The Drugging of the American Mind

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Wed, 30 Nov 2005 21:26:15 -0500

[sSRI-Research] Seattle Weekly - [cover story] The Drugging

of the American Mind

 

 

http://www.seattleweekly.com/features/0548/051130_news_psych.php

November 30 - December 6, 2005

 

 

 

The Drugging of the American Mind

 

A new generation of meds to treat mental illness has turned millions

of Americans into human guinea pigs. Among them is an eyewitness who

thinks the drug 'revolution' has gone too far.

 

by Philip Dawdy

In the 1990s, there was a small, quiet revolution in American health

care that promised to be as far reaching as the advent of

antidepressants like Prozac. The revolution involved a new class of

medications called atypical antipsychotics, designed for the treatment

of schizophrenia.

 

The atypicals were an instant hit with doctors and schizophrenics

alike. Initially, the drugs treated schizophrenia far better than

older drugs like Thorazine and Haldol had done. In mental-health

circles, atypicals were sometimes referred to as " the silver bullet, "

the breakthrough to a centuries-long quest to effectively treat the

most vicious of mental illnesses without turning patients into zombies.

 

But now this is a revolution in trouble.

 

The new meds don't work as well for schizophrenics as their initial

rock-star status suggested, according to recent research. Questions

about their effectiveness are now being raised. At the same time,

these very same meds are being handed out like candy to a different

class of patients: the millions of Americans with bipolar disorder, or

good old manic-depression. We are not talking about people in psych

hospitals or on the brink of suicide. We are talking about people with

plain vanilla bipolar disorder-the kind where you can't sleep and are

wound up for days but are a long way from diving off a bridge or

running naked down the street.

 

In other words, fairly regular, mainstream Americans now take the most

powerful mood-altering drugs in all of psychiatry. Last year, 23

million prescriptions were written for these drugs. Sales this year

are expected to hit $10 billion, three times what they were in 2000.

Atypicals are the fourth largest class of patented medications in America.

 

Patients aren't taking them for a few days or weeks, either. Doctors

expect their bipolar patients to take these drugs for years, much the

same as they've taken traditional mood stabilizers, like lithium,

which tamp down mood swings. In fact, there's a growing rumble in the

psych world that researchers would like to use atypicals to replace

mood stabilizers altogether.

 

Yet there is no comprehensive scientific evidence to support this

paradigm shift. Zero. The psychiatric industry says this isn't a

problem because real-world treatment has always outpaced research. But

if you happen to be a patient, it's a very big problem-atypicals have

the worst side effects of any drugs used to treat bipolar disorder. As

a patient, I've experienced this shift firsthand, sometimes as a

willing test subject. So, I have a question: Without scientific

evidence, why are doctors prescribing these meds so freely and

expecting patients to take them for so long?

 

For the past 15 years, psych meds have been touted as the answer for

every flaw of mood, feeling, and behavior in American society. We are

in the midst of what's called the psychopharmacological revolution, a

shift from the days of nasty meds that didn't work well to new

generations of meds that aren't nasty and work very well. That's the

hype, at any rate. But the revolution isn't playing out as advertised.

 

Even the habitually cautious National Institute of Mental Health

(NIMH) now says that psych meds-including atypicals-only work 50

percent of the time.

 

But the mental-health world is congenitally incapable of being

skeptical about how psych meds work in patients' lives. Doctors

quickly become wedded to new therapies, and patients follow. As a

result, a new treatment paradigm for millions of bipolars is charging

ahead when researchers, doctors, and patients ought to be very cautious.

 

 

A new class of drugs for treating mental illness, atypical

antipsychotics are becoming more widely used. Sales this year are

expected to hit $10 billion.

(Jay Vidheecharoen)

Bipolar patients should be asking why doctors want them to use meds

long term that regularly generate debilitating side effects in both

bipolars and schizophrenics-the kind of side effects that can mess

with a patient's life almost as much as the underlying illness. Last

summer, Eli Lilly quietly and with little media notice settled a

lawsuit for $750 million. The suit alleged that patients had injuries,

including diabetes, caused by Zyprexa, the top-selling atypical in the

world. Reportedly, 23 patients have died as a result of using the drug.

 

All psych meds generate side effects, but atypicals even more so. On

these meds, patients can gain 20 to 40 pounds in a year. Blood sugar

levels shoot upward. Cholesterol goes up as well. The question of side

effects is important not only because of short-term comfort, but

because of patients' long-term physical health. Extreme weight gain

and altered blood cholesterol levels, for example, give rise to what

doctors call the " metabolic syndrome, " a fancy way of saying

underlying cardiac and respiratory problems can be caused by these

medications over time.

 

That's not speculation, either. Recently published long-term data on

schizophrenics taking atypicals showed weight gain on the order of 2

pounds a month, for example. Researchers say the same dynamic is

present in bipolars. Any patient who takes atypicals can tell you all

about those effects. To date, however, there have been no long-term

studies of the effects of these medications on bipolar patients. There

are other effects, too, life-reducing ones. The daylong grogginess

that comes with atypicals like Seroquel. Cognitive slowing.

Risperdal's tendency to stiffen faces. An odd sense that somehow you

aren't the same person you were before. There's something about the

immediacy of sensation that changes. Nothing is as vivid as it was

before. You feel calm and diluted at the same time.

 

The goal of mental-health treatment is to enhance human life, not

limit it.

 

But something else about long-term treatment of bipolar disorder with

atypicals is as troubling as the side effects. These powerful meds

don't do a good job of knocking down symptoms over the long term. In

the five years that atypicals have been used aggressively in treating

the disorder, I have only encountered a handful of patients who say

that their original starter dose of Zyprexa, say, wiped out their

mania and depression and that life has been balanced ever since.

 

More commonly, patients will start on an atypical after failing to see

their symptoms disappear, or remit, on more traditional meds-and that

happens all the time. The atypical will perform well for a few months,

but then for many bipolars, the symptoms roar back to life. They begin

cycling out to the manic fringes again. Their minds race, they cannot

sleep, they fall apart. That's the nature of the bipolar beast-

limited symptom remission.

 

Let's talk best-case scenario: They are self-aware, responsible

patients and recognize what is happening. They go see their doctor. As

often as not, that's a general practitioner or internist instead of a

psychiatrist. The doctor's common response will be to either increase

the dosage or switch the patient to another atypical. Within a few

months, the process will be repeated because the patient has had yet

another bout of hypomania, a restless state of insomnia and racing

thoughts.

 

I know bipolars with fairly moderate forms of the illness who have

been on three different atypicals in three years. (There are five

commonly used atypicals; see chart, this page.) They have gone through

multiple dosages of each-and they are usually taking a mood stabilizer

and an antidepressant at the same time.

 

I am not the only bipolar who finds this medication and dosage

switching to be unacceptable.

 

Mental-health experts typically wave away such complaints by saying,

" Each patient is an individual and responds differently to different

medications, and patients must often switch from medication to

medication to find the treatment that works best for them. There are

medications that will work well for you. There is hope. "

 

Doctors, researchers, and advocates have trotted out the same line

since the psychopharmacological revolution hit the American mainstream

about 15 years ago. Its implied promise was that taking new-generation

psych meds would remit symptoms forever. Applied to mood stabilizers

and antidepressants, which have comparatively lesser side effects, the

promise doesn't sound like much more than harmless cheerleading. But

when the same logic is applied to atypicals, it sounds irresponsible

and coldhearted because, with their rotten side effects, they still

fall short of the goal. The name alone tells you that atypicals are a

wholly different class of drugs. All of these meds carry FDA-required

black-box warnings because their use can cause diabetes.

 

Atypical antipsychotics are major juju-a kick in the brain, the purple

pill that puts you on the floor, the white pill that turns your face

stony. Some patients pine for the side effects of lithium and Lexapro,

which are benign by comparison.

 

I say none of this lightly.

 

I've lived with bipolar disorder for 16-plus years. I have taken all

the major medications at one time or another. In that time, I have

interviewed, talked with, counseled, and basically hung out with

hundreds of bipolars, schizophrenics, and depressives. Few of us have

ever seen the promise of the psychopharmacological revolution fully

realized, except for short bursts at a time.

 

Much of what has become standard long-term treatment, or maintenance,

in mental illness is based on short-term studies. The FDA doesn't

require long-term tests in order to license medications. As a result,

most psych meds are typically studied in eight- to 12-week trials.

That tells doctors about patients' short-term response and little

more. There is little incentive for drug companies to fund further

studies. The federal government rarely steps into the breach to fund

long-term studies, either.

 

But most psychiatry involves giving patients drugs for maintenance,

not to bail them out of a short-term crisis. Absent long-term data,

maintenance becomes more of an art than science, though psychiatrists

and doctors don't like to admit that, especially to patients sitting

in their office.

 

There is a disconnect here that makes patients sitting ducks. Their

illness is lifelong not short term.

 

Patients are often downright desperate when they see their doctor,

especially if they've had a recent relapse-one of the most annoying

aspects of the disorder is that symptoms will re-emerge at some point,

even if you strictly adhere to treatment.

 

Besides trying to find a treatment that works, patients are also

trying to placate competing interests. Families and friends press them

to find some kind of medication that works-take anything! Employers

warn they are on thin ice. If they don't find something that works,

then they are likely to be bounced right out of American life.

 

They'll take damn near anything a psychiatrist or general practitioner

suggests to get a short-term result. That's potentially millions of

patients going to their doctors each year looking for something-

anything-that works. Often, these same patients find that the next

something doesn't work, either.

 

Nice psychopharmacological revolution we've got.

 

The irony is that as problematic as atypicals are for bipolars, they

are the best deal schizophrenics have ever seen. Until the 1950s,

schizophrenics were treated in some of the most inhumane ways

imaginable. Tied to a bed for weeks on end. Padded rooms. Lobotomies.

None of that worked very well.

 

Then along came Thorazine, Haldol, and a host of other antipsychotics

that, in many cases, stopped patients' hallucinations, paranoia,

delusions, and violent outbursts. The trouble was that antipsychotics

typically took a huge toll, inducing disabling side effects such as

frozen expressions, shuffling gaits, and shaking limbs- zombieism, in

effect.

 

In 1989, a medication called Clozaril hit the world that caused none

of these physical side effects. It was dubbed " atypical. " But this

medication proved toxic to some patients' immune systems. As a result,

the medication was used sparingly even though it seemed to work better

than the older antipsychotics.

 

By the mid-1990s, newer atypical antipsychotics were introduced. They

didn't have Clozaril's toxicity. Doctors quickly shifted to the new

meds. Within years, atypicals like Zyprexa, Risperdal, and Seroquel

almost completely displaced the older drugs. Patients seemed to do

well on them-no more tremors, no more frozen stares. Many people were

able to get out of state hospitals and restrictive group homes and

live fully realized lives in the community.

 

It was a watershed moment in treating mental illness.

 

In 2000, sales of atypicals reached $3.2 billion. But already

questions had emerged among psychiatrists about just how well these

newer meds performed against older antipsychotics, and whether the

expense was justified. Atypicals are not cheap-the bill for someone

with severe schizophrenia could easily run $1,000 a month, 10 times

more costly than the older drugs.

 

What's more, doctors and patients documented a new series of side

effects from these meds. In particular, patients' blood sugar levels

shot up, cases of diabetes were reported, and patients rapidly gained

weight.

 

The bind for doctors and patients was that there was a complete data

vacuum about just how good these meds were or weren't when it came to

maintaining schizophrenia. Doctors also had questions about whether

the side effects were as prevalent as many in the business feared.

 

In 2001, the NIMH funded a $43 million, 1,400-patient study of the

long-term performance of four atypicals (Zyprexa, Risperdal, Seroquel,

and Geodon) against one old antipsychotic (Trilafon). The CATIE study

was the first long-term study of atypicals in schizophrenics. The

results were published in the New England Journal of Medicine in

September, and generated a fair amount of media attention.

 

That was because 74 percent of the patients discontinued taking their

assigned medication. They either couldn't handle its side effects or

it wasn't working. This was a startling outcome in light of the

decade-long hype around atypicals.

 

The best of the atypicals in this respect was Zyprexa. Only 64 percent

of the Zyprexa patients had to stop taking that drug. Put another way,

only 36 percent of the Zyprexa patients found the drug's performance

justified taking it for 18 months. Among the other drugs, Seroquel had

the worst discontinuation rate at 82 percent. What's more, the newer

meds didn't treat schizophrenia's symptoms much better than Trilafon

did, another surprising outcome.

 

The CATIE study was the shot heard round psychiatry. NIMH went into

overdrive trying to explain to the media that the patients didn't stop

taking meds altogether, but switched to something else. Advocacy

groups put together media calls and stressed that CATIE wasn't an

indictment of an entire class of meds. Pharma companies issued press

releases claiming that their drug was the winner (Eli Lilly's Zyprexa)

and, in one case, that their drug had been used at too low a dosage

(Janssen's Risperdal). The general consensus was that atypicals remain

the best treatment available for schizophrenia no matter how side

effects cloud their use. No one wants to go back to the bad days of

the old antipsychotics.

 

In the media flurry, no one said a word about bipolars, who now make

up 50 percent of the market for atypicals. But there were obvious

implications.

 

As with schizophrenics, the same kind of search for the perfect

combination of meds to remit symptoms of bipolar disorder has been

going on for decades.

 

The disorder is marked by extreme mood swings between delusional

euphoria and psychosis and the black pit of depression. An estimated

15 percent to 20 percent of bipolars commit suicide. Although the

illness was long believed to affect about 3 million Americans, recent

estimates double or triple that figure to between 6 million and 9 million.

 

Bipolar is a tricky illness. It is linked to high levels of

intelligence and creativity, for example. Its effects on personality

are legendary-uninhibited people-seeking (bipolars are often the life

of the party), hypersexuality, and incessant talking, for example.

 

Classically, the disorder is treated with a mood stabilizer. Lithium

was long the gold standard. In recent years, there has been a shift to

anticonvulsants like Depakote or Lamictal. Often, bipolars are also

given an antidepressant like Paxil or Effexor to deal with bouts of

depression. Until 2000, the mood stabilizer plus antidepressant

approach was essentially the state-of-the-art treatment. It just

doesn't knock down symptoms forever.

 

Bipolars can " break through " these meds and wind up having acute

episodes of rage or suicidal depression. Another common breakthrough

symptom is hypnomania, when the mind races so quickly that the patient

cannot sleep for days on end.

 

In response, doctors loaded patients with higher doses of mood

stabilizers and antidepressants. Ten years ago, it wasn't unusual for

a bipolar to end up on 2,500 milligrams of lithium and 60 milligrams

of Prozac a day, both fairly high doses. Patients who didn't respond

at those levels would sometimes be given a small dose of an old

antipsychotic, if their doctor could trust them. The idea was that

patients would use it as needed for a few days until they returned to

baseline. Doctors didn't want patients on antipsychotics for long due

to the risk of giving bipolars the same ugly side effects the drugs

gave schizophrenics. I was one of those bipolars who was prescribed an

antipsychotic, a small dose of Mellaril in my case. I wasn't even

remotely psychotic, in the classic sense of that term. But there was

an angry edge that had crept into my daily life (this was in the

mid-1990s). On occasion, my mind was too ramped up for me to get

anything other than fitful sleep. So, I'd take Mellaril when I was

manic or hypomanic and just fog my brain and sleep. That way, I

wouldn't wind up in a hospital, or doing anything that couldn't be

redeemed.

 

I took 40 milligrams of Mellaril perhaps twice a year. It was never a

pleasant experience. Mellaril made me feel leaden and rendered me

impotent. Once a girlfriend of mine found the Mellaril in my medicine

cabinet. She asked what they were. Nuclear weapons, I told her.

 

Then I developed paranoia in late 2000. This was a new experience for

me, and it dogged me day and night. I knew it had to be addressed

quickly before something irreparable happened. So I went to my doctor.

He asked me what I knew about antipsychotics, and I told him I was no

fan of Mellaril. He suggested the atypical Risperdal. I knew that it

was being used by schizophrenics.

 

" So I take this for a few days? " I figured the deal would be the same

as with Mellaril.

 

" No, you take it all the time, " my doctor answered.

 

" Why? "

 

" It doesn't have the side effects of the old stuff, and you can take

it long term to remit your symptoms. "

 

I'd never heard of antipsychotics being used for maintenance of

bipolar disorder. " Are you telling me I'm schizophrenic? "

 

My doctor told me that his proposal was essentially experimental and

off-label. The drug was unstudied in bipolars, nor was it FDA-approved

for use in bipolar disorder. But he said there was plenty of anecdotal

evidence to support people like me giving it a whirl. And, no, I

wasn't a schizophrenic. So I went to Walgreens and gave it a whirl.

Later, I visited the Risperdal Web site. It was devoted to the drug's

use in schizophrenia. I was a guinea pig.

 

At first, I liked Risperdal. I took it at night along with Depakote

and Wellbutrin, an antidepressant. The paranoia disappeared within

days. Other than that, the drug kept me calm and made me sleep 10

hours a night. I'd be groggy in the morning. I put on 20 pounds, but I

figured it was a small price to pay for ditching that paranoia and

buying some peace of mind.

 

About a year later, my dose went to 1.5 milligrams a day-a baby dose

by schizophrenic standards of 4 to 6 milligrams a day-due to a couple

of episodes of hypomania that had slipped through the Risperdal

curtain. Once again, I had run into the prototypical bipolar complaint

of being unable to sleep.

 

On the higher dose, I felt slowed down and unable to think at my usual

clip. This is a common experience for patients taking atypicals long term.

 

One day, a friend of mine told me that my face had no emotional range.

She said I was fixed and stony when I should've been smiling. After

two years of daily use, the more troubling side effects had blossomed.

Weight gain and grogginess I could handle, but not looking emotionless

to the world. I had taken psych meds each day for the previous 14

years and was more or less stable, so I decided it was time to be a

guinea pig in a whole new way.

 

In the spring of 2003, I went to my then-doctor and told him I wanted

to go off all my meds. I wanted to see what my nonmeds baseline was like.

 

For three months, things went well. I lost weight, my facial

expressions snapped back to life, and my emotions had what seemed like

a normal range. Then the edge returned, and I couldn't sleep. Soon

after, I crashed.

 

My doctor put me back on Depakote and Risperdal. Within a day, I was

so agitated I couldn't sleep and my heart raced. I measured 140 beats

a minute at one point. I had to piss every five minutes and was so

nauseated that I couldn't eat. I almost checked myself into Harborview

Medical Center for monitoring. I had never had that kind of response

to meds of any kind before and I was frightened. When I visited him a

couple of days later, my doctor confirmed my hunch that Risperdal was

the culprit.

 

" Let's replace that with Zyprexa, " he said. I told him no. He gave me

samples in case I changed my mind.

 

Since then, I have continued to chase that edginess and have had

occasional bouts of insomnia. My new doctor and I decided last year

that I ought to try Seroquel. So I began taking the smallest possible

dose.

 

At first, it helped me sleep, although it took about two hours to be

fully alert the next morning. It was as if I had taken a Quaalude and

drank a fifth of whiskey the night before. I didn't like that, neither

did I like putting on weight all over again. Seroquel also caused me

to have bad dreams-horror-film bad-that I would awake from in full

shout. There were mornings where I'd look at myself in the mirror and

see scratches on my forehead.

 

Still, the edge was mostly gone. I liked that. But something about

Seroquel bugged me.

 

Seroquel is very much the med of the moment for treating bipolar

disorder. It is made by AstraZeneca. In the last two years, sales have

more than doubled to $2 billion. Earlier this year, AstraZeneca

officials bragged to investment analysts that they expected more than

30 percent growth in sales in 2005. Recently, the company began an

advertising campaign with banner ads on MySpace.com, the popular

social networking Web site.

 

Right now, it is only FDA-approved for short-term treatment of acute

mania. It is not approved for maintenance treatment of bipolar

disorder, rapid cycling (switching between mania and depression), or

bipolar depression. Doctors are free to prescribe it for those uses,

off-label. Seroquel is now the most prescibed atypical in the U.S.,

according to AstraZeneca.

 

Almost every bipolar I've spoken with has had Seroquel prescribed to

them because they've gone to their doctors complaining of insomnia-the

kind of insomnia that sleeping pills cannot address. Seroquel knocks

down this problem with sledgehammer efficiency. Patients tell me that

they've generally been started at 200 milligrams and then slept well

for a few weeks. Then they cannot sleep again and up goes the dosage.

One patient I know wound up taking 800 milligrams a day-the amount an

acute schizophrenic takes-and still couldn't sleep. That dose of

Seroquel runs $668 a month, according to drugstore.com.

 

All of them put on 20 to 30 pounds in short order. Most of these

patients had already tried one of the other atypicals, if not two or

three, before arriving at Seroquel. Interestingly, many patients I've

interviewed began taking Seroquel in 2003 or 2004. They stuck with it

for about a year, and then switched to something else in 2005 after

the heavy head in the morning became too great of a trade-off. For

this reason, I, too, had to stop taking the drug earlier this year.

 

I wonder what AstraZeneca's executives will be telling investment

analysts in 2006.

 

But the pharma giant recently went into press release overdrive. There

was an academic conference on bipolar disorder in Holland last month.

One study released at the conference claimed that Seroquel was highly

effective in treating bipolar depression based on an eight-week study.

Bipolar depression is a subtype of the broader disorder.

 

In recent interviews, several prominent researchers pointed to that

study as proof of Seroquel's efficacy in treating bipolar disorder.

Some researchers said that it ought to be used long term in bipolars,

as a result-and as the only drug a bipolar would take.

 

The study states that Seroquel worked on the depression of 53 percent

of the patients in the eight-week study. That means it didn't work for

47 percent of the patients. That's tantalizingly close to NIMH's own

assertion that psych meds work only about half the time. It also

dovetails with what patients I know have experienced on atypicals as a

whole-50 percent performance.

 

Half-performance is wholly unacceptable. It certainly doesn't justify

a paradigm shift.

 

The results are even less impressive in light of what Seroquel does to

patients' bodies as well as the expense of the medication. Least

impressive still is that if you are a bipolar taking an atypical like

Seroquel, and you need to be to work at 8 a.m. each morning, then

you'll likely need to take your pills around 9 p.m. the previous

evening. Seroquel will knock you out for a good eight hours, and

you'll need to devote two hours in the morning just to waking up. That

leaves you about four hours in the evening for the rest of your life.

 

And they call this treating bipolar disorder? The doctors think there

is solid evidence that it's a good idea to use these meds for

long-term maintenance? Why do they tout complete symptom remission as

a goal, when it creates an environment where patients, who are in no

position of power, are literally forced to take successively more

powerful meds when doctors themselves know that complete symptom

remission is a fantasy? They are kidding themselves.

 

Much of this shift to atypicals for treating bipolar disorder has gone

on under the noses of the media and advocates for the mentally ill.

Perhaps the questions that need to be asked are too subtle to permit

the kind of black-and-white answers that the media love and that

advocates need.

 

Still, it's puzzling to me that such a vast change could be going on

in the treatment of a major mental illness and the very people who

should be asking the hard questions are mute. Last month, actress

Linda Hamilton was a guest on Larry King Live on CNN. She was

discussing her " 20 years of bipolar hell. " At the top of the show,

King announced that the Terminator star was also there representing

Eli Lilly and their well-being approach-exercise and nutrition-for

" people with serious and persistent mental illness. " In other words,

she was talking to me. Too bad I wasn't asking the questions.

 

King is of course no exemplar of journalistic inquisitiveness. He

didn't ask her if maybe-just maybe-those side effects and all that

weight gain that she was on television saying patients needed to

address were, in fact, caused by products made by Eli Lilly-namely,

Zyprexa and Prozac. He didn't ask how reasonable it was to expect

someone taking Zyprexa (or Seroquel or Risperdal) in high doses to get

out there and exercise and eat good food, as she was saying they must,

when their weight, blood lipids, blood sugar levels, and cholesterol

were shot to hell by Zyprexa. I guess looking to the media and

advocates for cold-blooded honesty and accountability is naive. But

someone ought to be asking serious questions because atypical

antipsychotics have serious problems.

 

The people who most need to be held to account here are not the pharma

companies, however. They are acting much as you'd expect drug

companies to behave-designing drugs, calling half-performance a

victory for patients, and minting money.

 

It's doctors and researchers who must be held accountable. By dint of

their medical degrees, they are supposed to be ethical actors. I am

not convinced that it is ethical to ask millions of bipolars to take

medications long term that work about as well at remitting symptoms as

the old standby of a mood stabilizer plus antidepressant approach.

Their proposed paradigm shift is doubly questionable given the side

effects and hard-core nature of atypicals. Maybe I've become too much

of a skeptic about psych meds, if by skeptical you understand that I

actually expect meds to work and expect long-term treatments that

don't dumb down active, intelligent humans.

 

I still take meds, however. They are a constant in my life and will be

until I die. In fact, I still have a bottle of Seroquel in my medicine

cabinet. It's there for short-term use when I cannot sleep and the

edge dogs me once again, as it will. I'll take the Seroquel just like

I once took Mellaril, for a day or two, here and there.

 

This is an awkward time for mental- health experts, researchers, and

advocates. This month, a peer-reviewed academic paper was published on

the Public Library of Science Web site pointing out that researchers

still have not proved the serotonin-imbalance-in-the-brain hypothesis

of depression. What proof there is, the authors claim, is mostly

circumstantial. Two weeks ago, The Wall Street Journal ran an article

covering the same points in relation to antidepressants. And a pesky

reporter was calling around the country, asking questions about

bipolar disorder and atypical antipsychotics that prominent

researchers hadn't even asked themselves.

 

These are all matters that smart people should be willing to meet head-on.

 

The larger uncomfortable truth about the psychopharmacological

revolution is that psychiatric medications are now part of mainstream

American culture, but these meds do not consistently offer the kind of

long-term benefits that many in the mental-health field claim. Nor do

we fully understand the long-term consequences of their use. This is

as true of antidepressants as it is of atypical antipsychotics.

 

That's a lousy deal for patients, regardless of their diagnosis. It's

doubly lousy because there are no new classes of psych meds on the

horizon. And any talk of gene-based cures and therapies is just talk,

for now.

 

Meanwhile, patients have to live. They have to grapple with illnesses

that are poorly understood scientifically, in an environment where

medications can be as much of a problem as a solution, where

incomplete evidence is the guiding light of long-term care in a

revolution that's forgotten how to serve the patient first.

 

The hell with that.

 

pdawdy

 

 

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Atypical Antipsychotics

 

Drug Manufacturer Black-Box Warning* Year Introduced

Abilify (www.abilify.com) Otsuka America Yes 2002

Clozaril** (www.clozaril.com) Novartis Yes 1989

Geodon (www.geodon.com) Pfizer Yes 2001

Risperdal (www.risperdal.com) Janssen Yes 1994

Seroquel (www.seroquel.com) AstraZeneca Yes 1997

Zyprexa (www.zyprexa.com) Eli Lilly Yes 1996

 

* A special FDA-required warning alerting consumers and doctors to

known side effects of a drug, or class of drugs, owing to documented

deaths or injury.

 

**Due to cases of toxicity, Clozaril (clozapine) is rarely prescribed.

 

 

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1997-2004, Seattle Weekly and Village Voice Media. All

rights reserved.