DISTINCT EFFECTS IN PRIMARY MACROPHAGES AND LYMPHOCYTES OF THE HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 ACCESSORY GENES VPR, VPU, AND NEF - MUTATIONAL ANALYSIS OF A PRIMARY HIV-1 ISOLATE

被引：215

作者：

BALLIET, JW

KOLSON, DL

EIGER, G

KIM, FM

MCGANN, KA

SRINIVASAN, A

COLLMAN, R

机构：

[1] UNIV PENN,SCH MED,DEPT MED,DIV PULM & CRIT CARE,PHILADELPHIA,PA 19104

[2] UNIV PENN,SCH MED,DEPT MICROBIOL,PHILADELPHIA,PA 19104

[3] UNIV PENN,SCH MED,DEPT NEUROL,PHILADELPHIA,PA 19104

[4] UNIV PENN,SCH MED,DEPT PEDIAT,PHILADELPHIA,PA 19104

[5] WISTAR INST ANAT & BIOL,PHILADELPHIA,PA 19104

来源：

VIROLOGY | 1994年 / 200卷 / 02期

关键词：

D O I：

10.1006/viro.1994.1225

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

Macrophages and lymphocytes are the two main targets for productive HIV-1 infection in vivo. To compare the effects of the ''nonessential'' HIV-1 accessory genes vpr, vpu, and nef on Viral replication in these primary cell types, we generated a panel of mutant viruses derived from a molecularly cloned macrophage-tropic HIV-1 primary isolate. Mutant viruses had markedly different patterns of replication in macrophages, in contrast to lymphocytes in which differences were modest. Loss of vpr or vpu reduced viral antigen production in macrophages by up to 1000-fold, while replication in lymphocytes was only marginally affected. Loss of nef did not affect lymphocyte infection, but decreased replication in macrophages to a small extent. Mutation of multiple accessory genes restricted replication in both cell types, but to a much greater extent in macrophages, and frequently resulted in nonproductive infection. The degree to which replication depended on intact accessory genes varied in macrophages from different donors. The essential functions of these accessory genes in HIV-1 infection may be related to their combined effects in facilitating productive infection of macrophages. (C) 1994 Academic Press, Inc.

引用

页码：623 / 631

页数：9

共 32 条

[1] NEF FROM PRIMARY ISOLATES OF HUMAN-IMMUNODEFICIENCY-VIRUS TYPE-1 SUPPRESSES SURFACE CD4 EXPRESSION IN HUMAN AND MOUSE T-CELLS [J].