Protection from secondary human immunodeficiency virus type 1 infection inchimpanzees suggests the importance of antigenic boosting and a possible role for cytotoxic T cells
Ss. Balla-jhagjhoorsingh et al., Protection from secondary human immunodeficiency virus type 1 infection inchimpanzees suggests the importance of antigenic boosting and a possible role for cytotoxic T cells, J INFEC DIS, 184(2), 2001, pp. 136-143
Recent evidence suggests a much higher prevalence of human immunodeficiency
virus type 1 (HIV-1) recombinants than previously anticipated. These recom
binants arise from secondary HIV infections in individuals already infected
with the virus. It remains unclear why some individuals acquire secondary
HIV-1 infections and others do not. To address this question, a study was u
ndertaken of a small cohort of chimpanzees with well-defined HIV-1 infectio
n. After exposure to an infectious dose of heterologous primary isolate, 4
of 8 HIV-1 seropositive chimpanzees resisted secondary infection, whereas 2
naive controls became readily infected. Only animals who were immunologica
lly boosted were protected. Protection from heterologous secondary exposure
appeared to be related to the repertoire of the cytolytic CD8(+) T cell re
sponses to HIV-1. Data suggested that immunologic boosting by HIV-1 antigen
s or exposure to subinfectious doses of virus may be important events in su
staining sufficient immunity to prevent secondary infections from occurring
.