Hepatitis C Important Treatment Advance:
Interview
with Douglas Dieterich, M.D.
By John S. James
On May 4 the FDA's Antiviral
Drugs Advisory Committee recommended approval of combination treatment
with ribavirin plus interferon alpha for hepatitis C which had not been
cured by interferon alone. Ribavirin, a broad-spectrum antiviral long approved
for oral use in almost every country of the world except the U.S., is expected
to be officially approved and on pharmacy shelves here by this fall. Alpha
interferon is already a prescription drug.
As many as 40% of persons
with HIV are also infected with hepatitis C, which causes many deaths,
and is more serious for those who are HIV-positive than for the general
population. Some HIV physicians are now reporting more of their patients
dying from liver cirrhosis caused by this disease, than from AIDS. It is
estimated that about four million Americans have hepatitis C, but only
about one million know it.
Patients need to know that
hepatitis C might not be properly diagnosed and treated by physicians,
including specialists, who are not experienced in treating chronic viral
infections. Until now the only approved U.S. treatment has been alpha interferon
alone, usually given for six to 18 months; with this treatment, only about
10% to 20% of patients have been cured, but some of the others appear to
have greatly benefited from the drug. ("Cured" means that the hepatitis
C virus becomes undetectable and remains undetectable indefinitely, even
after discontinuation of treatment.) Combination treatment with ribavirin
appears to at least double the cure rate. But many patients who may need
treatment have not been receiving it.
The hepatitis C clinical
trial data so far is from patients who are HIV negative. The first trial
for persons with both infections, sponsored by the American Foundation
for AIDS Research, is starting now in 17 U.S. cities (see announcement
below).
For information on hepatitis
C treatment today we interviewed Douglas T. Dieterich, M.D., Associate
Professor of Medicine at New York University School of Medicine.
A gastroenterologist, Dr. Dieterich also treats patients at Liberty Medical
LLP in New York. He is co-principal investigator of the AmFAR clinical
trial.
Interview with Dr. Dieterich
AIDS TREATMENT NEWS: In the
recent hearing on hepatitis C, what did the FDA advisory committee recommend
for approval?
Dr. Dieterich: The approval
recommendation was for re- treatment of patients who had previously failed
to be cured by alpha interferon alone. The difference in the response rate
was about 4% cure rate in the interferon plus placebo group, and about
48.7% for the interferon plus ribavirin group, for these patients.
ATN: Is the data not available
yet for naive patients? From the HIV experience, it would seem that there
might be even better results with those who were treatment naive.
DD: Actually in the naive
studies, the numbers appear to be about in that 48% range--in the three
smaller studies that have been done.
ATN: What is known about
the benefits for those who are *not* cured--with the combination, and also
with interferon alone.
DD: We do not have data yet
on the combination, but those who were treated with interferon alone seem
to have a much lower risk of getting a hepatoma--a primary liver cancer—related
to hepatitis C. Also, progression to cirrhosis is lower, and their hepatitis
C viral load is lower as well, even after the treatment is stopped. So
there appears to be a positive effect on the immune system.
Diagnosis and Epidemiology
ATN: What about the problem
of cases being missed by the hepatitis C antibody test? Which patients
should also get a hepatitis C PCR test (which looks for the virus directly),
even if their antibody test is negative?
DD: Those at high risk--for
example, a patient who has a history of intravenous drug use, or who has
had a sex partner with a history of IV drug use or a history of hepatitis
C.
ATN: How would you test a
patient with that history, but who also has only a minor liver enzyme elevation,
or even no elevation?
DD: Certainly the hepatitis
C antibody test should be done first. But if that is negative, I think
I would go on to do the PCR. You could use either a qualitative or a quantitative
PCR; for diagnosis, the qualitative PCR is more than satisfactory. When
we are doing studies, we like to do the quantitative test. [A qualitative
test only tells whether or not something is present; a quantitative test
tells how much.]
Also, until 1990 the blood
supply was not tested. So anybody who had a transfusion before 1990 is
at risk for hepatitis C and should be checked. This summer the Surgeon
General is going to start a large campaign to look for these people; there
may be as many as 400,000 in the U.S.
ATN: Does there seem to be
more hepatitis C now than before--or is it just that we did not know about
it before?
DD: The number of new infections
today is mostly from IV drug users. But many cases we are seeing are baby
boomers who were playing around with injected drugs 20 or 30 years ago,
and are now getting diagnosed when they apply for life insurance, etc.
Who Needs More Aggressive
Treatment?
ATN: Which patients are likely
to progress rapidly, and which may be OK for years even without treatment?
DD: It is very hard to predict.
In general we know that people with HIV progress more rapidly than people
without HIV. And people with other immunodeficiencies, like renal failure
or transplant patients, also seem to progress more rapidly. But for patients
without those risks, it is hard to tell.
ATN: So if somebody does
have HIV or other immunodeficiency, that would be an indication to go ahead
with treatment, to be more aggressive?
DD: Absolutely. In addition,
a way to make some sort of prognosis is to do a liver biopsy. The amount
of fibrosis on the liver biopsy shows who is progressing most rapidly toward
cirrhosis.
ATN: What patients should
*not* be treated?
DD: That is not yet clear.
If people are extremely ill with hepatitis, and have decompensated cirrhosis,
the treatment with interferon can certainly make them worse in the beginning.
And people who have coronary artery disease should always have a stress
test before they take ribavirin, which has a side effect of anemia, which
can cause heart problems if somebody becomes very anemic.
And for the most healthy
people--those who are HIV negative, and who have normal SGOT and SGPT [liver
enzymes which are checked by a blood test]--we have been holding off treating
them, for now.
ATN: I understand that the
way hepatitis C progresses is that the virus develops resistance to the
body's defenses?
DD: Yes, relapses occur when
the virus mutates and produces a different quasispecies, and escapes from
lymphocyte control.
Side Effects of Treatment
ATN: How serious are the
side effects of alpha interferon and ribavirin?
DD: Alpha interferon has
many side effects. They can include fatigue, fever, flu-like symptoms,
aches and pains,depression, thyroid problems, weight loss, maybe wasting,
diarrhea, and nausea. With the doses used, people are likely to feel something.
Generally it is not terrible; patients can usually control most of the
symptoms with over-the-counter medicines.
With ribavirin, aside from
the anemia there may a little nausea, similar to the AZT nausea, which
usually resolves.
ATN: What are the usual doses
for both of the drugs?
DD: The AmFAR study is using
3 million units of alpha interferon three times a week, and 400 mg of ribavirin
twice daily.
ATN: Must the ribavirin be
taken on a full or empty stomach?
DD: It does not matter.
ATN: What about treatment
failures? What is the usually pattern of hepatitis C treatment not working?
DD: There are two different
ways we could look at failures. One is complete non-responders, whose PCR
never becomes undetectable. And also there are people who respond and then
relapse, either while on therapy or after discontinuing.
Progress Toward Better Drugs
ATN: Where are we in the
development of new kinds of drugs designed specifically to treat this virus--such
as hepatitis C protease inhibitors, and helicase inhibitors? Are these
several years away?
DD: That may be a realistic
time. Researchers have only recently figured out the structure of the viral
protease. There are no such drugs in trials yet.
Liver Transplants
ATN: There is now a movement
to end the automatic exclusion of persons with HIV from organ transplantation
(see AIDS TREATMENT NEWS #288, February 6, 1998). How often have liver
transplants been used to save the lives of patients with access to them?
DD: Hepatitis C is the number
one reason for liver transplants in the U.S. today. It is rapidly running
away from the other causes.
Finding Good Care
ATN: What advice could you
give on finding proper specialist care--if somebody is at risk for hepatitis
C infection, or has already been diagnosed?
DD: It is important to seek
a physician who understands chronic viral illnesses and their treatment,
and the importance of treatment. Many of the classical referrals have been
to gastroenterologists, many of whom have little or no experience or interest
in treating hepatitis, particularly in HIV patients.
However, there are some gastroenterologists
who are very experienced and knowledgeable--for example, the investigators
in our AmFAR trial. I would certainly recommend these people to anyone.
Among other physicians, there
are many infectious disease doctors who are quite knowledgeable and capable
of treating hepatitis C--and also HIV specialists who are internists or
primary-care docs. These physicians are more likely to understand the importance
of treating this infection, and the viral dynamics of the disease. So we
should not limit our options to just gastroenterologists.
Bibliography
Lai MY, Kao JH, Yang PM and
others. Long-term efficacy of ribavirin plus interferon alfa in the treatment
of chronic hepatitis C. GASTROENTEROLOGY. November 1995, volume 111, number
5, pages 1307-1312.
Chemello L, Cavalletto L,
Bernardinello E, Guido M, Pontisso P, and Alberti A. The effect of interferon
alfa and ribavirin combination therapy in naive patients with chronic hepatitis
C. JOURNAL OF HEPATOLOGY 1995; volume 23, supplement 2, pages 8-12.
Reichard O, Norkrans G, Fryden
A, and others. Randomized, double-blind, placebo-controlled trial of interferon
alpha-2b with and without ribavirin for chronic hepatitis C. THE LANCET
January 10, 1998; volume 351, pages 83-87.
Schalm SW, Brouwer JT, Chemello
L, and others. Interferon- ribavirin combination therapy for chronic hepatitis
C. DIGESTIVE DISEASES AND SCIENCES December 1996 supplement; volume 41,
number 12, pages 131S-134S.
Sherman KE, Sjogren M, Creager
RL, and others. Combination therapy with thymosin alpha-1 and interferon
for the treatment of chronic hepatitis C infection: A randomized, placebo-controlled
double-blind trial. HEPATOLOGY April 1998, volume 27, pages 1128-1135.
Farrell GC, Bacon BR, Goldin
RD, and the Clinical Advisory Group for the Hepatitis C Comparative Study.
Lymphoblastoid interferon alfa-n1 improves the long-term response to a
6- month course of treatment in chronic hepatitis C compared with recombinant
interferon alfa-2b: Results of an international randomized controlled trial.
HEPATOLOGY April 1998, volume 27, number 4, pages 1121-1127.
Heathcote EJL, Keeffe EB,
Lee SS, and others. Re-treatment of chronic hepatitis C with consensus
interferon. HEPATOLOGY April 1998, volume 27, number 4, pages 1136-1143.
Zeuzem S, Lee JH, Franke
A, and others. Quantification of the initial decline of serum hepatitis
C virus RNA and response to interferon alfa. HEPATOLOGY April 1998, volume
27, number 4, pages 1149-1156.
Donaghy A, Ross R, Wicks
C, and others. Growth hormone therapy in patients with cirrhosis: A pilot
study of efficacy and safety. GASTROENTEROLOGY 1997; volume 113, pages
1617- 1622.
Hepatitis
C and HIV: Ribavirin Plus Interferon Study Recruiting
AmFAR (the American Foundation
for AIDS Research) is now beginning the first study of treating hepatitis
C in persons who also have HIV. Trial sites are now opening in 14 U.S.
cities, and a few others may be added.
Volunteers will be randomly
assigned to either interferon alpha-2b plus ribavirin, or to the interferon
alone (plus a ribavirin placebo). However, those assigned to monotherapy
who have detectable virus at week 12 will be assigned to combination treatment
starting at week 16; this assignment will be blinded, so volunteers will
not know if their regimen has changed. The drug treatment period will last
for 48 weeks, with followup for 28 weeks after that.
Volunteers must be HIV-positive
and have hepatitis C disease, be at least 18 years of age, and been on
stable FDA-approved treatment for HIV (or on no treatment for HIV) for
at least four weeks. This study does not have CD4 count or HIV viral load
requirements. However, there are 29 exclusion criteria (mostly for specific
medical conditions or medications)-- which may make it difficult to recruit
the 200 volunteers being sought.
Also, this trial will only
pay for the ribavirin and the hepatitis C viral load tests; volunteers
are responsible for the other costs. For those unable to afford the interferon,
it is being made available through Schering Plough's patient assistance
program. (Schering Plough, which has the rights to distribute ribavirin
for hepatitis C in the U.S. and which also markets interferon alpha-2b,
is providing partial funding for this study.)
The trial will be conducted
at medical centers in the following cities:
East: Baltimore, Hershey,
Newark, New York, Philadelphia, Providence;
South: Atlanta, Chapel Hill,
Miami;
Midwest: St. Paul, Wichita;
West: Los Angeles, Portland,
Sacramento.
AmFAR also hopes to open
about three more sites in other cities, including San Francisco.
‘
For more information, call
Jeffery Smith at AmFAR, 602-340- 1207, who can discuss the trial in more
detail and refer you to one of the sites listed above.
Metabolic
Changes: Concerns About Heart, Circulatory Risks
By John S. James
A May 2 research letter in
THE LANCET, by AIDS, lipid, and cardiology specialists at Regions Hospital
in St. Paul and the University of Minnesota Medical School in Minneapolis,
highlighted growing concerns that high cholesterol and other metabolic
changes being seen in some HIV patients may be increasing the risk of heart
and circulatory disease.(1) The letter was prompted by two cases of unusual
coronary artery disease in young men being treated with protease inhibitors;
there has since been a third case. These incidents led to a chart review
of 124 patients on protease inhibitors, which found that 33% of them had
high enough lipid (fat) concentrations in their plasma to be referred for
treatment, either with diet and exercise or with lipid-lowering drugs.
The Regions Hospital HIV
clinic has developed interim recommendations, including getting baseline
blood tests before starting protease inhibitors, lifestyle changes such
as improved diet and stopping smoking, and treatment when necessary according
to the U.S. National Cholesterol Education Program (NCEP) guidelines for
lowering cholesterol in patients with heart disease.(2)
In a phone conversation on
May 11, lead author Keith Henry, M.D., explained why this problem may be
more important than some have realized:
Cardiovascular disease usually
develops over decades; this is why heart attacks usually happen to people
who are older. If this process is accelerated in some HIV patients—either
because of the virus, or because of some the drugs used to treat it--damage
could be happening now which could show up increasingly over the next few
years. The Regions Hospital HIV Clinic has not had any deaths from heart
problems yet, but Dr. Henry has heard of cases from other physicians.
* High cholesterol
levels may be a bigger problem than widel realized, since in many
of these patients the triglycerides are also high, which can prevent the
cholesterol from being measured accurately. But the plasma from many patients
"looks like thick cream." The abnormal fat which may be contributing to
cosmetic changes in some patients is carried through the circulation, with
unknown effects on parts of the body which are not seen. And a modest total
cholesterol elevation can be worse than it looks, because it often consists
of a combination of an increase in LDL cholesterol (the "bad" cholesterol)
and a decrease in the HDL cholesterol (the "good" cholesterol).
* Lifestyle problems,
including smoking, poor diet, and lack of exercise, are likely to increase
the risk further. Many patients are not on good diets, since in the past
the goal has been just getting calories in.
* There are interim
measures which can be taken now. The Regions Hospital clinic obtains a
fasting lipid profile before starting patients on protease inhibitors,
and then 3-6 months after. Abnormalities are treated according to the NCEP
guidelines--just as the same conditions would be treated in HIV-negative
persons with heart disease.
References
1. Henry K, Melroe
H, Huebsch J, and others. Severe premature coronary artery disease with
protease inhibitors. THE LANCET May 2, 1998; volume 351, page 1328.
2. National Institutes of
Health. CHOLESTEROL LOWERING IN THE PATIENT WITH CORONARY ARTERY DISEASE:
Physician Monograph-- National Cholesterol Education Program. September
1997 (NIH Publication 97-3794). This document is available at: http://www.nhlbi.nih.gov/nhlbi/cardio/chol/prof/chol_low.htm
NTZ:
Advisory Committee Votes Against Approval
By John S. James
On May 6 the FDA's Antiviral
Drugs Advisory Committee voted 9-1 against approval of NTZ for treatment
of cryptosporidiosis, which causes severe diarrhea in persons with AIDS.
The one community representative on the panel, Michael Marco of the Treatment
Action Group (TAG), cast the vote for approval. A number of treatment activist
and patient groups (including AIDS TREATMENT NEWS) had urged that NTZ be
approved, despite disappointment that better data was not available. "Even
though the quality of data UNIMED has presented is marginal, undeniably
there is a documented clinical response with an excellent safety profile"
(quoted from the consensus letter).
A government-sponsored placebo-controlled
trial (ACTG 336) was supposed to provide the most important data to support
the approval. But this study was closed recently when it proved impossible
to enroll. Sixty volunteers were needed, but only 10 had entered in 15
months. The main reason the ACTG trial could not recruit is that peoples'
health has greatly improved as a result of the new combination antiretrovirals,
reducing the incidence of cryptosporidiosis to a fraction of what it used
to be. Also, the trial was unattractive because volunteers had to remain
untreated until a positive diagnosis was made, and then risk being assigned
to a placebo for the first part of the treatment period.
The FDA acknowledged that
it would not be possible to get placebo-controlled data for this drug,
and invited the company to submit the results it had. FDA analysts could
not find proof of efficacy in the company's data.
NTZ, which "has the broadest
spectrum of antiparasitic activity ever achieved with a single drug"(1),
is chemically related to metronidazole (Flagyl), but does not have the
severe side effects of the latter. Since NTZ is only partially absorbed
from the gut, it is most likely to be useful against pathogens in the intestines.
Almost everyone familiar with this drug believes that it does have activity
against cryptosporidiosis--although this parasite is difficult to cure
in many cases, possibly because it can get into places where NTZ cannot
reach it well. In these cases, treatment may need to be continued. Also,
there is still disagreement and confusion about the best strategies for
dosing NTZ.
For background on NTZ, see
AIDS TREATMENT NEWS #239 (January 19, 1996), #250 (July 5, 1996), #258
(November 1, 1996), and #288 (December 6, 1997).
Comment
We are concerned about the
future of NTZ for several reasons:
* A significant number of
people will still need this drug. It is approved in Mexico and available
there, but most U.S. patients who need NTZ will not know about it, or be
able to obtain it easily.
* NTZ may have major uses
aside from cryptosporidiosis. It appears to be effective for microsporidiosis
as well, although no trial has been done. It may also be an important contribution
against giardia and other parasites which can be difficult to treat in
some cases, even though there are approved drugs available.
* Diarrhea caused by parasites
is often difficult to diagnose--especially in cost-constrained public clinics
or managed-care settings. Patients and physicians should have the option
of trying a broad-spectrum treatment which may be effective against organisms
which, for various reasons, could not be identified.
What should be done now?
Clearly a controlled trial for cryptosporidiosis is not feasible today--as
the FDA, and most of the members of its advisory committee, apparently
recognize. What seems to have gone wrong in this case is that once the
classical placebo-trial model was rejected, the development of this drug
was on new, unfamiliar ground—and the company did not get the guidance
it needed on how to operate in this new environment in a way that would
develop data useful for the regulatory process.
We are preparing a separate
article on study designs that would be appropriate for NTZ today--or for
similar situations when they occur in the future.
References
1. Dubreuil L, Houcke I,
Mouton Y, and Rossignol JF. In vitro evaluation of activities of nitazoxanide
and tizoxanide against anaerobes and aerobic organisms. ANTIMICROBIAL AGENTS
AND CHEMOTHERAPY October 1996; volume 40, number 10, pages 2266-2270.
Update on AIDS Wasting and Lipodystrophy: One-Day Seminar in Geneva, June
28
"Update on Wasting,
Metabolism, and Altered Body Shape in HIV/AIDS," a one-day seminar for
health professionals co- sponsored by Tufts University School of Medicine
and the U.S. National Institute on Drug Abuse, will take place immediately
before the 12th World AIDS Conference in Geneva, Switzerland, at the Hotel
President Wilson. There is no charge for this program, but preregistration
is requested. For those who cannot attend in Geneva, a summary will be
posted on the Internet one week after the conference. Funding is provided
by unrestricted educational grants from Serono Laboratories, Inc., and
Bristol-Myers Squibb.
Topics covered include:
hypogonadism, metabolic abnormalities, protease inhibitor associated lipodystrophy
(8 a.m. to 10:30 a.m.); dietary considerations, micronutrients, anorexia,
and protein-energy undernutrition (10:50 a.m. to 12:00 noon); and nutritional
support, testosterone and analogs, resistance exercise, growth hormone,
and other therapeutic approaches (1:15 p.m. to 4:00 p.m.). Each of the
three sessions consists of several talks by experts, followed by a panel
discussion. Speakers include Drs. Donald Kotler, Carl Grunfeld, Marianna
Baum, Steven Grinspoon, Morris Schambelan, and Marc Hellerstein.
More information and online
registration is available at the HealthCare Communications Group site,
http://www.healthcg.com/hiv;
the summary will also be available on this site. A registration form can
also be faxed to 617-636-0472.
Geneva
Conference: Call for Alternative and Traditional
Healing
Practices Material
The Global AIDS Program
of the National Council for International Health (NCIH), in Washington,
D.C., is helping to organize a symposium on "Alternative and Traditional
Healing Practices" for the 12th World AIDS Conference (Geneva, Switzerland,
June 28 to July 3, 1998).
The symposium program will
include: Research and Traditional Medicine (What has been documented? Have
the findings been distributed? How are the findings put to use?); Traditional
and Herbal Medicines (examples of what is being used and requested in selected
communities); Collaboration Between Traditional and Modern Medical Practitioners
(How have collaborative projects been organized? What are the benefits
of these collaborations?); and Life Philosophy (Spiritual practices, self-empowerment,
meditation, relaxation, etc.).
If you have materials available
for distribution at this symposium, please contact Mr. Mohcine Alami at
NCIH, 202-833-5900, fax 202-833-0075, email ncihaids@ncihaids.org,
by May 31 if possible.
AIDS
Vaccine: Major Report Available
On May 18 the AIDS Vaccine
Advocacy Coalition will release 9 YEARS AND COUNTING, a 53-page agenda
for action and report on the status of AIDS vaccine development.
The title refers to a speech one year ago by President Clinton, in which
he asked, "Today, let us commit ourselves to developing an AIDS vaccine
within the next decade... I am prepared to do all I can to make it happen."
But today, "the government's AIDS vaccine research program has continued
at the same unhurried pace as before with only nominal achievements and
developments, and corporate commitment is at an all-time low" (from AVAC
press release accompanying the report).
Every day 16,000 people are
infected with HIV, and experts agree that only a vaccine will be able to
stop the epidemic. A previous AVAC report found that pharmaceutical and
biotech representatives agreed that "sustained political leadership by
the President, Vice President and the rest of the administration, and scientific
leadership by the NIH" was needed. But "this has not yet happened." The
new report includes a 19-point agenda for action, including the U.S
government, private industry, and international organizations.
Copies of the report will
be available at http://www.vaccineadvocates.org,
http://www.thebody.com,
or
http://hivinsite.ucsf.edu.
Or contact the AIDS Vaccine Advocacy Coalition, P.O. Box 40190, San Francisco,
CA 94140- 0190, phone 415-643-3534, fax 415-821-9131, email avacscott@aol.com.
AIDS Treatment News
Published twice
monthly
Subscription and Editorial
Office:
P.O. Box 411256
San Francisco, CA 94141
800/TREAT-1-2 toll-free
U.S. and Canada
415/255-0588 regular office
number
Fax: 415/255-4659
Email: aidsnews@aidsnews.org
Editor and Publisher: John
S. James
Associate Editor: Tadd T.
Tobias
Reader Services: Tom Fontaine
and Denny Smith
Operations Manager: Danalan
Richard Copeland
Statement of Purpose:
AIDS TREATMENT NEWS reports
on experimental and standard treatments, especially those available now.
We interview physicians, scientists, other health professionals, and persons
with AIDS or HIV; we also collect information from meetings and conferences,
medical journals, and computer databases. Long-term survivors have usually
tried many different treatments, and found combinations which work for
them. AIDS Treatment News does not recommend particular therapies, but
seeks to increase the options available.
ISSN # 1052-4207
Copyright 1998 by John S.
James.
? Permission granted for
noncommercial reproduction, provided that our address and phone number
are included if more than short quotations are used.
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