Subject: AIDS Treatment News #118
Date: Jan 04 1991 (711 lines)      

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J O H N   J A M E S  writes  on  A I D S
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copyright 1991 by John S. James;
permission granted for non-commercial use.


AIDS TREATMENT NEWS Issue #118, January 4, 1991
     phone 415/255-0588

CONTENTS:  [titles are preceded by "*****"]

New Merck Antivirals in Human Tests

ddC/ddI Approval Update

Aspirin Update:  Warning, Promise, and Call for Information

Women and AIDS Conference Report

Announcements:  Women and AIDS San Francisco meeting;
National AIDS Update Conference postponed; Federal AIDS/HIV
care guidelines project; Arab nations AIDS conference



*****

New Merck Antivirals in Human Tests

     Merck & Co. is conducting human trials on two new
antivirals, known as L-697,639 and L-697,661.  The trials began
in Europe about a month ago, and are about to begin at the U. S.
National Institutes of Health in Bethesda, Maryland.  According
to a Merck spokesman quoted in the Los Angeles Times (December
22, business section), company scientists screened 23,000
compounds to find these two, then moved them from the laboratory
to human tests in the remarkably short time of six months.  An
NIH spokeswoman quoted in the same article said that 40
asymptomatic HIV positive volunteers were enrolled in the study
at NIH.

     These drugs are non-nucleoside RT inhibitors -- that is,
they block the enzyme reverse transcriptase (RT) without also
being nucleoside analogs -- false building blocks of DNA. AZT,
ddC, and ddI are RT inhibitors which are nucleoside analogs.  It
is hoped that non-nucleoside drugs can be found with very little
toxicity- -since the enzyme reverse transcriptase is found only
in retroviruses and has no use in the human body, while
nucleoside analogs can in some cases affect human DNA. Other
non-nucleoside RT inhibitors are the new Boehringer Ingelheim
drug BI-RG-587 discussed in AIDS TREATMENT NEWS #117, and the
class of drugs called TIBO derivatives being developed in Europe
by Janssen.

     We have heard that other companies have one or more non-
nucleoside RT inhibitors in pre-clinical development, but have
not announced them.  Reverse transcriptase appears to be a
practical target for anti-HIV drug development, since the enzyme
is well known and chemicals to block it can presumably be
screened by laboratory assays, without the special laboratory
facilities needed for handling live virus.  It is important that
more of these potential treatments be tested, since only one drug
in five which enters human trials ever reaches marketing
approval.


*****

ddC/ddI Approval Update

by John S. James

     Much AIDS news today concerns the campaign for a rapid FDA
evaluation of the experimental AIDS antivirals ddC and ddI -- the
issue we listed as the most important treatment development to
watch in 1991 (AIDS TREATMENT NEWS #117, December 21, 1990).  The
decisions now being made will affect not only these drugs, but
all critically important AIDS antivirals in the future; they will
determine whether any future AIDS treatment, no matter how well
it may work, could possibly travel the development and regulatory
pipeline without many months or years of medically unnecessary
delay.  We are now seeing the beginnings of major changes; but at
the same time there is widespread confusion, and sometimes
chaotic miscommunication.

     The meaning of the current controversies cannot be
understood without background on the situation which now exists,
and how it developed.

Background:  The Problem

     Neither ddC or ddI are new; both could have been developed
and approved at about the same time as AZT.  ddC was delayed
because of early toxicity; it was not known until later that the
right dose was about 200 times less than the dose of AZT or ddI.
As for ddI, it was well into human trials two years ago -- and
the subject of a loud and sometimes bitter public dispute between
Ellen Cooper, M. D., chief of the FDA's Division of Antiviral
Drug Products, and Samuel Broder, M. D., director of the U. S.
National Cancer Institute; the occasion was the first hearing of
the Lasagna Committee, which issued its report on approval of new
drugs for cancer and AIDS on August 15, 1990 (for background on
this report, see AIDS TREATMENT NEWS #110, September 7, 1990).
The dispute, an advance echo of what is happening today,
concerned the FDA's refusal to approve the NCI's plan to begin
testing ddI as a treatment for children with AIDS under two years
old; the U. S. National Cancer Institute was ready to start this
ddI trial two years ago, but apparently the FDA wanted tests on
adults to be finished before the tests with children began.  (For
detailed newspaper coverage of the ddI dispute of two years ago,
see "Cancer Institute:  AIDS Drugs Unduly Delayed,"  by Michael
L. Millenson, Chicago Tribune, January 5, 1989, and "The Battle
over FDA Drug Policy; The Pressure Is On to Speed New AIDS and
Cancer Drugs through the Agency's Slow Approval Process," by
Laurie Garrett, News- day, February 14, 1989.)

     Two years later, one activists spoke of the spreading
"ripple of terror that the trials [running now for ddI and ddC]
are not what should have been designed."  It seems that nobody
thought through how the information to be generated by these
trials -- scheduled to run for about 18 months more -- would be
used to support drug approval.  One effect of this lack of
planning is that AZT, the first AIDS antiviral to reach FDA
approval, shut the door behind it, keeping all rivals out.  This
happened despite the clear need for new therapies -- shown most
compellingly by epidemiological data suggesting that AZT has
extended average survival after AIDS diagnosis by no more than
several months. (This survival data includes patients not
receiving AZT because of drug intolerance or other reasons; the
benefit of AZT for those who do use it might be greater.)

     Much of the reason for the current complexity, confusion,
and miscommunication stirred up by the push for early evaluation
of ddC and ddI is the need to retrofit to cover for mistakes of
the past.  These mistakes occurred because of lack of higher-
level oversight and planning in the AIDS research process.  Key
positions have long been vacant, or filled with people unwilling
to deal effectively with AIDS.

     One of the problems in the current development of ddC and
ddI is the lack of definition of what the trials are trying to
prove. Normally, the goal would be to prove efficacy (i.e., that
the drug works better than no treatment) for some group of
patients.  It should not be necessary to prove that the new drug
is better than standard therapy -- or even equal to it, because
many patients cannot use the standard therapy, and because
combination treatment using both the new and standard treatment
is highly promising.

     But since it would be unethical to run a placebo trial, ddC
and ddI are being compared to AZT instead.  Statistical efforts
were made to use the old AZT-vs. -placebo trial of four years ago
to allow ddC and ddI to be mathematically compared with a
placebo, even though no real placebo is being used in the current
trial.  This desperate attempt to forge a case for approval out
of ill-designed trials seems to have led to some of the recent
controversy.

     If the new drugs must be compared to AZT, then the next
question is whether they must be proved superior, or only
equivalent, to merit FDA approval.  Equivalence, of course, would
be the standard preferred.  But there are statistical
complications in proving equivalence.  For example, in a trial to
test whether one drug is better than another, the incentives are
for researchers to run a tight, clean study, so that if there is
a difference, it will be found.  But in a test for equivalence,
the incentives are for researchers to run a sloppy trial, because
failure to find a difference means success.  For this and other
reasons, there is confusion now over whether proof of equivalence
will be enough for approval of ddC or ddI, or whether proof of
superiority will be required.

     There are other problems with the current ddC and ddI
trials, and with the regulatory process.  One concern is that
companies do not usually submit their data to the FDA until their
NDA (New Drug Application) is finished; the FDA prefers to get
the data all together, in order to save staff time.  But an NDA
is a large document, typically consisting of many volumes of
paperwork.  Anyone familiar with the influence of corporate and
organizational cultures would expect that any time one
organization generates such a document and passes it to another
for evaluation, many points of disagreement or friction will
almost certainly be found.  Without inside knowledge of the
operations at the FDA, we cannot know whether this potential
problem does or does not in fact cause serious, avoidable delays.
(If it does, procedures could be changed to encourage earlier
collaboration for NDA review of critically important drugs.)

     Two years ago, NCI's Dr. Samuel Broder saw that no new AIDS
antivirals would be approved unless procedures were changed. "If
we have to compare every drug to AZT, with death as the endpoint
of a trial, we're going to be in a situation where it will be
very difficult to get any other antiretroviral approved for AIDS.
It took us two years to get AZT out -- how long do you think the
next one will take?  Five years, ten years?  That's
unacceptable!" (Quoted in Newsday article cited above; the
comments were addressed to Dr. Ellen Cooper of the FDA.  The
context of the discussion was ddI. Dr. Cooper replied with the
question, "Why don't you want to see a year's research in
clinical trials on an antiretroviral before approval?  ")

     Two years later, the trials of ddC and ddI still have months
or years to run -- and as we pointed out above, they are not well
focused on the important questions.  This is the context of the
growing movement to ask the FDA to call in the existing data now,
look at all that is known about these drugs, and approve them if
there is "substantial evidence" that they work.


San Francisco Physicians Seek Early ddI, ddC Review

     On December 26, 1990, two San Francisco physicians'
organizations, representing almost all physicians with large
AIDS/HIV practices in the San Francisco area, filed a formal
petition with the FDA urging that Agency to use its existing
statutory authority to expedite submission of existing data on
ddI and ddC, and then make a decision on marketing approval by
March 1, 1991.  The petitioning organizations are:

     (1) The Community Consortium, which consists of over 180
physicians, nurses, physician's assistants, and other licensed
health care providers.  The Community Consortium has been
conducting community-based trials of AIDS treatments since 1986;
one of its trials made major contributions to FDA approval of
aerosol pentamidine for pneumocystis prophylaxis.

     (2) The Bay Area Physicians for Human Rights, an
organization with over 200 members dedicated to quality health
care for lesbians and gay men.  BAPHR has long been involved in
AIDS policy issues; for example, it was the first organization to
issue safer sex guidelines.

     This petition is especially important for several reasons:

     * It shows that the call for rapid evaluation of ddI and ddC
(and of other drugs which may be equally promising in the future)
has the clear support of the leading AIDS physicians in the San
Francisco area, who are among the most experienced in the world.
As far as we know, there was no opposition to the petition within
either medical organization.

     * It cites specific sections in the Code of Federal
Regulations which show that the FDA has the clear legal authority
and also the mandate to expedite the approval of critically
important drugs for life-threatening illnesses.

     * It also calls on the FDA to use its authority to establish
and publish criteria by which antiretroviral drugs will be judged
for approval, which would provide guidance for pharmaceutical
companies and reduce the confusion which now prevails.

     * The 11-page petition document itself (including 55
technical references) is the best single statement of the case
for early approval of these drugs.

     * The petition will become part of the Congressional Record,
available for easy reference by members of Congress.

     The initiative and the legwork for this petition were
provided by San Francisco activists Jim Driscoll and Barry
Freehill, with medical guidance and leadership by Donald Abrams,
M. D., Chairman of the Community Consortium.  The idea of using a
petition was suggested by Sidney Wolfe, director of the Public
Citizen Health Research Group.

     The petition is open for endorsements by other
organizations. Persons interested in receiving a copy should send
a large self- addressed stamped envelope to:  Jim Driscoll or
Barry Freehill, c/o Community Consortium, 3180 - 18th Street,
Suite 201, San Francisco, CA 94110.


Congressional Letters Support Expedited ddI and ddC Review

     On November 27 Congresswoman Barbara Boxer (Democrat,
California) released a letter from 25 members of Congress to the
new Commissioner of the FDA, David A. Kessler, M. D., asking for
early review and possibly early release of ddI and ddC.
Congresswoman Boxer stated, "It is imperative that incoming FDA
Commissioner Kessler make this a top priority.  His background,
as an AIDS pediatric physician from a Bronx public hospital, well
qualifies him to take a fresh look at medical evidence supporting
these drugs."

     Congressman Jerry Lewis (Republican, California), Chairman
of the House Republican Conference, wrote a separate letter
supporting early review of these drugs.

     Congressional involvement is important because in the past,
the FDA has often faced criticism from Congress for approving a
drug too soon, but almost never for delaying approval.  These
letters provide cover for the FDA, and greatly reduce the concern
that fear of Congress might prevent it from moving as rapidly as
it otherwise could.

     Mobilization Against AIDS first asked Congresswoman Boxer to
draft the letter and circulate it in Congress; she immediately
agreed to do so.  To obtain a copy of that letter, write or call
Mobilization Against AIDS, 1540 Market St., #160, San Francisco,
CA 94102, 415/863-4676.

     Paul Boneberg of Mobilization Against AIDS pointed out that
obtaining such assistance from members of Congress is not
difficult, if local organizations choose to develop an
appropriate relationship with their representatives.


Project Inform Consensus Statement on ddI, ddC Approval

     The first consensus statement in support of early licensing
of ddI and ddC has been circulated by Project Inform.  Over 25
organizations and a number of physicians have signed.

     On August 16 Martin Delaney of Project Inform first wrote to
Doctors Ellen Cooper and Paul Beninger of the Division of
Antiviral Drug Products of the FDA, warning them that early
approval of ddI and ddC was about to become a major public issue,
and exploring possibilities for expediting evaluation and
approval of these drugs.

     The first draft of the Project Inform statement called for
early approval of the drugs, not just early review.  Some
physicians objected to this draft, saying that they had not seen
the data, and therefore could not know whether or not the drugs
were ready for approval.  Later drafts of the Project Inform
statement -- as well as the physicians' petition, and the
Congressional letter, both described above -- took these
reservations into account, and called on the FDA to rapidly
review the existing data, and approve the drugs if justified.


Ellen Cooper Resigns As Antiviral Chief

     Late last month Dr. Ellen Cooper asked to be reassigned
within the FDA and leave her job as chief of the Division of
Antiviral Drug Products.  Most activists who worked with Dr.
Cooper consider this development bad news, since no one else at
the FDA has her experience with AIDS drugs.  It is widely agreed
that her job generated intolerable pressures.

     In an interview published in The Wall Street Journal,
December 24, 1990, Dr. Cooper cited the conflict between four
groups -- people with AIDS, pharmaceutical companies, scientists
running trials, and regulators (at the FDA).  (It is notable that
this list did not include a fifth group -- the frontline
physicians with large AIDS/HIV practices.)  She commented that
"Politics has become paramount, but science should have a role."
She said that she was open to using T-helper counts (or other
measurements short of death or disease progression) to prove drug
efficacy, "but there's got to be an analysis of the data by
statisticians, researchers, and clinicians.  That's just starting
now."

     One incident which must have contributed to job pressure
concerns recent letters from Dr. Cooper to Bristol-Myers and to
Hoffmann-La Roche concerning standards for approval for ddI and
ddC. We have not seen these letters nor talked to anyone who has.
Apparently they address the problems with using the old AZT-vs.
-placebo trial as a basis for interpreting the data from the
current ddI-vs. -AZT and ddC-vs. -AZT trials.

     These letters have barely been mentioned in the press, but
behind the scenes they generated a storm of controversy, because
they were widely interpreted as taking back decisions already
made and requiring data that everybody knew would not be
available -- in effect, therefore, saying that the FDA will not
approve either drug at this time.  There may have been a
misunderstanding, however, because others believe that the
purpose of these letters was not to rule out approval, but rather
to ask the companies to put forward their best case for the
drugs.  Without seeing the letters, we cannot know what message
was intended, and whether a different message may have been
received.


Comment

     We are too far from Washington to cover what is happening
inside the Government in AIDS treatment research and development,
or in other AIDS policy; we wish there were a Washington-based
newsletter to do so.  We do have impressions on why Dr. Cooper's
job has been such a difficult one, and on how that position could
be made more workable in the future.

     Over a year ago this writer was at the FDA for a class which
the Agency had very commendably organized for community-based
research groups; we were there as a member of San Francisco's
Community Research Alliance (now the Project Inform Community
Research Alliance).  One lecture concerning a highly technical
aspect of clinical trials was given by Dr. Cooper.  We commented
to an FDA staff member present that we were surprised that the
head of the division would be prepared to speak on such a
specialized area.  He answered, with obvious respect for Dr.
Cooper, that she could speak equally well on any aspect of
clinical trials and the FDA's role in regulating them.

     We see Dr. Cooper as a top expert on clinical trials, but
one who in fact had two jobs -- not only the scientific job she
wanted and could do well, but also a political job in addition.
Due to lack of national leadership on AIDS from higher levels of
government, Dr. Cooper had become not only the leader of the
antiviral division at FDA, but also, in effect, the sole umpire
to judge the standards of approval for all AIDS antiviral drugs
-- and in consequence, the designer of national policy on how to
respond to the epidemic, in so far as development of antiviral
drugs is concerned -- development on which the life of everyone
with HIV depends.  There is no way that such a role could not be
political.

     The best outcome now might be for the FDA to separate the
two jobs.  Then Dr. Cooper could return to being head of the
antiviral division, without also having to singlehandedly set
national policy on AIDS drug development and take up the slack
created by leadership default from the President on down.  The
head of the antiviral division is three levels below the
Commissioner of the FDA; the political decisions (such as whether
to insist on new technical standards now if the practical
consequence is that nothing will be approved) are ultimately the
responsibility of higher levels.  There now is a Commissioner of
the FDA -- David A. Kessler, M. D., who was installed on December
3, after the office had long been vacant -- so this best outcome
might now be possible.


*****

Aspirin Update:  Warning, Promise, and
      Call for Information

by John S. James

     Last August 17, AIDS TREATMENT NEWS published an in-depth
look at the possibility that ordinary aspirin might have a role
in AIDS treatment -- as an immune modulator, not just for minor
symptom relief.  One of the physicians we interviewed, Joseph
Sonnabend, M. D., in New York, called recently to warn us of the
importance of medical monitoring with aspirin use -- especially
the need to follow platelet count.  He has seen one case of
serious hemorrhage in a patient with a rapidly falling platelet
count, who was taking two 325-mg aspirin tablets four times a
day.  Fortunately, this person recovered.

     Dr. Sonnabend suggests that anyone with a platelet count of
under 100,000, or who has ever had thrombocytopenia (low platelet
count), should have frequent medical supervision if they use
aspirin, or other drugs which can interfere with blood clotting.
Anyone with HIV should be monitored by their physician if they
use aspirin.

     Background note:  platelets assist in blood clotting.
Platelet counts often decline in persons with HIV infection.  For
unknown reasons, this decline is usually less serious than if the
same numbers occurred in persons without HIV -- and platelet
counts often become normal again as HIV infection progresses.
Bleeding problems due to low platelets have been rare with HIV
infection; but the case mentioned above shows that risk does
exist, and appropriate precautions are necessary.


A Report of T-Helper Improvement

     We have heard of one case of an unexpected major improvement
in T-helper count after low-dose aspirin use.  We are reluctant
to mention a single case until there is confirmation; but here,
the patient was in an NIH epidemiological study and has very good
data available -- quarterly T-helper and other blood counts from
a quality- controlled lab for the last six years.  We also chose
to mention this case because it suggests that an easy-to-organize
community-based trial could tell quickly if the effect is real,
or just a chance result in one case.

     This patient's T-helper count had declined for four years,
then stabilized at an average of about 500 with AZT; he has taken
500 mg of AZT per day for two years.  He started taking a single
325-mg buffered aspirin tablet per day near the end of August,
1990.  His last T-helper count before starting aspirin was 553.
By mid September the count was unchanged at 556, although the
helper/suppressor ratio had changed from .56 to .78.  By mid
November the count was 895, and by mid December it was 968 (the
November test was to apply for a different NIH study). The T-
helper percent and helper/suppressor ratio showed substantial
increases.  There was no other change in therapy or other known
factor which would explain these improvements.

     The patient had selected the low dose (one aspirin a day)
because of a report1 that an even lower dose (one aspirin every
other day) had the greatest effect in increasing both
interleukin-2 (IL-2) and interferon gamma in healthy volunteers.
In this study, IL-2, which stimulates the growth of T-cells, was
increased to two to three times baseline levels by low-dose
aspirin.


Questions for a Clinical Trial

     * The first question for a trial to answer is whether
aspirin can have any consistent effect in raising T-helper
counts, or if the effect reported above was just happenstance or
only applied to one patient.  Clearly it would be easy to run a
trial with low- dose aspirin, and follow T-helper counts for at
least three months.

Some other questions:

     * Is antiviral therapy (in this case, AZT) necessary?
Stimulating the growth of T-helper cells without antiviral
therapy might increase the growth of the virus.  We have heard
good results from studies which combined IL-2 and AZT; one early
report found a T-helper increase of over 300 during IL-2 therapy,
although the increase disappeared after treatment was stopped2.
(As we went to press, we learned that results of an important
trial at Stanford University of combination HIV treatment with
IL-2 and AZT have recently been published; we could not obtain
this paper by press time.)  If low-dose aspirin does indeed
stimulate the body to produce more of its own IL- 21, then
aspirin might be an alternative easier to obtain, safer, and of
course less expensive than the experimental pharmaceutical IL-2.

     * Could this treatment approach also work for persons with
lower starting T-helper counts?  A community-based trial could
accept volunteers with a range of T-helper values.  Then -- if
any significant effect is seen -- the researchers could look for
a dose- response relationship.


Call for Information

     Any information about long-term use of aspirin, and its
effect (or lack of effect) on T-helper counts, could be helpful
for designing such a trial.  If you have information we should
know about, contact John S. James at AIDS TREATMENT NEWS.

References

1.  Hsia J., Simon GL, Higgins N, Goldstein AL, and Hayden FG.
Immune modulation by aspirin during experimental rhinovirus
colds.  Bulletin of the New York Academy of Medicine.  January
1989; volume 65, number 1, pages 45-56.  (Note:  the data cited
above was from volunteers who did not have colds.)

2.  Bartlett JA, Blankenship K, Waskin H, Sebastian M, Shipp K,
and Weinhold K. Zidovudine and interleukin-2 in WR2 HIV infected
patients:  Evidence for stimulated immunologic reactivity against
HIV [abstract S. B. 421].  Sixth International Conference on
AIDS, San Francisco, June 20-24, 1990.

Note:  For background on aspirin, and what is known or not known
about its different mechanisms of action, see the latest
Scientific American, January 1991, pages 84-90.


*****

Women and AIDS Conference Report

by Laura Thomas

     The first National Conference on Women and HIV Infection was
held December 13-14, 1990, in Washington, DC. It marked the first
time that so many women with HIV, care providers, and activists
had met specifically to talk about  women and AIDS. The main
issues discussed at the conference were the need for adequate
health care for women with HIV infection, the lack of knowledge
about the progression of disease in women, the problems of women
and clinical trials, and the difficulties of doing education and
prevention for women.  This is a preliminary report of some of
the information from the conference.

     Some of the most interesting statistics presented proved
conclusively what we already knew:  health care makes a
difference.  Pat Kloser, M. D., from the Newark Women's AIDS
Clinic, showed that the women who were cared for in her clinic
averaged 70.4 weeks between AIDS diagnosis and death, as compared
to the women who went through the emergency room and hospital
system there, who averaged only 27.5 weeks.

     The clearest recommendation for care was that women with
symptomatic HIV disease should get cervical and anal Pap smears
every six months, followed up by colposcopies if necessary.  Pap
smears are recommended for all women once a year, and men with
HIV may be interested in having anal Pap smears done, as well.  A
Pap smear is a test for unusual, possibly pre-cancerous cells.
Women with suppressed immune systems are especially vulnerable to
infection with HPV (human papilloma virus) which causes cervical
and other anogenital cancers.  While there are not yet any truly
effective treatments for cervical cancer or HPV infection in
people with HIV, early detection and treatment offers the best
hope of keeping it under control.  Pap smears should become part
of every woman's health care regimen, and we have heard that they
are now going to be included in the standard of care for
participants in AIDS Clinical Trials Group clinical trials.

     There seems to be some evidence that the antimicrobial
action of the PCP prophylaxis TMP-SMX (Bactrim or Septra) is
causing vaginal candidiasis, or yeast infections, in women.  It
is well known that antibiotics such as penicillin can cause such
infections, which many women have self-treated with acidophilus
or yogurt, although we have not heard of any women on Septra
taking acidophilus to counter the candidiasis. Vaginal
candidiasis is also very common in women with HIV, so it may be
hard to tell whether it is caused by Septra or not. TMP-SMX may
also be preventing some of the HIV-related bacterial pneumonias
that many women and injection drug users are getting.

     Conflicting data was presented on the interaction of
methadone and AZT.  One clinician stated that methadone lowered
levels of AZT in the blood, and another said that it nearly
doubled AZT levels.  Many recovering injection drug users are on
methadone, so this will be an important drug interaction to
study.  As a group, injection drug users in clinical trials
showed the same compliance rates as gay men did, debunking the
myth of IDUs as irresponsible people.  In fact, the most
important predictor of compliance in a Boston trial of AZT was
the belief in the efficacy of AZT, not the participant's drug
using status or transmission route.

     One woman with AIDS described her frustration at being
unable to find a doctor who was willing to operate on her
cervical cancer.  Doctors discussed their difficulties in getting
and keeping good nurses.  Many women talked about the need for
substance abuse treatment, and made it clear that they could not
take care of their HIV infection without taking care of their
substance use, and vice versa.  We were encouraged to hear of
community-based clinics for women with HIV; but speakers noted
that women enter the health care system everywhere, and there are
few obstretics and gynecology physicians, or emergency room
personnel, who are trained to care for women with HIV.


*****

Announcements


Women and AIDS Town Meeting, San Francisco, January 16

     There will be a town meeting on women and HIV on January 16,
1991, 7:30 p.m., at the Women's Building, 3543 - 18th Street, in
San Francisco.  The meeting will be a presentation to the
community of information from the first National Conference on
Women and HIV Infection, held in Washington, DC, in December.
Anyone interested in learning more about women and HIV or hearing
about the conference is encouraged to attend.  The meeting is
wheelchair accessible.  For more information, contact Lisa Auer
at Project Inform,  415/558- 8669.


     4th National AIDS Update Conference, San Francisco, May 19-
22; Abstract Deadline March 1

     The National AIDS Update Conference, which covers treatment,
care and services, policy/administration, and
education/prevention, has been postponed and rescheduled for May
19-22, 1991.  The deadline for submission of abstracts for papers
or posters is March 1; the deadline for reserving company or
organization exhibit space is April 5.

     Unlike the annual international AIDS conferences, which
focus on new scientific developments, the National AIDS Update
Conference focuses on practical information for health-care
professionals.  For more information, contact Krebs Convention
Management Services, 415/255-1293, or 415/255-8496 (fax).

     Federal Agency Developing Guidelines for AIDS/HIV Care;
Panel Nomination Deadline January 31

     The U. S. Agency for Health Care Policy and Research is
selecting a panel of experts to create national guidelines for a
medical standard of care for AIDS/HIV.  These guidelines will be
for use by "physicians, health care practitioners, providers,
medical educators, medical review organizations, and consumers of
health care."  Nominations for panel members or chairperson(s),
which must include a resume of the person being nominated, are
due by January 31.

     For more information, see the Federal Register, December 10,
1990, pages 50776-50777.


Arab Nations:  Third Annual Conference on AIDS

     The Third Arab International Conference on AIDS is scheduled
to be held in Cairo, May 3-6, 1991.  Dr. M. A. Hasan is
overseeing the planning of the conference, which will be
conducted in simultaneous Arabic and English.  Below are the
contact numbers to ask for more information:


* telephone:  (2) 3625042, (2) 3623908
* telex:  20948 TTEBB UN
* cable:  Excellent, Cairo
* fax:  (2) 3631464.
* mail:  Conference Secretariat, 5 Al Saraya St., Al Manial,
   Cairo, Egypt.

*****

     AIDS TREATMENT NEWS reports on experimental and
complementary treatments, especially those available now.  It
collects information from medical journals, and from interviews
with scientists, physicians, and other health practitioners, and
persons with AIDS or HIV.

     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.

     We also examine the ethical and public-policy issues around
AIDS treatment research and treatment access.

[Obsolete subscription information has been removed.  See the
latest issues for up-to-date information. -- sysop]

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