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Role of Microglial Cells in Selective Replication of Simian Immunodeficiency Virus Genotypes in the Brain

机译:小胶质细胞在猴中的猿猴免疫缺陷病毒基因型的选择性复制中的作用。

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摘要

An accelerated, consistent macaque simian immunodeficiency virus (SIV) model in which over 90% of pigtailed macaques (Macaca nemestrina) coinoculated with SIV/17E-Fr and SIV/DeltaB670 developed encephalitis was used to determine whether central nervous system (CNS) lesions are associated with the replication of specific genotypes in the brain and, more specifically, in the microglia. Ten of 11 inoculated macaques had severe (n = 3), moderate (n = 5), or mild (n = 2) encephalitis at 3 months postinoculation. To compare actively replicating viral genotypes in the CNS and in microglia with those in the periphery, the V1 region of the SIV envelope gene was amplified and sequenced from RNA extracted from basal ganglia, from microglial cells isolated from the brain, and from peripheral blood mononuclear cells (PBMC) isolated from blood at the time of death. To distinguish between actively replicating with latent viral genotypes in the CNS, viral genotypes in RNA and DNA from basal ganglia were compared. Two macrophage-tropic, neurovirulent viruses, SIV/17E-Fr and SIV/DeltaB670 Cl-2, predominated in the brain RNA of macaques with encephalitis, comprising 95% of the genotypes detected. The same two viral genotypes were present at the same frequencies in microglial cell RNA, suggesting that microglia are pivotal in the selective replication of neurovirulent viruses. There was a significantly greater number of viral genotypes in DNA than there were in RNA in the brain (P = 0.004), including those of both the macrophage- and lymphocyte-tropic viral strains. Furthermore, significantly fewer viral genotypes were detected in brain RNA than in PBMC RNA at the time of death (P = 0.004) and the viral strain that predominated in the brain frequently was different from that which predominated in the PBMC of the same animal. These data suggest that many viral genotypes enter the brain, but only a limited subset of macrophage-tropic, neurovirulent viruses replicate terminally in the brains of macaques with encephalitis. They further suggest that the selection of macrophage-tropic, neurovirulent viruses occurs not at the level of the blood-brain barrier but at a stage after virus entry and that microglial cells may play an important role in that selection process.
机译:一种加速一致的猕猴猿猴免疫缺陷病毒(SIV)模型,其中超过90%的猪尾猕猴(Macaca nemestrina)接种了SIV / 17E-Fr和SIV / DeltaB670发达的脑炎,用于确定中枢神经系统(CNS)病变是否与特定基因型在大脑中,尤其是在小胶质细胞中的复制有关。在接种后3个月,接种的11只猕猴中有10只患有严重(n = 3),中度(n = 5)或轻度(n = 2)脑炎。为了比较中枢神经系统和小胶质细胞与周围神经元中主动复制的病毒基因型,从基底神经节,从大脑分离的小胶质细胞和外周血单核中提取的RNA扩增并测序了SIV包膜基因的V1区死亡时从血液中分离出的细胞(PBMC)。为了区分中枢神经系统中潜在病毒基因型的主动复制,比较了来自基底神经节的RNA和DNA中的病毒基因型。在患有脑炎的猕猴的脑RNA中占主导地位的是两种嗜巨噬细胞型,神经毒性病毒SIV / 17E-Fr和SIV / DeltaB670 Cl-2,占所检测基因型的95%。小胶质细胞RNA中相同的两种病毒基因型以相同的频率出现,表明小胶质细胞在神经毒性病毒的选择性复制中起着关键作用。在大脑中,DNA中的病毒基因型数量明显多于RNA中的病毒基因型数量(P = 0.004),包括巨噬细胞型和淋巴细胞型病毒株。此外,在死亡时,脑RNA中检测到的病毒基因型明显少于PBMC RNA(P = 0.004),并且在脑中占主导地位的病毒株与同一动物的PBMC中占主导地位的病毒株不同。这些数据表明,许多病毒基因型进入大脑,但只有一部分巨噬细胞嗜性神经毒性病毒最终在患有脑炎的猕猴的大脑中复制。他们进一步表明,选择巨噬细胞型,神经毒性病毒不是在血脑屏障水平上发生,而是在病毒进入后的某个阶段发生,而小胶质细胞可能在选择过程中发挥重要作用。

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