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Partial
Control of Viremia Is Associated with Favorable Outcome in HIV Patients
Exposed to Multiple Antiretroviral Regimens
The goal of antiretroviral therapy is clinical benefit through the
suppression of viral replication and the immunologic reconstitution
of HIV-1-infected patients. In spite of the availability of different
highly active antiretroviral therapy only some patients sustain
undetectable plasma viremia.
Brazilian
researchers performed an observational study from October 1987 to
February 2001 on immunologic and clinical outcome of 148 HIV-1-infected
patients from an open clinical cohort at Sao Paulo University, Brazil.
The
median T CD4+ at starting first monitored regimen was 227 cells
per microliter, with 65% of patients previously exposed to antiretroviral
regimens, mostly dual therapy.
Virologic
response to antiretroviral therapy, after a median period of 179
weeks of monitored treatment, allowed classifying patients as aviremic
(RNA plasma viremia below 500 copies per milliliter); viremic
(current viral load at historic levels), and viremic-attenuated
groups (detectable viremia, but > 1 log viral suppression).
HIV
RNA viral load, T CD4+ cells count, HIV-1 pol sequencing, inflammatory
parameters, and clinical events were documented during a median
follow-up of 251 weeks.
This
study observed better clinical and immunologic responses in the
aviremic group, but the viremic-attenuated group showed a significant
gain in CD4+ cells (p < 0.013) and a decreased number of cases
progressing to an AIDS-defining clinical condition (p < 0.001)
compared to the viremic group.
Adolfo
Lutz Institute, Sao Paulo, Brazil; Brazilian AIDS Program, MS, Brazilia,
Brazil.
05/26/04
Reference
L
Brigido and others. CD4+ T-cell recovery and clinical outcome in HIV-1-infected
patients exposed to multiple antiretroviral regimens: partial control
of viremia is associated with favorable outcome. AIDS Patient Care STDS
18(4): 189-198. April 2004.
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