Dying medicine boss: 'Drug trials are pointless ...and unethical'
Exclusive: Volunteers stand little chance of recovery
Treatments kept from public
Companies scupper rivals
By Sarah-Kate Templeton, Health Editor
source: Sunday
Herald
For the past 40 years Professor David Horrobin has been developing new
medicines. In 1977 he
founded Scotia Holdings, which was once one of Scotland's most promising
biotechnology firms.
But today, as the drug company boss is dying of cancer, he has decided
to expose the
unethical experiments that his industry carries out on patients.
Horrobin reveals that patients recruited to clinical trials are prescribed
highly toxic drugs
with serious side effects, while they stand little chance of benefiting
personally. He says that
only around one in 30 patients on trials will respond positively to treatment,
but that
participants are not informed of this slim hope.
Horrobin, who is currently chairman of Stirling-based firm Laxdale Ltd,
which develops new
psychiatric drugs, claims that pharmaceutical companies even deliberately
recruit more
patients than they need for trials so that there are too few sufferers
left for competitors to
test rival drugs.
He also reveals that promising cancer treatments are not available to patients
because, unless
they are a completely new compound and qualify for a patent which will
secure profit from
their sale, no company will pay for them to go through the lengthy trial
process.
Two years ago Horrobin was diagnosed with lymphoma, cancer of the lymph
tissue. As the
cancer was at an advanced stage, he was told that he could not realistically
expect to live
more than six months.
In a paper in the Lancet medical journal, which was fast-tracked for urgent
pub lication, he
writes: 'I entered a universe parallel to the one in which I had lived
for 40 years. I became a
patient and suddenly saw everything from the other side. I discovered a
whole new attitude to
clinical trials and experimental treatments.
'I believe that patients who are asked to volunteer for large trials in
cancer or other lethal
diseases are being misled. Most such trials cannot be justified on ethical
grounds.'
He points out that large trials are needed to show up a small improvement
on present
treatments.
'If a trial has to be large, say more than 100 patients, it is large only
because the expected
effect size is very small. That means that most patients entering the trial
have little or no
chance of receiving benefit. With the toxic nature of many oncology [tumour]
treatment
regimens, there may well be a substantial chance of harm. Although the
risk of harm is usually
well described in patient inform ation leaflets, almost nothing adequate
is ever said about the
assumed effect size and the real chance of benefit. Almost all patients
volunteering for most
trials in oncology are doomed: at best they can expect little benefit.
They are not usually being
properly told about this low expectation.'
As a cancer patient, Horrobin came to the conclusion that it was not necessarily
in the best
interests of the sufferer to take part in trials. 'In view of the frequently
severe adverse
events, usually much more predictable and reliable in their occurrence
than ... a therapeutic
response, a decision on the patient's part not to be treated is not irrat
ional. I learned that
few patients are made aware of this fact: that is unethical.
'Patients with lethal diseases want to get better, not to have their lives
extended by a few
weeks or months at great cost in toxicity and time in treatment.'
The most damning alleg ation in Horrobin's paper is that pharmaceutical
companies actually try
to sign up as many patients as possible to their trials so that competitors
have difficulty
finding sufferers to test rival drugs. Speaking from the Western General
Hospital in Edinburgh
where he is currently undergoing treatment, Horrobin insisted he had been
present at
industry meetings where this unscrupulous practice had been discussed.
'For the past 20 years I have been working in the pharmaceutical industry.
Although everyone
in the industry will deny it, and I doubt whether there is documentary
evidence of this
statement anywhere, I know that several of the larger firms use overpowered
trials as a way
of keeping competitors out of that particular subject. Especially with
less common cancers, if
a company, by manipulating the power cal culations, can recruit for a trial
several times more
patients than is necessary, then they will gain a clear competitive advantage
by making it
more difficult for rivals to recruit.'
Horrobin addded that hospitals conducting clinical trials for pharmaceutical
firms profit
financially from the experiments -- without necessarily telling the patients.
'Most patients entering most oncology trials will be dead before the results
are known. But the
institutions in which they are being treated probably benefit greatly financially.
Most patient
information leaf-lets do not tell them either fact. This omission is unethical.
'I cannot find any patient information which states that the hospital will
benefit from that
patient taking part in the trial and by how much. This could be between
£3000 and £20,000 per
trial.'
Putting new medicines through trial is expensive, and the costs are covered
only when the
drug can be sold at a high profit. If a medicine is not considered novel
enough to be granted a
patent, guaranteeing a high price when it comes on the market, it will
not be financially
worthwhile pursuing. Unprofitable but helpful ther apies are therefore
denied to patients, says
Horrobin.
The former professor of medicine at Montreal University says his knowledge
has allowed him to
access medicines that would not be available to most patients.
'The high cost of large trials means that they can be done only on patent-protected
new
chemical entities. Since such companies have to seek a return for investment,
trials will be
conducted for only a tiny part of the wide range of potential cancer therapies.
Cancer
patients are, of course, not told that such a small part of potential therapies
is open to them.
'The Western General has collaborated with me completely. I have had no
difficulty using the
treatment I wanted -- but I have a special position in that I am running
a pharmaceutical
company.'
Charles Warlow, professor of medical neurology at Edinburgh University
and a consultant at
the city's Western General hospital, is a staunch advocate of clinical
trials. But even he admits
he refused to take part in a clinical trial himself when he was diagnosed
with colon cancer.
'I declined to be randomised in a trial of chemotherapy after my carcinoma
of the colon was
removed seven years ago. I was too frightened by the side effects of the
new treatment and
didn't think the risk could be worth the likely benefit so I stuck with
the old treatment. So far
so good.
'The problem is that if a benefit is very small, does it offer anything
to patients and is it worth
the side effects of treatment? It depends. If there is a very small benefit
it may be worthwhile
if the drug is cheap, easy to take, and there are no or very few side effects
-- like aspirin to
prevent another stroke in a stroke survivor. Yet with some cancer drugs
there may only be a
small advantage, allowing patients to live for just a few weeks or months
longer, but they may
have to put up with some pretty toxic side effects. In that case it may
not be worth it and I
don't know if patients are always informed of that -- although I myself
certainly was.'
Warlow added that patients in clin ical trials generally get better care
than those in routine
practice because they are closely followed up by doctors.
Jim Eadie, director of the Association of the British Pharmaceutical Industry
in Scotland, said:
'Clinical trials are essential to develop new and better treatments for
patients, and play a
crucial part in ensuring that the UK and Scotland are at the forefront
of the development of
modern treatments and research.
'It is important that trials involve as many patients as possible in order
to obtain the most
accurate, scientifically valid data. Companies carry out multi-centre clinical
trials all over the
world and are not restricted to seeking patients only in the UK. It is
therefore impossible for
any single company to sign up all patients with a particular condition
for its clinical trial work.
'It is true that sometimes medicines may be withdrawn at a late stage in
development, but this
will invariably be because of problems assoc iated with safety and efficacy,
not because of
imminent expiry of patent life.' |