in the FDA in warning about the
dangers of suicidal attempts when antidepressants are given to youth?

RW: Yes. The children's story is unbelievably tragic. It's also a really
sordid story. Let's go back a little to see what happened to children and
antidepressants. Prozac comes to market in 1987. By the early 1990s, the
pharmaceutical companies making these drugs are saying, "How do we expand
the market for antidepressants?" Because that's what drug companies do --
they want to get to an ever-larger number of people. They saw they had an
untapped market in kids. So let's start peddling the drugs to kids. And
they were successful. Since 1990, the use of antidepressants in kids went
up something like seven-fold. They began prescribing them willy-nilly.

Now, whenever they did pediatric trials of antidepressants, they found that
the drugs were no more effective on the target symptom of depression than
placebo. This happened again and again in the pediatric drug trials of
antidepressants. So, what that tells you is there is no real therapeutic
rationale for the drugs because in this population of kids, the drugs don't
even curb the target symptoms over the short term any better than placebo;
and yet they were causing all sorts of adverse events.

For example, in one trial, 75 percent of youth treated with antidepressants
suffered an adverse event of some kind. In one study by the University of
Pittsburgh, 23 percent of children treated with an SSRI developed mania or
manic-like symptoms; an additional 19 percent developed drug-induced
hostility. The clinical results were telling you that you didn't get any
benefit on depression; and you could cause all sorts of real problems in
kids -- mania, hostility, psychosis, and you may even stir suicide. In
other words, don't use these drugs, right? It was absolutely covered up.

SS: How was it covered up?

RW: We had psychiatrists -- some of those obviously getting money from the
drug companies -- saying the kids are under-treated and they're at risk of
suicide and how could we possibly treat kids without these pills and what a
tragedy it would be if we couldn't use these antidepressants.

Finally, a prominent researcher in England, David Healy, started doing his
own research on the ability of these drugs to stir suicide. He also managed
to get access to some of the trial results and he blew the whistle. He
first blew the whistle in England and he presented this data to the review
authorities there. And they saw that it looks like these drugs are
increasing the risk of suicide and there are really no signs of benefits on
the target symptoms of depression. So they began to move there to warn
doctors not to prescribe these drugs to youth.

What happens in the United States? Well, it's only after there's a lot of
pressure put on the FDA that they even hold a hearing. The FDA sort of
downplays the risk of these drugs. They're slow to even put black box
warnings on them. Why? Aren't kids lives worth protecting? If we know that
we have a scientifically shown risk that these drugs increase suicide,
shouldn't you at least warn about it? But the FDA was even digging in its
heels about putting that black box warning on the drugs.

SS: If Prozac is the nation's most complained about drug, if Paxil is shown
to be a suicide risk for youth, how do these antidepressants continue to
have a reputation as near-magic cures for depression? And why did the FDA
failed to warn us about Paxil and Prozac for such a long time?

RW: There's a couple reasons for that. The FDA's funding changed in the
1990s. An act was passed in which a lot of the FDA's funding came from the
drug industry: the PDUFA Act, or Prescription Drug User Fee Act. Basically,
when drug companies applied for FDA approval they had to pay a fee. Those
fees became what is funding a large portion of the FDA's review of drug
applications.

So all of a sudden, the funding is coming from the drug industry; it's no
longer coming from the people. As that act comes up for renewal, basically
the drug lobbyists are telling the FDA that their job is no longer to be
critically analyzing drugs, but to approve drugs quickly. And that was part
of Newt Gingrich's thing: Your job is to get these drugs to market. Start
partnering with the drug industry and facilitating drug development. We
lost this idea that the FDA had a watchdog role.

Also, in a human way, a lot of people who work for the FDA leave there and
end up going to work for the drug companies. The old joke is that the FDA
is sort of like a showcase for a future job in the drug industry. You go
there, you work awhile, then you go off into the drug industry. Well, if
that's the progression that people make, in essence they're making good old
boy network connections, so they're not going to be so harsh on the drug
companies. So, that's what really happened in the 1990s. The FDA was given
new marching orders. The orders were: "Facilitate getting drugs to market.
Don't be too critical. And, in fact, if you want to keep your funding,
which was coming now from the drug industry, make sure you take these
lessons to heart."

SS: So the giant pharmaceutical companies have a vast amount of power to
cook the results of drug tests and make researchers and even the FDA itself
bow to their will?

RW: The FDA, in essence, was kneecapped in the early 1990s, and we really
saw it with the psychiatric drugs. The FDA became a lapdog for the
pharmaceutical industry, not a watchdog. It's only now that this has become
common knowledge. We have Marcia Angell, the former editor of the New
England Journal of Medicine, write a book in which she says that the FDA
became a lapdog. It's basically now well recognized that you had this
decline and fall. As the editor of the New England Journal of Medicine, the
most prestigious medical journal we have, Marcia Angell is someone who was
at the very heart of American medicine, and she concluded that the FDA let
down the American people. And she lost her job at the New England Journal
of Medicine for starting to criticize pharmaceutical companies.

She was the editor of the journal in the late 1990s and there was a
corresponding doctor named Thomas Bodenheimer who decided to write an
article about how you couldn't even trust what was published in the medical
journals anymore because of all the spinning of results. So they did an
investigation about how the pharmaceutical companies are funding all the
research and spinning the trial results, so you can no longer really trust
what you read in scientific journals. They pointed out that when they tried
to get an expert to review the scientific literature related to
antidepressants, they basically couldn't find someone who hadn't taken
money from the drug companies.

Now, the New England Journal of Medicine is published by the Massachusetts
Medical Society which publishes a lot of other journals, and they get a lot
of pharmaceutical advertising. So what happens after that article appears
by Thomas Bodenheimer and an accompanying editorial by Marcia Angell about
the sorry state of American medicine because of this? They both lose their
jobs! She's gone and so is Thomas Bodenheimer. Think about this. We have
the leading medical journal firing people, letting them go, because they
dared to criticize the dishonest science and the dishonest process that was
poisoning the scientific literature.

So we have the FDA that's acting as lapdogs. You can't trust the scientific
literature. All this shows how the American public was betrayed and didn't
know about all the problems with these drugs and why it was kept from them.
It has to do with money, prestige and old boy networks.

SS: It also has to do with the silencing of critics. Eli Lilly uses the
media to trumpet Prozac's benefits and gives perks to doctors to attend
conferences to hear about its benefits, and buys off researchers. But don't
they also use their power and money to silence their critics?

RW: An example is Dr. Joseph Glenmullen, a psychiatrist who also works for
Harvard University Health Services, and who wrote a book called Prozac
Backlash to warn about the dangers of Prozac. He's finding that the drugs
are being overused and cause severe side effects. He even raises questions
about long-term memory problems with the drugs and cognitive dysfunction.
Well, Eli Lilly then mounted a public relations campaign to try to
discredit him. They sent out notices to the media questioning his
affiliation with Harvard Medical School, etc. It was all about silencing
the critics.

If you sing the tune that the drug companies want, at the very top levels,
you get paid a lot of money to fly around and give presentations about the
wonders of the drugs. And those who come, and don't ask any embarrassing
questions, get the lobster dinners and maybe they get a little honorarium
for attending this educational meeting. So if you want to be part of this
gravy train, you can. You sing the wonders of the drug, and you don't talk
about their nasty side effects, and you can get a nice payment as one of
their guest speakers, as one of their experts.

But if you're one of the ones saying, "What about the mania, what about the
psychosis?" -- they do silence you. Look at what happened to David Healy.
Healy is even the best example. David Healy has this sterling reputation in
England. He's written several books on the history of psychopharmacology.
He's like the former Secretary of the Psychopharmacology Association over
there. He gets offered a job at the University of Toronto to head up their
psychiatry department. So while he's waiting to assume that position at the
University of Toronto, he goes to Toronto and delivers a talk on the
elevated risk of suicide with Prozac and some of the other SSRIs. By the
time he's back home, the job offer has been rescinded.

Now does Eli Lilly donate some money to the University of Toronto?
Absolutely. So, to answer your question, yes, Eli Lilly silences dissenters
as well.

SS: What is the story behind the secret settlement between Eli Lilly and
the survivors who sued the company after Joseph Wesbecker shot 20 coworkers
after being put on Prozac?

RW: During this trial in which Eli Lilly was being sued, the judge was
going to allow some very damaging evidence showing wrongdoing by Eli Lilly
in a previous instance. The judge said, "Go ahead and introduce this at the
trial." But next thing you know, they don't introduce this; and in fact,
all of a sudden, the plaintiffs no longer are presenting very damaging
evidence to make their case. So the judge wonders why they are not
presenting their best case anymore. He smells a rat. He suspects Eli Lilly
has settled with the plaintiffs secretly and the deal is that, as part of
this settlement, the plaintiffs will go ahead with a sham trial so that Eli
Lilly will win the trial. Then Eli Lilly can claim, "See our drug doesn't
cause people to become violent."

And, indeed, that's what happened. Eli Lilly felt it was going to lose this
trial. They went to the plaintiffs and said they would give them a lot of
money. They agreed to go ahead and settle the case, but had the plaintiffs
go ahead with the trial. That way Eli Lilly can publicly claim that they
won the trial and Prozac doesn't cause harm.

SS: How did this even come out into the light of day?

RW: We would never have known about this except for two things. One,
believe it or not, the judge, in essence, appealed the decision in his own
court. He said, "I smell a rat." And through that, he found out that there
was this secret settlement and that it was a sham proceeding that continued
on. He said it was one of the worst violations of the integrity of the
legal process that he'd ever seen. And second, an English journalist named
John Cornwell wrote a book called Power to Harm: Mind, Medicine, and Murder
on Trial. He wrote about this case, and yet in the United States, we got
almost no news about this secret settlement and this whole perversion of
the legal process. It was an English journalist who was exposing this story.

My point here is this: They silence people like Marcia Angell. They pervert
the scientific process. They pervert the legal process. They pervert the
FDA drug review process. It's everywhere! And that's how we as a society
end up believing in these psychiatric drugs. You asked the question a while
back, "Why do we still believe in Prozac?" One of the reasons is that the
story about Prozac is, in effect, maintained. It's publicly maintained
because we do all this silencing along all these lines.

The other thing to remember is that some people on Prozac do feel better.
That's true. That shows up, just in the same way that some people on
placebos feel better. And those are the stories that get repeated: "Oh, I
took Prozac and I'm feeling better." It's that select group that does
better that becomes the story that is told out there, and the story that
the public hears. So that's why we continued to believe in the story of
these wonder drugs that are very safe in spite of all this messy stuff that
gets covered up.

SS: Let's now move from the antidepressants like Prozac to consider another
new group of supposed wonder drugs -- the new antipsychotic drugs. You
write that long-term use of antipsychotic drugs -- both the original
neuroleptic drugs like Thorazine and Haldol and the newer atypicals like
Zyprexa and Risperdal -- cause pathological changes in the brain that can
lead to a worsening of the symptoms of mental illness. What changes in
brain chemistry result from the antipsychotics, and how can that lead to
the most frightening prospect you describe -- chronic mental illness that
is locked in by these drugs?

RW: This is a line of research that goes across 40 years. This problem of
chronic illness shows up time and time again in the research literature.
This biological mechanism is somewhat well understood now. The
antipsychotics profoundly block dopamine receptors. They block 70-90
percent of the dopamine receptors in the brain. In return, the brain
sprouts about 50 percent extra dopamine receptors. It tries to become extra
sensitive.

So in essence you've created an imbalance in the dopamine system in the
brain. It's almost like, on one hand, you've got the accelerator down --
that's the extra dopamine receptors. And the drug is the brake trying to
block this. But if you release that brake, if you abruptly go off the
drugs, you now do have a dopamine system that's overactive. You have too
many dopamine receptors. And what happens? People that go abruptly off of
the drug, do tend to have severe relapses.

SS: So people that have been treated with these antipsychotic drugs have a
far greater tendency to relapse, and have new episodes of mental illness,
as opposed to people who have had other kinds of non-drug therapies?

RW: Absolutely, and that was understood by 1979, that you were actually
increasing the underlying biological vulnerability to the psychosis. And by
the way, we sort of understood that if you muck with the dopamine system,
that you could cause some symptoms of psychosis with amphetamines. So if
you give someone amphetamines enough, they're at increased risk of
psychosis. This is well known. And what do amphetamines do? They release
dopamine. So there is a biological reason why, if you're mucking up the
dopamine system, you're increasing the risk of psychosis. That's in essence
what these antipsychotic drugs do, they muck up the dopamine system.

Here's just one real powerful study on this: Researchers with the
University of Pittsburgh in the 1990s took people newly diagnosed with
schizophrenia, and they started taking MRI pictures of the brains of these
people. So we get a picture of their brains at the moment of diagnosis, and
then we prepare pictures over the next 18 months to see how those brains
change. Now during this 18 months, they are being prescribed antipsychotic
medications, and what did the researchers report? They reported that, over
this 18-month period, the drugs caused an enlargement of the basal ganglia,
an area of the brain that uses dopamine. In other words, it creates a
visible change in morphology, a change in the size of an area of the brain,
and that's abnormal. That's number one. So we have an antipsychotic drug
causing an abnormality in the brain.

Now here's the kicker. They found that as that enlargement occurred, it was
associated with a worsening of the psychotic symptoms, a worsening of
negative symptoms. So here you actually have, with modern technology, a
very powerful study. By imaging the brain, we see how an outside agent
comes in, disrupts normal chemistry, causes an abnormal enlargement of the
basal ganglia, and that enlargement causes a worsening of the very symptoms
it's supposed to treat. Now that's actually, in essence, a story of a
disease process -- an outside agent causes abnormality, causes symptoms...

SS: But in this case, the outside agent that triggers the disease process
is the supposed cure for the disease! The psychiatric drug is the
disease-causing agent.

RW: That's exactly right. It's a stunning, damning finding. It's the sort
of finding you would say, "Oh Christ, we should be doing something
different." Do you know what those researchers got new grants for, after
they reported that?

SS: No, what? You'd guess they got funding to carry out these same studies
on other classes of psychiatric drugs.

RW: They got a grant to develop an implant, a brain implant, that would
deliver drugs like Haldol on a continual basis! A grant to develop a drug
delivery implant so you could implant this in the brains of people with
schizophrenia and then they wouldn't even have a chance not to take the drugs!

SS: Unbelievable. Designing an implant to provide a constant dose of a drug
that they had just discovered causes pathology in the brain chemistry.

RW: Right, they had just found that they're causing a worsening of
symptoms! So why would you go on to a design a permanent implant? Because
that's where the money was. And no one wanted to deal with this horrible
finding of an enlargement of the basal ganglia caused by the drugs, and
that is associated with the worsening of symptoms. No one wanted to deal
with the fact that when you look at people medicated on antipsychotics, you
start to see a shrinking of the frontal lobes. No one wants to talk about
that either. They stopped that research.

SS: What other side effects are caused by prolonged use of these
antipsychotic drugs?

RW: Oh, you get tardive dyskinesia, a permanent brain dysfunction; and
akathisia, which is this incredible nervous agitation. You're just never
comfortable. You want to sit but you can't sit. It's like you're crawling
out of your own skin. And it's associated with violence, suicide and all
sorts of horrible things.

SS: Those kinds of side-effects were notorious with the first generation of
antipsychotic drugs, like Thorazine, Haldol and Stelazine. But, just as
with Prozac, so many people are still touting the new generation of
atypical antipsychotics -- Zyprexa, Clozaril and Risperdal -- as wonder
drugs that control mental illness with far fewer side effects. Is that
true? What have you found?

RW: No, it's just complete nonsense. In fact, I think the newer drugs will
eventually be seen as more dangerous than the old drugs, if that's
possible. As you know, the standard neuroleptics like Thorazine and Haldol
have had quite a litany of harm with the tardive dyskinesia and all. So
when we got the new atypical drugs, they were touted as so much safer. But
with these new atypicals, you get all sorts of metabolic dysfunctions.

Let's talk about Zyprexa. It has a different profile. So it may not cause
as much tardive dyskinesia. It may not cause as many Parkinsonian symptoms.
But it causes a whole range of new symptoms. So, for example, it's more
likely to cause diabetes. It's more likely to cause pancreatic disorders.
It's more likely to cause obesity and appetite-disregulation disorders.

In fact, researchers in Ireland reported in 2003 that since the
introduction of the atypical antipsychotics, the death rate among people
with schizophrenia has doubled. They have done death rates of people
treated with standard neuroleptics and then they compare that with death
rates of people treated with atypical antipsychotics, and it doubles. It
doubles! It didn't reduce harm. In fact, in their seven-year study, 25 of
the 72 patients died.

SS: What were the causes of death?

RW: All sorts of physical illnesses, and that's part of the point. You're
getting respiratory problems, you're getting people dying of incredibly
high cholesterol counts, heart problems, diabetes. With olanzapine
(Zyprexa), one of the problems is that you're really screwing up the core
metabolic system. That's why you get these huge weight gains, and you get
the diabetes. Zyprexa basically disrupts the machine that we are that
processes food and extracts energy from that food. So this very fundamental
thing that we humans do is disrupted, and at some point you just see all
these pancreatic problems, faulty glucose regulation, diabetes, etc. That's
really a sign that you're mucking with something very fundamental to life.

SS: There's supposedly an alarming increase in mental illness being
diagnosed in children. Millions are diagnosed with depression, bipolar and
psychotic symptoms, attention deficit hyperactivity disorder, and social
anxiety disorder. Is this explosive new prevalence of mental illness among
children a real increase, or is it a marketing campaign that enriches the
psychiatric drug industry, a bonanza for the pharmaceutical corporations?
RW: You're touching on something now that is a tragic scandal of monumental
proportions. I talk sometimes to college classes, psychology classes. You
cannot believe the percentage of youth who have been told they were
mentally ill as kids, that something was wrong with them. It's absolutely
phenomenal. It's absolutely cruel to be telling kids that they have these
broken brains and mental illnesses.

There's two things that are happening here. One, of course, is that it's
complete nonsense. As you remember as a kid, you have too much energy or
you behave sometimes in not altogether appropriate ways, and you do have
these extremes of emotions, especially during your teenage years. Both
children and teenagers can be very emotional. So one thing that's going on
is that they take childhood behaviors and start defining behaviors they
don't like as pathological. They start defining emotions that are
uncomfortable as pathological. So part of what we're doing is pathologizing
childhood with straight-out definition stuff. We're pathologizing poverty
among kids.

For example, if you're a foster kid, and maybe you drew a bad straw in the
lottery of life and are born into a dysfunctional family and you get put
into foster care, do you know what happens today? You pretty likely are
going to get diagnosed with a mental disorder, and you're going to be
placed on a psychiatric drug. In Massachusetts, it's something like 60 to
70 percent of kids in foster care are now on psychiatric drugs. These kids
aren't mentally ill! They got a raw deal in life. They ended up in a foster
home, which means they were in a bad family situation, and what does our
society do? They say: "You have a defective brain." It's not that society
was bad and you didn't get a fair deal. No, the kid has a defective brain
and has to be put on this drug. It's absolutely criminal.

Let's talk about bipolar disorder among kids. As one doctor said, that used
to be so rare as to be almost nonexistent. Now we're seeing it all over.
Bipolar is exploding among kids. Well, partly you could say that we're just
slapping that label on kids more often; but in fact, there is something
real going on. Here's what's happening. You take kids and put them on an
antidepressant -- which we never used to do -- or you put them on a
stimulant like Ritalin. Stimulants can cause mania; stimulants can cause
psychosis.

SS: And antidepressants can also cause mania, as you pointed out.

RW: Exactly, so the kid ends up with a drug-induced manic or psychotic
episode. Once they have that, the doctor at the emergency room doesn't say,
"Oh, he's suffering from a drug-induced episode." He says he's bipolar.

SS: Then they give him a whole new drug for the mental disorder caused by
the first drug.

RW: Yeah, they give him an antipsychotic drug; and now he's on a cocktail
of drugs, and he's on a path to becoming disabled for life. That's an
example of how we're absolutely making kids sick.

SS: It's like society or their schools are trying to make them manageable
and they end up putting them on a chemical roller coaster against their will.

RW: Absolutely.

SS: There's an astonishing number of kids being given Ritalin to cure
hyperactivity. But what 10-year-old boy in a confined school setting isn't
hyperactive? You write that the effect of Ritalin on the dopamine system is
very similar to cocaine and amphetamines.

RW: Ritalin is methylphenidate. Now methylphenidate affects the brain in
exactly the same way as cocaine. They both block a molecule that is
involved in the reuptake of dopamine.

SS: So they both increase the dopamine levels in the brain?

RW: Exactly. And they do it with a similar degree of potency. So
methylphenidate is very similar to cocaine. Now, one difference is whether
you're snorting it or if it's in a pill. That partly changes how quickly
it's metabolized. But still, it basically affects the brain in the same
way. Now, methylphenidate was used in research studies to deliberately stir
psychosis in schizophrenics. Because they knew that you could take a person
with a tendency towards psychosis, give them methylphenidate, and cause
psychosis. We also knew that amphetamines, like methylphenidate, could
cause psychosis in people who had never been psychotic before.

So think about this. We're giving a drug to kids that is known to have the
possibility of stirring psychosis. Now, the odd thing about methylphenidate
and amphetamines is that, in kids, they sort of have a counterintuitive
effect. What does speed do in adults? It makes them more jittery and
hyperactive. For whatever reasons, in kids amphetamines will actually still
their movements; it will actually keep them in their chairs and make them
more focused. So you've got kids in boring schools. The boys are not paying
attention and they're diagnosed with ADHD and put on a drug that is known
to stir psychosis. The next thing you know, a fair number of them are not
doing well by the time they're 15, 16, 17. Some of those kids talk about
how when you're on these drugs for the long term, you start feeling like a
zombie; you don't feel like yourself.

SS: Hollowed-out, blunted emotions. And this is being done to millions of
kids.

RW: Millions of kids! Think about what we're doing. We're robbing kids of
their right to be kids, their right to grow, their right to experience
their full range of emotions, and their right to experience the world in
its full hue of colors. That's what growing up is, that's what being alive
is! And we're robbing kids of their right to be. It's so criminal. And
we're talking about millions of kids who have been affected this way. There
are some colleges where something like 40 to 50 percent of the kids arrive
with a psychiatric prescription.

SS: It looks like a huge social-control mechanism. Society gives kids
Ritalin and antidepressants to subdue them and make them conform. On the
one hand, it's all about social control and conformity. But it also has a
huge marketing payoff.

RW: You're right, it creates customers for the drugs, and hopefully
lifelong customers. That's what they're told, aren't they? They're told
they are going to be on these drugs for life. And next thing they know,
they're on two or three or four drugs. It's brilliant from the capitalist
point of view. It does serve some social-control function. But you take a
kid, and you turn them into a customer, and hopefully a lifelong customer.
It's brilliant.

We now spend more on antidepressants in this country than the Gross
National Product of mid-sized countries like Jordan. It's just amazing
amounts of money. The amount of money we spend on psychiatric drugs in this
country is more than the Gross National Product of two-thirds of the
world's countries. It's just this incredibly lucrative paradigm of the mind
that you can fix chemical imbalances in the brain with these drugs. It
works so well from a capitalistic point of view for Eli Lilly. When Prozac
came to market, Eli Lilly's value on Wall Street, its capitalization, was
around 2 billion dollars. By the year 2000, the time when Prozac was its
number-one drug, its capitalization reached 80 billion dollars -- a
forty-fold increase.

So that's what you really have to look at if you want to see why drug
companies have pursued this vision with such determination. It brings
billions of dollars in wealth in terms of increased stock prices to the
owners and managers of those companies. It also benefits the psychiatric
establishment that gets behind the drugs; they do well by this. There's a
lot of money flowing in the direction of those that will embrace this form
of care. There's advertisements that enrich the media. It's all a big gravy
train.

Unfortunately, the cost is dishonesty in our scientific literature, the
corruption of the FDA, and the absolute harm done to children in this
country drawn into this system, and an increase of 150,000 newly disabled
people every year in the United States for the last 17 years. That's an
incredible record of harm done.

SS: Everyone gets rich -- the drug companies, the psychiatrists, the
researchers, the advertising agencies -- and the clients get drugged out of
their minds and damaged for life.

RW: And you know what's interesting? No one says that the mental health of
the American people is getting better. Instead, everyone says we have this
increasing problem. They blame it on the stresses of modern life or
something like that, and they don't want to look at the fact that we're
creating mental illness.

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