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Development
of HIV with Drug Resistance after CD4 Cell Count-guided Structured
Treatment Interruptions
For
HIV patients, structured
treatment interruption (STI) is an attractive
alternative strategy to continuous treatment, particularly
in resource-restrained settings, because it reduces both
side effects and costs. One major concern, however,
is the development
of resistance to antiretroviral drugs that
can occur during multiple cycles of starting and
stopping therapy.
HIV
genotypic drug resistance
was investigated in 20 HIV-infected Thai patients
treated with highly active antiretroviral therapy (HAART)
and CD4 cell count guided
STI after dual nucleoside
reverse transcriptase inhibitor (NRTI) treatment.
Resistance was tested at the time of the switch
from dual-NRTI treatment to HAART and when HAART
was stopped during the last interruption.
Results
After
STI, one major drug-resistance mutation occurred
(T215Y), and, in the 4 samples with preexisting
major mutations (D67N [n = 2], K70R [n
= 2], T215Y [n = 2], and T215I [n
= 1]), the mutations disappeared.
All
mutations in the HIV protease gene were minor
mutations already present, in most cases, before
STI was started, and their frequency was not
increased through STI, whereas the frequency
of reverse-transcriptase gene mutations significantly
decreased after the interruptions.
After
the 48-week study period, no patients had
virological
failure. Long-term follow-up (108 weeks)
showed 1 case of virological failure in the
STI arm and 1 in the continuous arm.
No
virological failure was seen in patients with major
mutations.
Conclusions
The
authors conclude, “Major HIV drug-resistance mutations
were not induced through CD4 cell count guided
treatment interruptions in HIV-infected patients
successfully treated with HAART after dual-NRTI therapy.
02/14/05
Reference
R Nuesch and others. Development of HIV
with Drug Resistance after
CD4 Cell Count Guided
Structured Treatment Interruptions
in Patients Treated with
Highly Active Antiretroviral Therapy
after Dual Nucleoside
Analogue Treatment. Clinical
Infectious Diseases 40(5): 728-734. March 1, 2005.
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