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1型人类免疫缺陷病毒V3序列与艾滋病期间痴呆症的发展

HIV type 1 V3 sequences and the development of dementia during AIDS.

作者信息

Di Stefano M, Wilt S, Gray F, Dubois-Dalcq M, Chiodi F

机构信息

Microbiology and Tumor Biology Center, Karolinska Institute, Stockholm, Sweden.

出版信息

AIDS Res Hum Retroviruses. 1996 Apr 10;12(6):471-6. doi: 10.1089/aid.1996.12.471.

Abstract

The most frequent neurological complication of AIDS is a dementia-like syndrome. Power and collaborators (J Virol 1994; 68:4643-4649) have reported an association between the clinical signs of AIDS dementia and the amino acid composition of two positions (305 and 329) within the V3 region of HIV-1 strains amplified from brain tissue. Similarly, we analyzed position 305 in the V3 region of HIV-1 present in the brain or cerebrospinal fluid of 25 nondemented subjects at different clinical stages of HIV-1 infection. Our results are, however, at variance with the findings presented by Power and colleagues. Histidine, found to be common among sequences derived from demented patients, was also present in the majority (16 of 25) of nondemented patients analyzed by us. In the hands of Power and colleagues, sequences derived from nondemented patients contained proline at position 305. None of our patients had proline in this position. We also asked the question whether the presence of a specific amino acid at position 305 of the V3 loop is linked to an increased capacity of HIV-1 isolates to infect primary microglial cells, the major target cell for HIV-1 infection in the brain. Primary HIV-1 isolates derived from blood and cerebrospinal fluid of five patients, two asymptomatic and three AIDS patients, were used to infect microglia cell cultures. Infection was monitored by syncytium formation and by p24 antigen release in the culture supernatant. All but one of the paired blood/CSF isolates replicated in human brain cultures. Replication occurred independently from the amino acid present at position 305 of the V3 region of the viral envelope. Our results indicate that the majority of HIV-1 isolates, even derived during the asymptomatic stage, have the capacity to infect microglial cells. The relevance of viral envelope sequences in determining tropism for microglial cells and development of neurological symptoms remains an open question.

摘要

艾滋病最常见的神经并发症是一种类似痴呆的综合征。鲍尔及其同事(《病毒学杂志》,1994年;68:4643 - 4649)报告称,艾滋病痴呆的临床症状与从脑组织中扩增出的HIV - 1毒株V3区域内两个位置(305和329)的氨基酸组成之间存在关联。同样,我们分析了25名处于HIV - 1感染不同临床阶段的未患痴呆受试者的脑或脑脊液中HIV - 1 V3区域的305位。然而,我们的结果与鲍尔及其同事的发现不一致。在痴呆患者的序列中常见的组氨酸,在我们分析的大多数(25例中的16例)未患痴呆患者中也存在。在鲍尔及其同事的研究中,未患痴呆患者的序列在305位含有脯氨酸。我们的患者在该位置均无脯氨酸。我们还提出了一个问题,即V3环305位特定氨基酸的存在是否与HIV - 1分离株感染原代小胶质细胞(脑中HIV - 1感染的主要靶细胞)的能力增强有关。从5名患者(2名无症状患者和3名艾滋病患者)的血液和脑脊液中分离出的原发性HIV - 1毒株用于感染小胶质细胞培养物。通过多核巨细胞形成和培养上清液中p24抗原释放来监测感染情况。除一对血液/脑脊液分离株中的一个外,其他所有分离株均在人脑培养物中复制。复制的发生与病毒包膜V3区域305位存在的氨基酸无关。我们的结果表明,大多数HIV - 1分离株,即使是在无症状阶段获得的,都有感染小胶质细胞的能力。病毒包膜序列在决定对小胶质细胞的嗜性和神经症状发展方面的相关性仍然是一个悬而未决的问题。

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