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嗜淋巴细胞性猴免疫缺陷病毒可在恒河猴大脑中引起持续性感染。

Lymphocyte-tropic simian immunodeficiency virus causes persistent infection in the brains of rhesus monkeys.

作者信息

Stephens E B, Liu Z Q, Zhu G W, Adany I, Joag S V, Foresman L, Berman N E, Narayan O

机构信息

Department of Microbiology, Molecular Genetics and Immunology, Marion Merrell Dow Laboratory for Viral Pathogenesis, University of Kansas Medical Center, Kansas City 66160-7240, USA.

出版信息

Virology. 1995 Nov 10;213(2):600-14. doi: 10.1006/viro.1995.0032.

Abstract

Molecularly cloned SIVmac239 is the prototypical SIVmac lymphocyte-tropic virus that replicates productively in lymphocytes but poorly in macrophages. In macaques, the virus causes activation and productive infection of T lymphocytes which invade the central nervous system (CNS) early after infection in the animal. However, infected animals develop immunosuppression and AIDS but rarely overt neurological disease. In this study, we examined multiple regions of the brain and spinal cord for the presence of SIV env sequences and histological lesions in five macaques that had been infected with SIVmac239 for 1.7 to 2.25 years. Histopathological examination of the brain revealed no lesions consistent with encephalitis; however, viral DNA was found in all five brains. In one animal the virus caused infection in a widely disseminated pattern from the frontal cortex to the distal end of the spinal cord, whereas in the other four animals infection in the CNS occurred in a nonspecific, focal pattern. Sequence analyses were performed on gp120 sequences isolated from selected regions of the CNS and compared to gp120 sequences isolated from corresponding lymph nodes, a tissue known to support productive replication of SIVmac239. Examination of the viral sequences from the CNS tissue from two animals (macaques 10F and 14F) revealed a low mutation rate when compared to the sequences isolated from the lymph node tissues. The percentage change in the amino acid sequence was approximately 1% for CNS clones versus > or = 3% for clones isolated from the lymph node. The majority of the CNS viral sequences of macaques 10F and 14F had none of the genetic markers shown in a previous study to be associated with macrophage-tropic variants and indeed retained a nucleotide sequence of similar to the original lymphocyte-tropic virus used for inoculation despite almost 2 years of persistent infection in the animals. Construction of chimeric viruses with V1-V5 regions of selected macaque 10F and macaque 14F CNS-gp120 clones confirmed the predicted lymphocyte-tropic nature of these env genes. In contrast, the gp120 sequences isolated from the CNS tissue of one of the other three animals (macaque 13F) had a mutation rate comparable to that observed for the lymph node clones. The CNS clones from this animal had amino acid substitutions that were previously shown to be associated with macrophage tropism. Compared to the chimeric viruses constructed with V1-V5 sequences from macaques 10F and 14F, viruses constructed with the V1-V5 sequences of several macaque 13F brain clones did not yield infectious virus.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

分子克隆的SIVmac239是典型的嗜淋巴细胞性SIVmac病毒,它能在淋巴细胞中高效复制,但在巨噬细胞中复制能力较差。在猕猴中,该病毒可导致T淋巴细胞活化并产生有效感染,这些T淋巴细胞在动物感染后早期就侵入中枢神经系统(CNS)。然而,受感染的动物会出现免疫抑制和艾滋病,但很少出现明显的神经疾病。在本研究中,我们检查了5只感染SIVmac239达1.7至2.25年的猕猴的脑和脊髓的多个区域,以检测SIV env序列的存在和组织学病变。脑的组织病理学检查未发现与脑炎一致的病变;然而,在所有5只猕猴的脑中均发现了病毒DNA。在1只动物中,病毒以广泛播散的模式从额叶皮质感染至脊髓远端,而在其他4只动物中,CNS中的感染呈非特异性的局灶性模式。对从CNS选定区域分离的gp120序列进行了序列分析,并与从相应淋巴结分离的gp120序列进行比较,淋巴结是已知支持SIVmac239有效复制的组织。对2只动物(猕猴10F和14F)CNS组织中的病毒序列进行检查发现,与从淋巴结组织分离的序列相比,其突变率较低。CNS克隆的氨基酸序列变化百分比约为1%,而从淋巴结分离的克隆的氨基酸序列变化百分比≥3%。猕猴10F和14F的大多数CNS病毒序列没有先前研究中显示与嗜巨噬细胞性变体相关的遗传标记,并且尽管在动物中持续感染了近2年,但实际上保留了与用于接种的原始嗜淋巴细胞性病毒相似的核苷酸序列。用选定的猕猴10F和猕猴14F CNS - gp120克隆的V1 - V5区域构建嵌合病毒,证实了这些env基因具有预测的嗜淋巴细胞性。相比之下,从其他3只动物之一(猕猴13F)的CNS组织分离的gp120序列的突变率与在淋巴结克隆中观察到的相当。该动物的CNS克隆具有先前显示与巨噬细胞嗜性相关的氨基酸替代。与用猕猴10F和14F的V1 - V5序列构建的嵌合病毒相比,用几只猕猴13F脑克隆的V1 - V5序列构建的病毒不能产生感染性病毒。(摘要截短于400字)

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