The role of viral phenotype and CCR-5 gene defects in HIV-1 transmission and disease progression

被引:416
|
作者
Michael, NL
Chang, G
Louie, LG
Mascola, JR
Dondero, D
Birx, DL
Sheppard, HW
机构
[1] HENRY M JAKCSON FDN,ROCKVILLE,MD 20850
[2] UNIV CALIF BERKELEY,SCH PUBL HLTH,BERKELEY,CA 94720
[3] USN,MED RES INST,DEPT INFECT DIS,BETHESDA,MD 20889
[4] CALIF DEPT HLTH SERV,BERKELEY,CA 94704
关键词
D O I
10.1038/nm0397-338
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Delta ellular entry of human immunodeficiency virus type 1 (HIV-1) requires binding to both CD4 (ref. 1, 2) and to one of the chemokine receptors recently discovered to act as coreceptors(3-11). Viruses that infect T-cell lines to form syncytia (syncytium-inducing, SI) are frequently found in late-stage HIV disease and utilize the chemokine receptor CXCR-4; macrophage-tropic viruses are non-syncytium-inducing (NSI), found throughout disease and utilize CCR-5 (ref. 3-11). We postulated that CCR-5 gene defects might reduce infection risk in seronegative subjects and prolong AIDS-free survival in seropositive subjects with NSI but not SI virus. Homozygous (Delta ccr5/Delta ccr5) and heterozygous (CCR5/Delta ccr5) CCR-5 deletions (Delta ccr5)(12,13) were found in 7 (2.7%) and 51 (19.5%), respectively, of 261 seronegative subjects from the San Francisco Men's Health Study. CCR-5/Delta ccr5 genotype was identified in 33 of 172 (19.2%) nonprogressors and 25 of 234 (10.7%) progressors from the seropositive arm of this cohort. The Delta ccr5 allele conferred a significant protective effect against HIV-1 infection (P = 0.001) and a survival advantage against disease progression (P = 0.02). Although both progressing and nonprogressing CCR5/Delta ccr5 subjects were identified, a distinct survival advantage was shown for those with NSI virus (P < 0.0001). Thus, the protective effect of Delta ccr5 against disease progression is lost when the infecting virus uses CXCR-4 as a coreceptor.
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页码:338 / 340
页数:3
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