Publication

Functional and structural defects in HIV type 1 nef genes derived from pediatric long-term survivors

Journal Paper/Review - Nov 20, 2000

Units
PubMed
Doi

Citation
Geffin R, Wolf D, Müller R, Hill M, Stellwag E, Freitag M, Sass G, Scott G, Baur A. Functional and structural defects in HIV type 1 nef genes derived from pediatric long-term survivors. AIDS research and human retroviruses 2000; 16:1855-68.
Type
Journal Paper/Review (English)
Journal
AIDS research and human retroviruses 2000; 16
Publication Date
Nov 20, 2000
Issn Print
0889-2229
Pages
1855-68
Brief description/objective

DNA sequences and three distinct in vitro functions of Nef were evaluated in a group of seven perinatally infected children. nef gene sequences obtained before and after virus culture showed that one of the five non-/slow progressors harbored a virus with large deletions. nef genes from the remaining four children were full length but contained discrete changes at a higher frequency than the rapid progressors. In functional studies, 40 of 44 Nef proteins derived from the whole study group were capable of binding the cellular serine kinase p62, indicating that this function is well conserved among naturally occurring viruses. In contrast, representative Nef proteins derived from the long-term non-/slow progressors were found to be defective or far less capable of enhancing viral replication and/or viral infectivity in herpesvirus saimiri-transformed human T cells and peripheral blood mononuclear cells. On reversion of highly prevalent point mutations in the defective proteins, viral replication could be restored to wild-type levels. Our results suggest that nef genes derived from pediatric long-term nonprogressors have gross deletions in isolated cases but a higher prevalence of discrete changes that may impair Nef function in primary T cell assays, but not all functions reported for Nef.