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CD4 and MHC-I downregulation are conserved in primary HIV-1 Nef alleles from brain and lymphoid tissues, but Pak2 activation is highly variable

期刊

VIROLOGY
卷 358, 期 1, 页码 119-135

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.virol.2006.07.053

关键词

human immunodeficiency virus type 1 (HIV-1); Nef; brain; lymph node; CD4; MHC-1; Pak2

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资金

  1. NIAID NIH HHS [AI33331, R01 AI033331] Funding Source: Medline
  2. NINDS NIH HHS [NS37277, R01 NS037277, R01 NS035734, NS35734] Funding Source: Medline

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HIV-1 compartmentalization in the CNS has been demonstrated for gag, pol, and env genes. However, little is known about tissue compartmentalization of nef genes and their functional characteristics in brain. We have cloned 97 nef genes and characterized 10 Nef proteins from autopsy brain and lymphoid tissues from 2 patients with AIDS and HIV-1-associated dementia. Distinct compartmentalization of brain versus lymphoid nef genes was demonstrated within each patient. CD4 and MHC-I downregulation were conserved in all tissue-derived Nefs. However, MHC-I downregulation by brain-derived Nefs was weaker than downregulation by lymphoid-derived Nefs. The motifs KEEE- or EKEE- at the PACs-1 binding site represented brain-specific signature patterns in these 2 patients and contributed to the reduced MHC-1 downregulation activity of brain-derived Nets from these patients. Pak2 association was highly variable in Nets from both patients. Three of 10 tissue-derived Nets coimmunoprecipitated activated Pak2, with strong association demonstrated for only 2 Nefs. The ability of Nef to associate with activated Pak2 did not correlate with brain or lymphoid tissue origin. Nef genes from viruses isolated from brain by coculture with PBMC were not closely related to sequences amplified directly from brain tissue, suggesting that viral selection or adaptation occurred during coculture. This study of tissue-derived HIV-1 Nets demonstrates that CD4 and MHC-1 downregulation are highly conserved Nef functions, while Pak2 association is variable in late stage AIDS patients. (c) 2006 Elsevier Inc. All rights reserved.

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