Surrogate markers for survival in patients with AIDS and AIDS related complex treated with zidovudine
M A Jacobson, P Bacchetti, A Kolokathis, R E Chaisson, S Szabo, B Polsky, G T Valainis, D Mildvan, D Abrams, J Wilber, M A Jacobson, P Bacchetti, A Kolokathis, R E Chaisson, S Szabo, B Polsky, G T Valainis, D Mildvan, D Abrams, J Wilber
Abstract
Objective: To determine whether early effects of zidovudine treatment on CD4+ lymphocyte count and concentrations of beta 2 microglobulin, neopterin, or HIV p24 antigen or antibody are correlated with survival in patients with AIDS or AIDS related complex.
Design: Retrospective study of changes in laboratory markers and survival.
Setting: Multicentre trial at university hospital clinics.
Subjects: 90 Patients with AIDS or AIDS related complex.
Intervention: Patients started zidovudine 200 mg orally every four hours. Fifty six of the patients died a median 17 months after starting zidovudine; the remaining 34 patients were followed up for a median 25.5 months.
Main outcome measures: Changes in CD4+ lymphocyte count and serum concentrations of p24 antigen and antibody, beta 2 microglobulin, and neopterin; survival of the patient.
Results: The pretreatment characteristics that independently predicted poor survival were determined using a multivariate proportional hazards model: a diagnosis of AIDS (v AIDS related complex), age over 45 years, and the logarithm of serum neopterin concentration. When these baseline characteristics were controlled for the logarithm of CD4+ lymphocyte count at weeks 8-12 of treatment (p = 0.007) and an increase in serum beta 2 microglobulin concentration at weeks 8-12 (p = 0.05) also independently correlated with survival. In the 38 patients with a better pretreatment prognosis, 24 month survival estimated by the product-limit method was 88% for those with a good response on both surrogate markers during early treatment compared with only 50% for those with a poor response on either marker. In the 38 with a worse pretreatment prognosis, 24 month survival was estimated to be 49% for those with a good response on both surrogate markers compared with only 18% for those with a poor response on either.
Conclusion: These data suggest that CD4+ lymphocyte count at 8-12 weeks and, perhaps, change in serum beta 2 microglobulin concentration could be surrogate end points for clinical outcome in trials of antiretroviral drugs for patients with HIV disease.
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Source: PubMed