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一种编码来自CCR5嗜性HIV-1 Ba-L包膜基因的猿猴人类免疫缺陷病毒的特性分析。

Characterization of a simian human immunodeficiency virus encoding the envelope gene from the CCR5-tropic HIV-1 Ba-L.

作者信息

Pal Ranajit, Taylor Brian, Foulke J Scott, Woodward Ruth, Merges Michael, Praschunus Rob, Gibson Andrew, Reitz Marvin

机构信息

Advanced BioScience Laboratories, Kensington, Maryland, USA.

出版信息

J Acquir Immune Defic Syndr. 2003 Jul 1;33(3):300-7. doi: 10.1097/00126334-200307010-00003.

Abstract

The tat, rev, vpu, and env genes from the monocytotropic CCR5-dependent HIV-1 Ba-L isolate were substituted for homologous simian immunodeficiency virus (SIV) sequences in the SIV genome. The resultant SHIV (SHIV Ba-L) replicated in CCR5-positive PM-1 cells but not in CCR5-negative CEMX174 cells. Infection of HOS cells expressing different co-receptors showed SHIV Ba-L to be strictly CCR5-dependent. Infection of PM-1 cells and rhesus peripheral blood mononuclear cells (PBMCs) was highly sensitive to RANTES but not to SDF-1. Although SHIV Ba-L infected rhesus and pigtail macaques intravenously or rectally, plasma viremia was controlled after 3 weeks. After serial passage through 4 pigtails by blood and bone marrow transfer, virus from pigtail PBMCs had higher in vitro infectious titers on rhesus PBMCs and was efficiently transmitted vaginally in rhesus and cynomolgus macaques. Plasma viremia generally persisted longer than after infection with unpassaged virus but was eventually controlled with no significant decrease in CD4+ T-cell counts in peripheral blood. The envelope gene of SHIV Ba-L revealed a very little genetic drift during in vivo passage. SHIV Ba-L provides a potentially useful model for R5 HIV-1 infection of humans.

摘要

将嗜单核细胞的CCR5依赖性HIV-1 Ba-L分离株的tat、rev、vpu和env基因替换为SIV基因组中的同源猴免疫缺陷病毒(SIV)序列。所得的SHIV(SHIV Ba-L)在CCR5阳性的PM-1细胞中复制,但不在CCR5阴性的CEMX174细胞中复制。对表达不同共受体的HOS细胞进行感染,结果显示SHIV Ba-L严格依赖CCR5。对PM-1细胞和恒河猴外周血单个核细胞(PBMC)的感染对RANTES高度敏感,但对SDF-1不敏感。尽管SHIV Ba-L通过静脉内或直肠途径感染恒河猴和猪尾猕猴,但3周后血浆病毒血症得到控制。通过血液和骨髓转移在4只猪尾猕猴中连续传代后,来自猪尾猕猴PBMC的病毒对恒河猴PBMC具有更高的体外感染滴度,并能有效地经阴道传播给恒河猴和食蟹猕猴。血浆病毒血症通常比感染未传代病毒后持续的时间更长,但最终得到控制,外周血中CD4+ T细胞计数没有显著下降。SHIV Ba-L的包膜基因在体内传代过程中显示出很少的基因漂移。SHIV Ba-L为人类R5 HIV-1感染提供了一个潜在有用的模型。

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