Subject: AIDS Treatment News #195
Date: Mar 18 1994 (944 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 1994 by John S. James;
permission granted for non-commercial use.

AIDS TREATMENT NEWS Issue #195, March 18, 1994
   phone 800/TREAT-1-2, or 415/255-0588

CONTENTS:  [items are separated by "*****" for this display]

Kaposi's Sarcoma (KS):  Angiogenesis Inhibitors in Early
Trials

DOX-SL (Doxil) Kaposi's Sarcoma Treatment:  Trials,
Development Status

California:  AIDS Drug Assistance Program, New Drugs Available
April 1

FDA Holds Buyers' Club Drugs:  Review OF Access Issues



*****

Kaposi's Sarcoma (KS):  Angiogenesis Inhibitors in Early
      Trials

by Michael Marco

     [Note:  New York treatment activist Michael Marco heads the
     Oncology Project of the Treatment Action Group (TAG), which
     reports on treatments and research for various AIDS-related
     malignancies, and for Kaposi's sarcoma (KS).  He is also co-
     authoring (with Marty Majchrowicz from AIDS Project Los
     Angeles) a report on KS pathogenesis, treatments, and
     current opinions of noted clinicians and researchers.]

     Angiogenesis -- the formation of new blood vessels -- takes
place normally during wound healing.  But abnormal angiogenesis
is an important contributor to certain diseases. In cancer, for
example, solid tumors must be able to stimulate the growth of new
blood vessels to nourish the tumor cells, or they cannot grow
beyond a small size.  And evidence now suggests that Kaposi's
sarcoma may not be a true cancer in most cases, but instead may
be due to abnormal blood-vessel growth caused by dysregulation of
angiogenesis.

     Since normal growth of blood vessels is not necessary at
most times during a person's life, researchers are developing
drugs which inhibit angiogenesis (both normal and abnormal), in
the hope of creating an entirely new class of treatments for
cancer and for KS.  This article outlines the current status of
the research into three of these potential drugs, and describes
the clinical trials which are currently open. (Note:  For
previous coverage of angiogenesis inhibitors, see AIDS TREATMENT
NEWS issues #188, #162, #135, and #122.)

     Three anti-angiogenesis compounds currently in early
clinical trials as KS treatments are Tecogalan (SP-PG, also
called DS- 4152), TNP 470 (formerly called AGM-1470), and
recombinant human platelet factor 4 (rPF4).  They have only been
tested in a small number of patients with KS, and have mostly
shown a lessening of KS-associated swelling, and some minor
activity on existing lesions.  Many researchers now feel that
angiogenesis inhibitors might be most effective in preventing new
lesions from occurring rather than affecting pre-existing
lesions.(1) If this is true, these drugs might work best as
maintenance therapy after systemic chemotherapy.

Tecogalan (SP-PG):  Los Angeles, New York, San Antonio, San
Francisco

     Tecogalan is an angiogenesis inhibitor which has been
isolated from the bacterium Arthrobacter.  Tecogalan prevents a
protein (called fibroblast growth factor) from binding to
endothelial cells (the cells which line the insides of blood
vessels) and stimulating those cells to migrate and reproduce.
In animal tests conducted by Robert Gallo, M. D., and colleagues,
"nude" mice (special immunodeficient mice) were given a form of
KS by injection of human KS cells; Tecogalan "led to degeneration
of newly formed vascular lesions."(2)

     Four sites are currently recruiting patients for a phase I
dose-escalating pharmacokinetic and safety trial of intravenous
Tecogalan.  Preliminary results have shown some activity on
existing lesions, and a considerable lessening of edema
(swelling).  So far, no serious toxicities have been seen, except
for prolonged APTT (activated partial thromboplastin time, which
can affect the time it takes for blood to clot), which normalizes
after the infusion.(3)  Some patients have also noted chills and
fever.

     Volunteers may have any T-helper count for this trial, but
they must have at least five cutaneous (skin) lesions, and no
evidence of systemic visceral involvement.  During the first
dose, volunteers will be hospitalized for 24 hours for
monitoring; later doses will be given on an outpatient basis.

     This trial is being conducted at the following four sites:

* Los Angeles:  Kenneth Norris Jr.  Cancer Hospital/USC.
Investigator:  Parkash Gill, M. D. Contact:  213/224-6668.

* New York City:  Memorial Sloan-Kettering Cancer Center.
Investigator:  Susan Krown, M. D. Contact:  212/639-7426.

* San Antonio:  Cancer Therapy Research Center.  Investigator:
Gail Eckardt, M. D. Contact:  210/616-5798.

* San Francisco:  San Francisco General Hospital. Investigator:
James Kahn, M. D. Contact:  415/476-9296x84104


TNP-470:  Bethesda, Boston, Chicago, Los Angeles, St. Louis

     TNP-470 is a synthetic chemical analog of fumagillin, which
is produced by a fungus.  In 1990, researchers at Harvard Medical
School found that fumagillin and TNP-470 inhibited angiogenesis
in laboratory tests, and inhibited the growth of solid tumors in
mice; TNP-470 was found to be less toxic and 50 times as powerful
as fumagillin.(4)  Researchers at the U. S. National Cancer
Institute also found that TNP-470 inhibited abnormal spindle
cells, which have a major role in the development of KS.

     Animal tests showed that very large doses, given all at
once, caused toxicity, most notably small hemorrhages in the
brain, lungs, heart, and retinas of dogs.  The drug was better
tolerated when given as an infusion.  Therefore, initial clinical
testing used a one-hour infusion, starting at low doses.

     In preliminary results from the phase I trial of TNP-470 in
persons with KS, researchers at the NCI reported that the drug
showed some activity on existing lesions (especially in lessening
edema, or swelling), and a decrease in the development of new
lesions.  No dose-limiting toxicities were found.(5)

     This trial, as well as a four-site study by the AIDS
Clinical Trials Group (ACTG), is still ongoing; both are open for
volunteers.  There is no T-helper count requirement for these
dose-escalating trials, but patients with pulmonary KS are
excluded from the NCI trial; the ACTG trial excludes all
potential volunteers with symptomatic visceral KS.

     Note that the NCI trial, although conducted in Bethesda,
Maryland (near Washington, D. C.)  , is open to volunteers from
throughout the country.  The NCI will pay travel expenses (except
for the first trip), and will pay a stipend toward living
expenses while volunteers are in Bethesda.  The trial lasts 24
weeks.

     The first listing, below, is for the NCI trial.  The other
four are locations of sites for the ACTG trial.

Bethesda, Maryland:  U. S. National Cancer Institute.
Investigator:  Robert Yarchoan, M. D. Contact:  301/496-8959.

Boston:  Beth Israel Hospital.  Investigator:  Bruce Dezube, M.
D. Contact:  Beryl Chapman, 617/735-4149.

Chicago:  Northwestern University Medical Center. Investigator:
Jamie Von Roenn, M. D. Contact:  312/908-9412.

Los Angeles:  Kenneth Norris Cancer Center Hospital/USC.
Investigator:  Parkash Gill, M. D. Contact:  213/224-6668.

St. Louis:  Washington University School of Medicine.
Investigator:  Lee Ratner, M. D. Contact:  Mary Gould, R. N.,
314/454-0058.


Recombinant Platelet Factor 4 (rPF4):  Los Angeles, Philadelphia,
San Francisco

     Recombinant platelet factor 4, a genetically engineered
version of a substance normally found in the body, has been found
to inhibit endothelial cells in laboratory tests.(6) Another
research group, following up this result, found that rPF4 also
inhibited KS cells in a dose-dependent manner.(7)

     In the early phase I/II (safety and preliminary efficacy)
trial, rPF4 was injected into one lesion, while another lesion on
the same patient was given an inactive injection as a control.
An anti-KS effect was found in six of the 12 patients given rPF4.
The only side effect was a mild rash around the lesion in
approximately 20 percent of the patients.(8)

     There are three phase I/II trials of rPF4 which are
currently open for volunteers in the U. S. They differ in how the
drug is administered; subcutaneously in Los Angeles,
intralesionally in Philadelphia, and intravenously in San
Francisco.  There is no requirement for T-helper count.  These
trials will last for a maximum of eight weeks.

Los Angeles:  Kenneth Norris Cancer Center/USC. Investigator:
Parkash Gill, M. D. Contact:  213/224-6668.

Philadelphia:  Graduate Hospital of Philadelphia. Investigator:
Arthur Staddon, M. D. Contact:  215/893-7520.

San Francisco:  San Francisco General Hospital.  Investigator:
James Kahn, M. D. Contact:  415/476-9296 x84104.

References

1.  Pluda JM, Parkinson DR, Feigal E, and Yarchoan R.
Noncytotoxic approaches to the treatment of HIV-associated
Kaposi's sarcoma.  ONCOLOGY. December 1993; volume 7, number 12,
pages 25-33.

2.  Nakamura S, Sakurada S, Salahuddin SZ, and others. Inhibition
of development of Kaposi's sarcoma-related lesions by a bacterial
cell wall complex.  SCIENCE. 1992; volume 255, pages 1437-1440.

3.  Gill PS, PA-C Kidane S, Tulpule A, and others.  A phase 1
study of DS-4152, a novel angiogenesis inhibitor in the treatment
of AIDS-related Kaposi's sarcoma.  E. O. R. T. C., Amsterdam,
March 15-18, 1994.

4.  Ingber D, Fujita T, Kishimoto S, and others.  Synthetic
analogues of fumagillin that inhibit angiogenesis and suppress
tumor growth.  NATURE. December 6, 1990; volume 348, pages 555-
557.

5.  Pluda JM, Wyvill K, Lietzau J, and others.  A phase I trial
of TNP-470 (AGM-1470) administered to patients with HIV-
associated Kaposi's sarcoma (KS).  The First National Conference
on Human Retroviruses and Related Infections, Washington, D. C.,
December 1993 [abstract #31].

6.  Maione TE, Gray GS, Petro J, and others.  Inhibition of
angiogenesis by recombinant human platelet factor-4 and related
peptides.  SCIENCE. January 5, 1990; volume 247, pages 77-79.

7.  Miles S, Rezai A, Martinez-Maza O, and Maione TE.  
Recombinant platelet factor 4 (rPF4) and a non-heparin 
binding derivative inhibit AIDS-Kaposi sarcoma derived cell 
lines.  VII International Conference on AIDS, Florence, June 
1991 [abstract # W. A. 1066].

8.  Kahn J, Ruiz R, Kerschmann R, and others.  A phase I/II study
of recombinant platelet factor 4 (rPF4) in patients with AIDS-
related Kaposi's sarcoma (KS).  Proceedings:  Annual Meeting of
the American Society of Clinical ONCOLOGY. 1993; volume 12:A4.


*****

DOX-SL (Doxil) Kaposi's Sarcoma Treatment:  Trials,
      Development Status

by John S. James

     DOX-SL (formerly called Doxil -- the name has been changed
to avoid a trademark dispute in Europe) is an experimental
treatment, now being tested for Kaposi's sarcoma and for some
cancers, which has generated considerable interest in the AIDS
treatment community.  This article outlines what DOX-SL is, what
trials are underway, and what needs to happen to make the drug
more widely available (provided that the results of clinical
trials confirm early impressions that it may be useful).

     DOX-SL is a liposomal form of doxorubicin (also called
Adriamycin), a cancer chemotherapy drug.  Liposomes are
microscopic spheres of lipids (fats), which can contain active
drugs within them.  The liposomes can be specially prepared to
give the drug desired pharmacological properties
 --  especially to improve the targeting of the active compound,
so that it is more selective in reaching the intended tissues in
the body, to improve efficacy and reduce side effects.

     DOX-SL consists of very small liposomes, smaller than the
cells of the body.  Each one contains about ten thousand
molecules of doxorubicin.  These liposomes have two lipid layers;
the outer layer contains a chemical, polyethylene glycol (PEG),
which makes the liposomes less likely to be destroyed by the
immune system, a major problem in the early development of
liposomal drugs.

     An early phase I (dosage and toxicity) trial of DOX-SL, in
volunteers with Kaposi's sarcoma, has found that it delivers
about four to ten times the concentration of doxorubicin to the
lesion as the conventional free form of the drug.  Also, DOX-SL
has a half-life of about 48 hours in the bloodstream, compared to
10 to 15 minutes for the free drug.  No one knows for sure why
the liposomal drug is targeted selectively to the KS lesions.
One theory is that these lesions (and also cancer tumors)
stimulate abnormal blood-vessel growth, producing leaky
capillaries; the liposomes keep the drug in the bloodstream long
enough that it has time to leak out into the abnormal tissue,
while the free drug tends to be deposited indiscriminately.

     DOX-SL is being developed by Liposome Technology, Inc.
(LTI), of Menlo Park, California.  About 500 people have now used
the drug as a KS treatment in trials.

Published Experience

     The AIDSLINE database, the most complete listing of AIDS-
related journal articles, conference presentations, and letters
to journals, currently includes 12 citations on the use of DOX-SL
to treat AIDS-related KS.  Most of these reports are from
Germany.  Six of the twelve were presented at the IX
International Conference on AIDS, June 6-11, 1993, in Berlin.
Only one of the 12 was published before 1993.

     Most of these reports are favorable, suggesting that
liposomal doxorubicin was effective for the large majority of
patients, sometimes producing dramatic benefits.  But these
results are not from controlled studies comparing the drug to a
different treatment regimen.  Therefore, we will need data from
ongoing trials (see below) to evaluate the benefits and risks of
DOX-SL compared to the available alternatives.  The FDA usually
requires two controlled trials before approving a drug.

     The main toxicities have been hematologic; these have been
manageable, sometimes with the help of G-CSF. On the positive
side, cardiac toxicity (which can occur with ordinary
doxorubicin) has not been a problem so far; however, this effect
is cumulative, related to the total lifetime use of doxorubicin,
so it might appear later after the liposomal drug has been used
longer.

     There are published reports of two deaths from liver failure
among AIDS patients using DOX-SL; these may have been drug
related, but that is not known (see Hengge and others -- second
reference -- and Simpson and others, in References section,
below).  In the only case published in any detail, the patient
had a history of hepatitis and a T-helper count of 17, and had
been taking rifampicin, cycloserine, clofazimine, fluconazole,
and itraconazole, in addition to DOX-SL.  LTI has not seen any
abnormal elevation of liver enzymes in its trials, and does not
know any other way to screen or test for this possible problem.

     Most of the reports suggest that liposomal doxorubicin was
well tolerated, often with no serious side effects, or none at
all.  But clearly there are risks, as with any chemotherapy, so
the drug will have to be used carefully.  The phase III protocol
includes special testing for cardiac toxicity, but no special
warning to physicians about the possibility of liver problems.

DOX-SL Clinical Trials

     Besides the early phase I trial mentioned above, a larger
phase II (early efficacy) trial of DOX-SL has now been completed.
The results are not yet available, however, because the data is
still being analyzed.

     Full approval of DOX-SL will also require completion of a
phase III trial, which began over a year ago and still needs
about 100 more volunteers; about 125 are already enrolled.  This
trial, now being conducted at over 30 sites in the U. S., has
been slow to recruit, apparently because lack of information or
misunderstandings about it.

     The trial, which was designed with activist input, is for
patients with KS which is severe enough to require systemic
chemotherapy.  They are randomly assigned to receive either DOX-
SL, or the conventional chemotherapy called ABV -- Adriamycin
(another name for doxorubicin, the active ingredient in DOX-SL)
plus bleomycin, plus vincristine. However, those randomly
assigned to ABV will only receive six courses of it, at two-week
intervals; then they will be able to switch to DOX-SL. Also, if
the ABV has unacceptable side effects, or does not seem to be
working, they can switch to DOX-SL immediately.  (The most
serious toxicities of ABV -- especially cardiac toxicity which
can be caused by the Adriamycin -- tend to be cumulative, and
unlikely to occur early in the use of the treatment.)

     Volunteers with any T-helper count can enter this study.
They must have "progressing KS with at least 25 mucocutaneous
lesions and/or the development of 10 or more new lesions in prior
month, and/or documented visceral disease and at least 2
assessable cutaneous lesions, and/or 2 assessable cutaneous
lesions with edema."  They must have hemoglobin greater than 8,
neutrophil count over 1200, and platelet count over 75,000.  They
must not have "active opportunistic infection with mycobacteria,
cytomegalovirus, toxoplasma, P. carinii or other microorganism if
under treatment with myelotoxic drugs."  There are also other
inclusion/exclusion criteria.


     No placebo is used in this study.  Patients are randomly
assigned to a therapy, but then they are told what they are
getting.

     Why has this trial been slow to recruit?  There seem to be
several reasons.  A major one, we believe, is that information
about the trial has not been effectively communicated.  For
example, we spent well over ten hours researching this article
before we learned how a patient who wanted to volunteer could go
about doing so.  And as far as we know, the list of cities where
the trial is being run (see below) has never been published
before, although a major phase III trial has been open for over a
year in the U. S. For effective recruiting, such how-to-plug-in
information should be everywhere.

     Some volunteers are rejected by the study's entry criteria,
of course; others are too far from a city where the trial is
being run.  Another problem is that DOX-SL has not been well
known in the activist community until recently.  And many who do
know about it have wanted to receive it and not risk being
randomized to ABV -- even though ABV is known to be effective in
a large majority of cases, and the trial allows everyone to get
DOX-SL after no more than six courses of ABV.

     Another reason why this trial has been slow to recruit is
that it does not pay all costs -- and some insurance companies
have denied reimbursement for the costs which are not covered.
All the study drugs are paid for -- including the ABV, not only
the DOX-SL, which of course is provided free.  And LTI now pays
for the cardiograms, which are required as a safety measure.  But
it does not pay the cost of the infusions.

     Insurance will usually cover this cost (which should not be
surprising, since the infusions are necessary in any case,
because patients are not eligible for this trial unless they need
systemic chemotherapy).  In San Francisco, Kaiser San Francisco
is now preparing to conduct the trial; but it has not paid the
costs at non-Kaiser sites, so until now it has been difficult,
even in the San Francisco area, for Kaiser patients to enter.

     LTI reimburses its trial sites for each patient.  Sometimes
the physician may be willing to give patients a break on the
infusion cost, if there is no other way to pay for it.  If
financing remains a problem, physicians should call LTI, to see
if some way that these costs can be paid for.

Expanded Access

     In addition to the comparative trials, LTI has made DOX-SL
available to patients who cannot use ABV successfully and have no
other option.  This expanded-access protocol now has about 300
patients enrolled.

     Earlier this year LTI closed the expanded access to new
"refractory" patients -- those for whom ABV does not work -- but
re-opened it after furious protests from physicians and
activists.  It might be closed in the future, however, as it is a
serious financial burden on the company, since this particular
protocol requires major paperwork for each patient.  Also, this
expanded access (which will not contribute much toward approval
of the drug) appears to have reduced recruitment in the all-
important phase III trial -- as some patients, for example, would
get their physician to give them ABV just so they could say it
didn't work and become eligible.  The company hopes to replace
the current expanded access system with a "treatment IND," -- a
different procedure which would provide the same treatment, but
with much less documentation overhead.  The treatment IND
requires FDA approval, however, and that is not assured.

Approval Strategy

     LTI intends to apply to the FDA for two different marketing
approvals for DOX-SL. First, it will ask for approval as a
salvage therapy, for patients who cannot benefit from ABV. This
kind of application can be considered quickly, based on the data
that already exists, without waiting for the phase III trial to
be finished.

     LTI will apply for full approval later, after the phase III
trial is complete.

     Pending approval for marketing, LTI hopes to replace its
current expanded access with a treatment IND, as explained above.
However, any approval for DOX-SL must go through the oncology
staff and advisory committee of the FDA -- not the same people
that usually judge AIDS treatments.  The FDA's oncologists have
little personal experience in treating KS; they are experts in
cancer, not in AIDS.  They may not be entirely aware of the need
for new treatment options, unless oncologists and other
physicians let them know what their needs are.

Other Trials

     In addition to the U. S. trial, a major European trial is
comparing DOX-SL to a conventional treatment called BV (bleomycin
plus vincristine) -- a treatment commonly used in Europe,
apparently to avoid the side effects of the Adriamycin.
(Although mainly a European study, this trial also has three U.
S. sites, Boston, Houston, and Seattle; however, we do not know
at press time if all three are still open.)

     One future possibility is to combine DOX-SL with BV. This
would appear to offer the advantage of the three-way combination
which is the accepted therapy in the U. S., but with the
presumably better efficacy and lower toxicity of the Adriamycin
(doxorubicin) component.  The AIDS Clinical Trials Group (ACTG)
of the U. S. National Institute of Allergy and Infectious
Diseases (NIAID) is now planning a trial, in collaboration with
LTI, to compare DOX-SL plus BV to DOX-SL alone; it could begin as
early as summer 1994.

How to Volunteer

     DOX-SL trials are currently being conducted in the cities
listed below (alphabetically, by state); this list only includes
U. S. sites.  Not all trials are available at all sites.  If more
than one physician or medical center is conducting DOX-SL trials
in a city listed, the total number of sites appears after the
city name.

     Patients interested in more information should have their
physician call a physician conducting DOX-SL trials in a city
convenient to them, if their physician knows who that is.
Otherwise, their physician should call George Tidmarsh, M. D.,
staff oncologist at LTI, 415/323-9011.

California:  Berkeley, Encino, Greenbrae, Los Angeles (2), San
Diego, San Francisco (5)

District of Columbia:  Washington Florida:  Miami, Tampa Georgia:
Atlanta (2) Illinois:  Chicago (2) Massachusetts:  Boston,
Cambridge Michigan:  Detroit Missouri:  St. Louis New York:
Buffalo (2), New York City (4) Pennsylvania:  Philadelphia Texas:
Dallas, Houston (3) Washington:  Seattle

References

The following are all of the published articles and conference
presentations we could find on liposomal doxorubicin for treating
AIDS-related KS.  All but one were published in 1993.  They are
in alphabetical order by lead author.

Bogner JR, Zietz C, Held M, and others.  Ultrasound as a tool to
evaluate remission of cutaneous Kaposi's sarcoma.  AIDS. August
1993; volume 7, number 8, pages 1081-1085.

Boyle MJ, Marshall NE, Dolan GM, and others.  A phase II study of
stealth liposomal doxorubicin HCL (S-DXR) in HIV- associated
Kaposi's sarcoma (KS).  IX International Conference on AIDS,
Berlin, June 6-11, 1993 [abstract #1570].

Goebel FD, Bogner JR, Spathling S, and others.  Quantitative
ultrasound volume measurement serves as noninvasive method to
follow response of cutaneous Kaposi's sarcoma lesions to Doxil
therapy.  PROCEEDINGS:  ANNUAL MEETING OF THE AMERICAN SOCIETY OF
CLINICAL ONCOLOGY. 1993; 12:A7.

Goebel FD, Bogner JR, Spathling S, Held M, Sandor P, and Rolinski
B.  Efficacy and toxicity of liposomal doxorubicin in advanced
AIDS-related Kaposi sarcoma (KS).  An open study.  IX
International Conference on AIDS, Berlin, June 6-11, 1993
[abstract #WS-B15-6].

Goebel FD, Liebschwager M, Held M, and others.  Successful
treatment of advanced Kaposi sarcoma (KS) with liposomal
doxorubicin -- short term observations.  VIII International
Conference on AIDS, Amsterdam, July 19-24, 1992 [abstract #3108].

Hengge UR, Brockmeyer NH, Baumann M, Reimann G, and Goos M.
Liposomal doxorubicin in AIDS-related Kaposi's sarcoma [letter].
LANCET. August 21, 1993; volume 342, page 497.

Hengge UR, Brockmeyer NH, Rasshofer R, and Goos M. Fatal hepatic
failure with liposomal doxorubicin [letter; see comments].
LANCET. February 6, 1993; volume 341, pages 383- 384.

Jablonowski H, Szelenyi H, Armbrecht C, Mauss S, Niederau C, and
Strohmeyer G.  Liposomal doxorubicin -- a new formulation for the
treatment of Kaposi's sarcoma:  a study on safety and efficacy in
AIDS patients.  IX International Conference on AIDS, Berlin, June
6-11, 1993 [abstract #1573].

Northfelt DW, Martin FJ, Kaplan LD, and others. Pharmacokinetics
(PK), tumor localization (TL), and safety of Doxil (liposomal
doxorubicin) in AIDS patients with Kaposi's sarcoma (AIDS-KS).
PROCEEDINGS:  ANNUAL MEETING OF THE AMERICAN SOCIETY OF CLINICAL
ONCOLOGY. 1993; 12:A8.

Sandor P, Bogner JR, Held M, Spathling S, Rolinski B, and Goebel
FD.  Use of G-CSF in the management of chemotherapy- induced
neutropenia in patients with advanced-stage Kaposi- sarcoma.  IX
International Conference on AIDS, Berlin, June 6- 11, 1993
[abstract #1890].

Simpson JK, Cottrill CP, Miller RF, and Spittle MF.  Liposomal
doxorubicin:  initial experience in a major London centre.  IX
International Conference on AIDS, Berlin, June 6-11, 1993
[abstract #1603].

Szelenyi H, Jablonowski H, Armbrecht C, Mauss S, Niederau C, and
Strohmeyer G.  Long term treatment with liposomal doxorubicin in
patients with AIDS-related Kaposi's sarcoma. IX International
Conference on AIDS, Berlin, June 6-11, 1993 [abstract #1574].


*****

California:  AIDS Drug Assistance Program, New Drugs
      Available April 1

by Bruce Mirken

     As we reported in the last two issues of AIDS TREATMENT
NEWS, California recently added 13 new medications to its AIDS
Drug Assistance Program (ADAP), as a result of new Federal
funding through the Ryan White CARE Act.  A total of 27 drugs
(see below) are now approved for this program for uninsured
persons with low or moderate income.  But we recently learned
that the 13 new drugs will not be available at least until April
1, when the Federal funding is received.

     There could be an additional wait in some counties, due to
paperwork.  This happened the last time there was major expansion
of the program, when some county health-department officials did
not move quickly to make the newly added drugs available.

     Steven Roger, Chief of Early Intervention Services for the
California state Office of AIDS, said he is confident that the
new drugs will be available after April 1 without delay. We asked
what clients should do after that date if they encounter local
officials either unaware of or unable to provide the newly added
medicines.  "Call me," he replied.  His number is 916/327-6784.

     Activists are concerned that the program has been
inadequately publicized, and Roger says he is considering an
informational mailing to all California physicians -- if he can
find the time and resources.  "There's just so much we can do,"
he commented.  "We've got a really small staff."

     Readers outside of California should note that similar
programs are available in most states, but the lists of available
drugs and other details vary considerably.  Your local health
department or AIDS service organization may be able to provide
information for your area.

     The following drugs are now included in the California AIDS
Drug Assistance Program:  acyclovir*, amphotericin B*,
atovaquone*, azithromycin*, AZT, clarithromycin*, clindamycin,
clofazimine*, clotrimazole, dapsone, ddC*, ddI, ethambutol*,
flucytosine*, fluconazole, foscarnet*, ganciclovir, ketoconazole,
nystatin, paromomycin*, pentamidine (aerosol), pentamidine
(intravenous)*, pyrimethamine, rifabutin*, sulfadiazine,
trimethoprim- sulfamethoxazole.  Those marked with the asterisk
should be available after April 1.

     Note:  In California and probably most other states it is
usually necessary to go to the county pharmacy or other special
locations to receive ADAP drugs.  Some states provide the drugs
by mail or through ordinary pharmacies, apparently reducing
administrative costs as well as hardship for some patients.

*****

FDA Holds Buyers' Club Drugs:  Review of Access Issues

by John S. James

     Since February 22, three packages of pharmaceuticals shipped
from Mexico to the PWA Health Group in New York have been held by
the Cincinnati office of the U. S. Food and Drug Administration.
On March 16, as this issue goes to press, one of the three has
been released; the other two are still being held.  The PWA
Health Group has openly imported all three of the drugs involved
for several years; however, the FDA insists that there has been
no change in policy.  (The drugs are:  albendazole -- now
released -- used for treating microsporidiosis, when nothing else
works; tinidazole, an anti-parasite drug which works more quickly
than Flagyl; and isoprinosine, an immune modulator which has
shown good results in a major Scandinavian trial with hundreds of
patients, but was never developed in the U. S. because political
disputes held it up until the patent ran out.  The PWA Health
Group has long required a prescription for albendazole and for
tinidazole, but not for isoprinosine, which is commonly sold over
the counter.)

     The current incident did not result from any problem with
the drugs, nor from any policy change.  What precipitated it is
that the PWA Health Group switched to a different shipping
company, whose flights from Mexico to New York connect through
Cincinnati.  Two agents in the FDA office there held up the
drugs.  After the PWA Health Group called the Office of AIDS and
Special Health Issues, at the FDA headquarters near Washington,
to get the shipments released, the Cincinnati agents called
physicians who had written albendazole prescriptions, "to warn
the doctors about participating in a if they don't comply with
the investigation," according to a March 7 memo from the PWA
Health Group.  Sally Cooper, executive director of the PWA Health
Group, told us that the physicians she talked to were outraged by
this attempt to interfere with their medical practice, when their
use of the drug is widely accepted as reasonable by experts in
the field.  But they were unwilling to write or call the FDA
about it, apparently fearing that they might make enemies who
could hurt them in their profession.  The PWA Health Group
complained to the FDA; but after an internal FDA meeting on March
4, they were told that the AIDS office was no longer handling
this issue and they had to work through the Office of Regulatory
Affairs.

     While the immediate problem may be resolved -- largely by
using other freight carriers, so that packages will no longer be
shipped through Cincinnati -- there are larger issues around the
edges.  While it appears true that there has been no change in
official FDA policy, there are concerns that this case, among
others, may signal changes in attitude.  Problems cleared up 
years ago not only have returned, but have been more difficult 
than expected to resolve.

Background:  FDA Personal-Use Import Policy

     The regulations involved in this case concern the much-
discussed FDA policy on importing small quantities of
pharmaceuticals, not available in the U. S., for personal use.
This policy was formalized in December 1989; it was modified on
May 25, 1993, in a letter from the FDA to AIDS buyers' clubs, and
is in force today.  Because of considerable confusion about the
policy, we reproduce the key section, dated December 11, 1989,
from the Regulatory Procedures Manual.  (We also include the
section which follows, on import alerts, although it is not
involved in the Cincinnati case.)

9-71-30 GENERAL GUIDANCE

Section C. Drugs, Biologics, and Devices

     When personal shipments of drugs and devices that appear
violative are brought to FDA's attention by Customs, FDA
personnel will have to use their discretion to decide on a case
by case basis whether to sample or detain.  Generally, drugs and
devices subject to the Import Alerts are not amenable to this
guidance.  Devices to be used by practitioners for treating
patients should not be viewed as personal importations subject to
this chapter.  Drugs subject to Drug Enforcement (DEA)
jurisdiction should be returned to Customs for handling.

     In deciding whether to exercise discretion to allow personal
shipments of drug or devices, FDA personnel should consider a
more permissive policy in the following situations:

* when the intended use is appropriately identified, such use is
not for treatment of a serious condition, and the product is not
known to represent a significant health risk; or

* when 1) the intended use is unapproved and for a serious
condition for which effective treatment may not be available
domestically either through commercial or clinical means; 2)
there is no known commercialization or promotion to persons
residing in the U. S. by those involved in the distribution of
the product at issue; and 3) the product is considered not to
represent an unreasonable risk; and 4) the individual seeking to
import the product affirms in writing that it is for the
patient's own use (generally not more than 3 month supply) and
provides the name and address of the doctor licensed in the U. S.
responsible for his or her treatment with the product or provides
evidence that the product is for the continuation of a treatment
begun in a foreign country.

     Where there are any questions about the application of these
factors to any product, the product should be detained and FDA
personnel should consult with the appropriate headquarters
office.

     Where a shipment is not detained or refused, FDA personnel
should "Release with Comment" and, as appropriate, advise the
recipient that 1) the drug (or device) that has been obtained for
personal use appears to be unapproved in the United States; 2)
the drug (or device) should be used under medical supervision; 3)
FDA may detain future shipments of this product; and 4) the
patient's physician should consider enrolling the patient in an
Investigational study or applying for an Investigational New Drug
(IND) exemption.

9-71-40 IMPORT ALERTS

     FDA personnel should recommend to HFC-131 the issuance of an
import alert if they encounter:

* personal importation of products that represent either a direct
or indirect risk;

* the promotion of unapproved foreign products for mail-order
shipment; or

* repeated importation of products that represent a health fraud.

     This policy was updated in the May 1993 letter to buyers'
clubs (see AIDS TREATMENT NEWS #176, June 4, 1993, for portions
of that letter, and for an interview with Randy Wykoff, M. D.,
head of the FDA's Office of AIDS and Special Health Issues).  The
letter interpreted the 1989 policy to address three major
concerns of the FDA:  lack of physician involvement in the care
of people getting products through alternative mechanisms;
promotion and commercialization of products; and drugs from
unknown sources.

     Neither the original policy nor the clarification requires a
prescription for drugs to be imported.  Instead, from the letter
to buyer's clubs:

     "Documentary evidence should be available for immediate
review onsite, demonstrating that any patient importing products
for personal use has a licensed physician who is accepting
responsibility for the patient's care, including the
administration of the imported product.  FDA does not believe
that the best interests of any individual are served by having
access to drugs for serious conditions without adequate physician
oversight."

Comment and Recommendations

     The PWA Health Group appears to have more than met the
requirements of the personal use policy.  The policy does not
require a prescription, only evidence that a physician is
supervising the treatment -- a matter which activists fought hard
for in 1989, when the policy was developed.  The PWA Health Group
does require a prescription for albendazole and tinidazole.

     Persons should be aware, however, that the personal-use
import policy allows discretion by the FDA, and provides guidance
to agents on using that discretion.  It does not create a legal
right to import drugs in every case, but attempts to formalize
procedures for making case-by-case decisions.

     The issue, then, is one of discretion.  During the last
several years the FDA has made important efforts to avoid being
an obstacle to persons with AIDS or other serious or life-
threatening conditions obtaining treatment which is medically
appropriate.  And usually the problem now is no longer the FDA,
but the lack of interest by pharmaceutical companies in
developing products for AIDS, and especially for opportunistic
infections, since the U. S. market for each infection is likely
to be small.

     The Cincinnati incident has precipitated fears that the FDA
may be diluting its commitment to avoid blocking patients' access
to unapproved but medically appropriate care for serious
conditions for which no adequate approved therapy is available.

     The FDA appears to be concerned that if it uses its
discretion in favor of persons with life-threatening conditions
-- and AIDS in particular -- then promoters of health foods or
questionable remedies can argue in court that they are victims of
discriminatory enforcement, that the FDA is giving special breaks
to people with AIDS that it is not giving to them.  In fact,
under the laws and regulations, the FDA is clearly given areas of
discretion, and is expected to exercise this discretion in the
furtherance of medically rational policies.  But attitudes toward
AIDS in some parts of the country are such that the promoters'
discriminatory- enforcement argument could have influence,
regardless of laws, regulations, or rationality.  We understand
that the FDA recently lost a case in which that argument was
raised -- apparently a bizarre case which started by accident but
turned into a decade-long crusade.  The FDA may also be concerned
that overruling local officials' moves against AIDS groups may
damage morale -- even though the regulations plainly state that
local officials should seek guidance from FDA headquarters when
questions arise.

     Meanwhile, the recent events are raising fears about whether
the AIDS community can still defend itself.  Many people have
died, and there is widespread discouragement due failures in
treatment research; will people still mobilize if necessary to
maintain access to medically appropriate treatments, when their
access is under political attack?  This is why the small incident
in Cincinnati invokes issues which will not go away.

     We have two suggestions -- not for the immediate case, but
for building strength to be used if necessary in the future.
First, we can begin groundwork on what could be a powerful
response to official obstacles to medically accepted treatments
-- actions for wrongful death, raising the issue in the courts,
Congress, the media, and otherwise, in cases where the lack of
treatment appears to cause or contribute to the death.  The way
to prepare for this possibility is for organizations to do the
advance work to handle the obstacles -- legal, financial, 
technical -- to such actions.  If the preparations are thorough 
and professional, then all that will be necessary, when an 
appropriate case arises, is for the family or other 
representative -- or for the deceased themselves, through a will 
-- to say, "Yes."  It would not take many such cases to have an 
impact.

     Our other suggestion for building community strength is much
broader.  AIDS and treatment organizations need to make certain
changes in how they operate, in order to be able to grow into a
mass movement.  (AIDS may not be a mass movement in itself, but
needs to be able to function as part of one, in coalition with
others.)  The main problem is that most organizations do not
offer a workable path for new people to approach the group and
get plugged in -- an easy, appealing way to volunteer, or just to
hang out for a while with as little or as much commitment as they
want to give, and see what develops for them.  AIDS organizations
which do offer a clear, unambiguous path (such as the Walkathon,
etc.) often get tens of thousands of volunteers; people are
ready to help, but organizers must do their job first to make it
possible for them to do so.  The elitism and ego fights, which
can occur in any organization, can poison the development of the
mass-movement style which may become necessary for our survival.


*****

AIDS TREATMENT NEWS
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   John S. James
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AIDS TREATMENT NEWS reports on experimental and
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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.

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ISSN # 1052-4207

Copyright 1994 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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