Virus particle core defects caused by mutations in the human immunodeficiency virus capsid N-terminal domain.

J Virol

Vollum Institute and Department of Microbiology, Mail Code L220, Oregon Health & Science University, 3181 SW Sam Jackson Park Rd., Portland, OR 97201-3098, USA.

Published: February 2005

AI Article Synopsis

  • The N-terminal domains of the HIV-1 capsid protein form hexamer rings in virus cores, with their assembly influenced by pH.
  • Mutations at histidine residue 84 (H84) affect the assembly and infection capability of the virus, while mutations at histidine 87 (H87) maintain infectivity.
  • H84 mutations lead to poorly infectious viruses with abnormal core structures, indicating its role in hexamer assembly and organization.

Article Abstract

The N-terminal domains (NTDs) of the human immunodeficiency virus type 1 (HIV-1) capsid (CA) protein have been modeled to form hexamer rings in the mature cores of virions. In vitro, hexamer ring units organize into either tubes or spheres, in a pH-dependent fashion. To probe factors which might govern hexamer assembly preferences in vivo, we examined the effects of mutations at CA histidine residue 84 (H84), modeled at the outer edges of NTD hexamers, as well as a nearby histidine (H87) in the cyclophilin A (CypA) binding loop. Although mutations at H87 yielded infectious virions, mutations at H84 produced assembly-competent but poorly infectious virions. The H84 mutant viruses incorporated wild-type levels of CypA and viral RNAs and showed nearly normal signals in virus entry assays. However, mutant CA proteins assembled aberrant virus cores, and mutant core fractions retained abnormally high levels of CA but reduced reverse transcriptase activities. Our results suggest that HIV-1 CA residue 84 contributes to a structure which helps control either NTD hexamer assembly or the organization of hexamers into higher-order structures.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC544128PMC
http://dx.doi.org/10.1128/JVI.79.3.1470-1479.2005DOI Listing

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