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01 March 2007 |
Sydney-Los Angeles, March 1, 2007 – New data released
by the international medical humanitarian organization Médecins
Sans Frontières (MSF) at the 14th Conference on Retroviruses and
Opportunistic Infections (CROI) in Los Angeles this week demonstrates
good clinical outcomes for second-line antiretroviral therapy (ART) in
resource-poor settings. Newer medicines needed for second-line regimens,
however, remain unaffordable and largely unavailable in affected countries,
and adapted diagnostic tools needed to appropriately monitor lifelong
treatment are missing.
MSF presented a study of 352 adult patients from 50 MSF-supported ART
projects in 22 countries who had been on first-line treatment for at
least six months and then needed to switch to a second-line regimen either
because of a drop in CD4 count or a clinical event. The second-line regimen
included a new drug class, a protease inhibitor, and at least one change
in the nucleoside component. The median follow-up period was seven months.
Overall probability of survival was 86% at 12 months, and median CD4
gain +131 at 12 months.
“Our outcomes tell us that second-line AIDS therapy is working
for people living with AIDS in resource-poor settings,” said Dr.
Alexandra Calmy, HIV/AIDS Advisor at Médecins Sans Frontières
Campaign for Access to Essential Medicines, speaking at a press conference
at CROI. “This despite several obstacles, like the lack of access
to the best regimens and the fact that patients tend to go on second
line late in the course of the disease.”
According to the MSF study, there was a switch rate to second-line treatment
of 4.4/1,000 patients per year, indicating that patients in resource-poor
settings tended to stay on a first-line regimen much longer than in developed
countries.
“Patients might die before they even get a chance to switch to
a second-line regimen,” Dr. Calmy added. “We simply lack
the diagnostic tools to efficiently diagnose treatment failure early
enough. And doctors are reluctant to switch to second line because it
is the last therapeutic option and they are afraid to burn the two treatment
lines available by switching patients unnecessarily.”
While the needs for a second-line regimen are likely to increase in
the coming years, medicines used for second-line therapy are mostly unavailable
or unaffordable in developing countries. For example, the heat-stable
form of the boosted protease-inhibitor lopinavir/ritonavir, marketed
as Kaletra by Abbott Laboratories, is only sold in high-income countries
[US, Europe, Australia] because Abbott has taken few steps to make it
available in any resource-poor country except South Africa. The company’s
price for middle-income countries such as Thailand is unacceptably high.
The technology required to monitor the viral load in patients’ blood
is also extremely expensive and not very accessible in developing countries.
Without viral load testing, determining the moment at which patients
need to be switched to a newer regimen is difficult and relying on clinical
symptoms or immunological failure is often too late.
MSF currently provides ART to more than 80,000 patients in over 30 countries.
In one MSF project in Khayelitsha, South Africa, where regular monitoring
with viral load testing is available, 20% of people needed to be switched
to a second-line regimen after being on treatment for five years, according
to data presented at CROI by Dr. Gilles van Cutsem, from MSF in South
Africa.
“We need newer medicines and viral load tests rapidly and at a
large-scale because we know that we’re going to be seeing a growing
number of people who need to switch regimens in our projects,” said
Dr. Laurent Ferradini, also of MSF, who presented the first study based
on virological indicators on the efficacy of second-line ART in Cambodia. “But
the medicines we now use in second-line regimens are used as a final,
salvage-therapy option. What will we do once people start to again fail
on this regimen?”
Regimens that consist of newer medicines can cost between 10 and 50
times more than today’s standard first-line therapy. Beyond price,
many newer medicines are marketed under monopoly-like conditions, as
was the case for first-line drugs in the late 1990s. Competition among
multiple manufacturers, including generic producers is what helped bring
prices of first-line therapy down by 99% and increase availability. But
due to increased patenting in key generics producing countries such as
India, sources of affordable medicines are increasingly drying up.
For more information contact James Nichols, MSF Australia: 0407
525 700 or 02 8570 2600.
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