Apoptosis as a mechanism of cell death in cultured T lymphoblasts acutely infected with HIV-1.
C Terai, RS Kornbluth, CD Pauza… - The Journal of …, 1991 - Am Soc Clin Investig
C Terai, RS Kornbluth, CD Pauza, DD Richman, DA Carson
The Journal of clinical investigation, 1991•Am Soc Clin InvestigThe mechanisms by which HIV-1 infection kills T lymphocytes are not clearly established.
Apoptosis is an internally programmed cell death pathway that may regulate both T cell
development and senescence, and that is characterized by cleavage of DNA at
internucleosomal regions. The present experiments show that acute HIV-1 infection of MT2
lymphoblasts and activated normal peripheral blood mononuclear cells induces apoptosis.
The addition of anti-gp120 neutralizing antibody, after HIV-1 infection of MT2 cells, permitted …
Apoptosis is an internally programmed cell death pathway that may regulate both T cell
development and senescence, and that is characterized by cleavage of DNA at
internucleosomal regions. The present experiments show that acute HIV-1 infection of MT2
lymphoblasts and activated normal peripheral blood mononuclear cells induces apoptosis.
The addition of anti-gp120 neutralizing antibody, after HIV-1 infection of MT2 cells, permitted …
The mechanisms by which HIV-1 infection kills T lymphocytes are not clearly established. Apoptosis is an internally programmed cell death pathway that may regulate both T cell development and senescence, and that is characterized by cleavage of DNA at internucleosomal regions. The present experiments show that acute HIV-1 infection of MT2 lymphoblasts and activated normal peripheral blood mononuclear cells induces apoptosis. The addition of anti-gp120 neutralizing antibody, after HIV-1 infection of MT2 cells, permitted sustained high levels of viral replication, but blocked apoptosis and cell death. Apoptosis may account for the direct cytopathologic effects of HIV-1 in T cells.
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The Journal of Clinical Investigation