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Cellular and Molecular Life Sciences: CMLS logoLink to Cellular and Molecular Life Sciences: CMLS
. 2008 May 26;65(20):3134–3144. doi: 10.1007/s00018-008-8147-6

Role of HIV Gp41 mediated fusion/hemifusion in bystander apoptosis

H Garg 1, R Blumenthal 1,
PMCID: PMC2574860  NIHMSID: NIHMS57116  PMID: 18500445

Abstract.

Mechanisms of HIV-mediated CD4+ T cell loss leading to immunodeficiency are amongst the most extensively studied yet unanswered questions in HIV biology. The level of CD4+ T cell depletion in HIV infected patients far exceeds the number of infected T cells, suggesting an indirect mechanism of HIV pathogenesis termed bystander cell death. Evidence is accumulating that the HIV envelope glycoprotein (Env) is a major determinant of HIV pathogenesis and plays a critical role in bystander cell death. The complex structure and function of HIV Env makes the determination of the mechanism of Envmediated apoptosis more complex than previously thought. This review will examine the complex relationship between HIV Env phenotype, coreceptor expression and immune activation in determining HIV pathogenesis. We review data here corresponding to the role of HIV Env hemifusion activity in HIV pathogenesis and how it interplays with other AIDS associated factors such as chemokine receptor expression and immune activation.

Keywords. HIV-1, Env, pathogenesis, fusion, hemifusion, apoptosis, gp41, CD4 Cells

Footnotes

Received 21 March 2008; received after revision 29 April 2008; accepted 30 April 2008


Articles from Cellular and Molecular Life Sciences: CMLS are provided here courtesy of Springer

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