HIV Infections Clinical Trial
Official title:
A Pilot Study of the Short-Term Effects of Antiretroviral Management Based on Plasma Genotypic Antiretroviral Resistance Testing (GART) Compared With Antiretroviral Management Without Plasma GART
To determine the short-term virologic and immunologic effects of using plasma genotypic
antiretroviral resistance testing (GART) results (interpreted by study virologists AS PER
AMENDMENT 9/17/97) in the management of therapy for antiretroviral-experienced patients
failing on one of the following regimens:
1. zidovudine (ZDV) + (lamivudine) 3TC + (indinavir) IDV
2. ZDV + 3TC + saquinavir (SQV)
3. ZDV + 3TC + ritonavir (RTV)
4. stavudine (d4T) + 3TC + IDV. [AS PER AMENDMENT 11/26/97: To determine the short-term
effects of using plasma GART in the management of antiretroviral-experienced patients
failing on a triple drug regimen that includes a single protease inhibitor (indinavir
[IDV], saquinavir [SQV], ritonavir [RTV], or nelfinavir [NFV]) and two licensed
nucleoside reverse transcriptase inhibitors (NRTIs).] A growing body of evidence
suggests that antiretroviral resistance is associated with an increased risk of disease
progression and death. All commercially available antiretrovirals and many of those in
development have been associated with resistance. Fortunately, techniques are available
to define HIV genotypic resistance in "real time" as compared to techniques that
measure phenotypic resistance that is not practical in a clinical setting. Using
genotypic antiretroviral resistance testing (GART) results, along with other currently
available markers, may lead to improved treatment decisions compared with using
currently available markers alone.
A growing body of evidence suggests that antiretroviral resistance is associated with an
increased risk of disease progression and death. All commercially available antiretrovirals
and many of those in development have been associated with resistance. Fortunately,
techniques are available to define HIV genotypic resistance in "real time" as compared to
techniques that measure phenotypic resistance that is not practical in a clinical setting.
Using genotypic antiretroviral resistance testing (GART) results, along with other currently
available markers, may lead to improved treatment decisions compared with using currently
available markers alone.
128 patients are randomized to GART or no GART within each of four strata defined by current
antiretroviral regimen:
1. ZDV plus 3TC plus IDV
2. ZDV plus 3TC plus SQV
3. ZDV plus 3TC plus RTV
4. d4T plus 3TC plus IDV. Each of the four strata contains 22 patients with CD4+ counts of
50 - 199/mm3 and 11 patients with CD4+ counts of 200 - 500/mm3. Upon randomization,
clinicians determine a treatment strategy with supplied baseline GART results (GART
arm) or without them (no-GART arm). All patients remain on the triple antiretroviral
regimen initiated at the randomization visit until at least the 8-week visit. At this
time, changes in treatment will be allowed based on an inadequate response to therapy.
[AS PER AMENDMENT 9/17/97: 128 patients are randomized to therapy based on GART results or
therapy not based on these results. Patients are stratified into 8 groups defined by current
antiretroviral regimen (ZDV/3TC/IDV vs. ZDV/3TC/SQV vs. ZDV/3TC/RTV vs. d4T/3TC/IDV) and
screening CD4+ count (50-199 vs. 200-500). Management of patients assigned to the GART group
is based on recommendations of study virologists after independent review of patient plasma
GART results in addition to current clinical practice. Up to four different treatment
regimens using only licensed drugs may be recommended, ranked but considered approximately
therapeutically equivalent. The management of patients assigned to the no-GART group is
based on current clinical practice and includes only licensed antiretrovirals.] [AS PER
AMENDMENT 11/26/97: 160 patients are randomized to GART or no GART within each of 8 strata
defined by current antiretroviral regimen (NRTI-1 plus NRTI-2 plus IDV vs. NRTI-1 plus
NRTI-2 plus SQV vs. NRTI-1 plus NRTI-2 plus RTV vs. NRTI-1 plus NRTI-2 plus NFV) and
screening CD4+ cell count.]
;
Observational Model: Cohort, Time Perspective: Prospective
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