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Fwd: THE MOSS REPORTS Newsletter (05/29/02)

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Note: forwarded message attached.

 

 

 

 

- Official partner of 2002 FIFA World Cup

http://fifaworldcup.

 

 

--

Ralph W. Moss, Ph.D. Weekly CancerDecisions.com

Newsletter #37 05/29/02

-----------

 

 

Report from ASCO: Trials and Tribulations of a New

Cancer Drug

 

 

 

Everything about the 38th Annual Meeting of the

American Society of Clinical Oncology (ASCO) was huge.

There were 26,000 attendees, including 19,000

oncologists, many of whom came from Europe, Latin

America and Asia. For nearly a week in mid-May they

converged on the Orange County Convention Center in

Orlando, Florida, rushing to hear thousands of

lectures, seminars and presentations. The Exhibition

Hall was a multistoried bazaar of new therapies, each

vying for the attention of those who prescribe drugs to

cancer patients. Even the press room was gargantuan,

with row after row of telephones and computers, and

reporters busily filing stories for their newspapers,

TV and radio stations, and websites.

 

 

 

Yet, after four days, I came away with a hollow

feeling. There were incremental advances, to be sure.

But overall, I was disappointed by the lack of

breakthroughs in the treatment of cancer. Other

observers expressed a similar disappointment. One

veteran science writer told me this was the most

unsatisfactory cancer meeting he had ever attended, with

an almost total lack of exciting results.

 

 

 

One of the highlights of the ASCO meeting was the 2002

Karnofsky Lecture, " Targeting the EFG Receptor for

Cancer Therapy, " by John Mendelsohn, MD. Dr. Mendelsohn

is the president of the M.D. Anderson Cancer Center in

Houston and has had a distinguished medical career.

Listening to him speak, I caught some of his excitement

and could see why he was chosen to receive this high

honor from his peers. Dr. Mendelsohn's speech,

concerning the science behind a new drug called Erbitux

(formerly known as IMC-C225), was enthusiastically

received by an overflowing crowd.

 

 

 

Carefully targeted drugs like Erbitux are central to

the oncology profession's latest strategy for

conquering cancer. As the director of the National

Cancer Institute, Andrew von Eschenbach, MD, said in

another lecture, these newer drugs mark a transition

from the " seek and destroy " strategy of 20th century

chemotherapy to the " target and control " strategy of

the 21st, from " weapons of destruction " to

" interventions for control and prevention. " In

principle, advocates of complementary and alternative

medicine (CAM) support such a development, since it

represents a departure from the slash-burn-and-poison

school of conventional cancer treatment. There are side

effects of Erbitux, but they are relatively mild, and

consist mainly of an acne-like rash. Who in their right

mind wouldn't want these new drugs to succeed?

 

 

 

Dr. Mendelsohn was a pioneer in using monoclonal

antibodies, or " guided missiles, " to block the growth

of cancer cells. As early as 1983, he and a colleague

suggested that tumors could be prevented from growing

by blocking the receptors for growth factors that lie

on the surface of cancer cells. It was an elegant

concept. The primary outcome of their work was the

development of Erbitux, which targets epidermal growth

factor (EGF) receptors. EGF is present in all cells

that line our organs and skin, and high levels of EGF

have been found to correlate with a poorer prognosis

for cancer patients.

 

 

 

Preliminary research looked highly promising, and the

alleged " proof of principle " came with the clinical

trial of Herceptin, a drug that targets a molecule very

similar to the EGF receptor identified by Dr.

Mendelsohn. In 1995, Dr. Mendelsohn and his colleagues

claimed that 10 percent of patients with advanced

cancer who were treated with Herceptin had a clinical

response. Seemingly, a new era in cancer treatment was

born. At the 2001 ASCO annual meeting, the manufacturer

of Erbitux, ImClone Systems, claimed a 22.5 percent

response rate in patients with advanced cancer treated

with a combination of Erbitux and chemotherapy. The

jubilation at ASCO culminated in a Doobie Brothers

concert that ImClone sponsored for the doctors

attending the conference.

 

 

 

In his lecture this year, Dr. Mendelsohn, who serves on

the board of directors of ImClone, naturally emphasized

the positive aspects of Erbitux. He mentioned a

clinical trial involving six patients who had

previously been failed by conventional treatment: when

these patients were treated with a combination of

Erbitux and cisplatin, three had complete responses and

three had partial responses. This 100 percent response

rate may sound fantastic. However, a " response " does not

imply a cure or even a prolongation of life.

" Responses " are simply tumor shrinkages, which can last

as little as one month. Ultimately, the most meaningful

measurement of a therapy's effectiveness is its impact

on quality of life and overall survival. But meaningful

data about survival can only be derived from phase III

randomized controlled trials (RCTs).

 

 

 

The world's first phase III clinical trial of Erbitux

was reported at ASCO 2002 a few days after Dr.

Mendelsohn's inspiring speech. In it, the standard drug

cisplatin was compared to combination therapy using

cisplatin and Erbitux in the treatment of head and neck

cancer. The results were less than stellar. Just one

patient out of 44 (2.3 percent) achieved a complete

response and five (11.4 percent) had a partial

response. The median disease-free survival for the

group as a whole was 6.7 months and the median overall

survival was just 7.2 months.

 

 

 

More details were given in a company press release. It

turned out that the response rate, poor as it was,

enclosed an even more sobering reality: the response

rate among so-called " real world " patients (patients

who received their treatment outside the rarefied

atmosphere of clinical trials) was just 5.7 percent.

And that was a measurement of tumor shrinkages, not

survival.

 

 

 

The trial's investigators had hoped to show that

patients in the Erbitux-added group would experience a

doubling of their progression-free survival compared to

the cisplatin-alone group. That didn't happen. For the

Erbitux-added patients, the median time until the

tumors worsened was just 4.10 months, compared to 3.37

months for the control patients. This difference of

three weeks was not statistically significant.

Scientists reluctantly concluded that there were " no

meaningful differences between the two groups in terms

of progression-free survival or overall survival, "

according to an ImClone press release.

 

 

 

So, while on Saturday oncologists were applauding Dr.

Mendelsohn for his brilliant insights, on Monday they

were hearing that a treatment based on these insights

simply did not work. If it were true that EGF " plays a

critical role in the process that regulates tumor cell

growth and survival, " as ImClone still claims on its

website, then one would expect a treatment that targets

EGF to yield significant clinical results. It doesn't.

 

 

 

All this shows the danger of judging new cancer

treatments by the elegance of the theory behind them. I

am reminded of the 1959 statement of Dr. David

Karnofsky (after whom the Karnofsky Lecture is named):

" The relevant matter in examining any form of treatment

is not the reputation of its proponent, the

persuasiveness of his theory, the eminence of its lay

supporters, the testimony of patients, or the existence

of public controversy, but simply...does the treatment

work? " Karnofsky was criticizing what he characterized

as " cancer quackery, " but his words apply equally well

to conventional treatments, especially those that are

over-hyped by Wall Street.

 

 

 

Because of the weak performance of Erbitux, the FDA

(much to the credit of its evaluation committees) has

refused to approve it. This has led to a crisis for its

manufacturer, ImClone Systems. The company's stock,

which traded at $75 per share at the end of last

year, now hovers around $10. In the wake of the ASCO

meeting, the president and CEO, Samuel Wachsal,

resigned all his posts. (His brother, Harlan Wachsal,

took over as CEO.) According to CBS Market Watch,

" The most significant challenge for ImClone will be

finding a way to revive its troubled application to

market the anti-cancer drug Erbitux. "

 

 

 

ImClone may have other troubles, as a congressional

panel is investigating trading in ImClone stock by

Wachsal family members. The problems besetting this

biotech firm have even dragged down the stock of the

giant Bristol-Myers Squibb, which last year paid $2

billion for the right to co-market Erbitux. Bristol-Myers

is said to blame Samuel Wachsal's aggressive personality

for Erbitux's troubles. However, a more serious problem

facing ImClone and other biotech firms involved in

high-stakes cancer research is the lack of

effectiveness of their innovative therapies, especially

in extending life. Wall Street's biotech bubble is

bursting.

 

 

 

What are the lessons for patients and their advocates?

First, we should not get caught up in the hysteria

surrounding new cancer treatments. A great theory, an

impressive board of directors, and a well-oiled

publicity machine are no substitute for randomized

controlled trials that demonstrate convincingly a

cancer therapy's effectiveness.

 

 

 

We should be especially wary of drugs that are heavily

touted by Wall Street. The memory of the Enron debacle

is still fresh. (Coincidentally, Dr. Mendelsohn, who is

on the board of directors of ImClone, is also a member

of the executive committee of Enron's board of

directors.) According to ASCO's disclosure statement,

some of those involved in the current clinical trial of

Erbitux received honoraria and funding from Bristol

Myers-Squibb and own stock or serve on the board of

ImClone. The search for a magic bullet for cancer is

understandable, but it detracts attention from the

study of approaches that actually extend the lives of

cancer patients while maintaining or improving their

quality of life. It also detracts attention from cancer

prevention strategies using natural and nutritional

substances. These less toxic (and less expensive)

approaches represent for me the real promise of cancer

research.

 

 

 

Next Week: The CAM Symposium at ASCO

 

 

 

Here at the Moss Reports

 

 

 

We are busy maintaining and improving our nearly 200

reports on cancer diagnoses. We are also planning major

improvements in our website, which we will reveal

shortly. I continue to work on my book on radiation

therapy, which will apply the standards of

evidence-based medicine to this supposedly " proven "

therapy.

 

 

 

---Ralph W. Moss, Ph.D.

 

 

 

Sources

 

Burtness BA, et al. Phase III trial comparing cisplatin

© + placebo to C + anti-epidermal growth factor

antibody (EGF-R) C225 in patients (pts) with

metastatic/recurrent head & neck cancer (HNC). ASCO

2002 Abstract #901.

 

Karnofsky DA. Cancer quackery: its causes, recognition

and prevention. The American Journal of Nursing, April

1959.

 

More details on ASCO at:

http://virtualmeeting.asco.org/vm2002/default.cfm

 

On ImClone:

http://www.thestreet.com/tech/adamfeuerstein/10023148.html

 

---------------

IMPORTANT DISCLAIMER

 

 

The news and other items in this newsletter are

intended for informational purposes only. Nothing in

this newsletter is intended to be a substitute for

professional medical advice.

--------------

 

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