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本文引用的文献

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Multifactorial nature of noncytolytic CD8+ T cell-mediated suppression of HIV replication: beta-chemokine-dependent and -independent effects.非细胞溶解性CD8 + T细胞介导的HIV复制抑制的多因素性质:β-趋化因子依赖性和非依赖性效应。
AIDS Res Hum Retroviruses. 1997 Jan 1;13(1):63-9. doi: 10.1089/aid.1997.13.63.
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Sensitivity to inhibition by beta-chemokines correlates with biological phenotypes of primary HIV-1 isolates.对β趋化因子抑制作用的敏感性与原发性HIV-1分离株的生物学表型相关。
Proc Natl Acad Sci U S A. 1996 Dec 24;93(26):15382-7. doi: 10.1073/pnas.93.26.15382.
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Role of beta-chemokines in suppressing HIV replication.β趋化因子在抑制HIV复制中的作用。
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HIV replication in CD4+ T cells of HIV-infected individuals is regulated by a balance between the viral suppressive effects of endogenous beta-chemokines and the viral inductive effects of other endogenous cytokines.HIV感染者CD4+ T细胞中的HIV复制,受内源性β趋化因子的病毒抑制作用与其他内源性细胞因子的病毒诱导作用之间的平衡所调控。
Proc Natl Acad Sci U S A. 1996 Nov 26;93(24):14076-81. doi: 10.1073/pnas.93.24.14076.
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CD4-induced interaction of primary HIV-1 gp120 glycoproteins with the chemokine receptor CCR-5.CD4诱导的原发性HIV-1 gp120糖蛋白与趋化因子受体CCR-5的相互作用。
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RANTES, MIP and interleukin-16 in HIV infection.
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Chemokine production in HIV-seropositive long-term asymptomatic individuals.HIV血清阳性长期无症状个体中的趋化因子产生
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The V3 domain of the HIV-1 gp120 envelope glycoprotein is critical for chemokine-mediated blockade of infection.HIV-1 gp120包膜糖蛋白的V3结构域对于趋化因子介导的感染阻断至关重要。
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Chemokines in immune-mediated inflammation of the central nervous system.趋化因子在中枢神经系统免疫介导性炎症中的作用
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β趋化因子在HIV感染中具有临床相关性吗?

Do beta-chemokines have clinical relevance in HIV infection?

作者信息

Mackewicz C E, Barker E, Greco G, Reyes-Teran G, Levy J A

机构信息

Department of Medicine and Cancer Research Institute, University of California, School of Medicine, San Francisco, California 94143-1270, USA.

出版信息

J Clin Invest. 1997 Aug 15;100(4):921-30. doi: 10.1172/JCI119608.

DOI:10.1172/JCI119608
PMID:9259592
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC508265/
Abstract

The role of beta-chemokines in HIV infection was evaluated. The kinetics of regulated upon activation of normal T cell expressed and secreted, macrophage inflammatory protein-1alpha, and macrophage inflammatory protein 1beta production by stimulated T lymphocytes did not differ substantially between HIV-infected (asymptomatic and with AIDS) and uninfected subjects. Maximal production of these beta-chemokines by activated peripheral blood cells was higher in the infected individuals than in uninfected individuals, but no significant difference was observed between healthy infected subjects and AIDS patients. Evaluation of the effect of HIV replication on beta-chemokine production indicated that acute infection of CD4+ T cells with non-syncytia-inducing (NSI) viruses generally increased beta-chemokine production two to eightfold, whereas with SI strains, it led to decreased production. The sensitivity of an individual's virus to beta-chemokine-mediated inhibition correlated with the NSI virus phenotype and a healthy clinical state. 50% of the AIDS patients, however, had NSI viruses that were sensitive to beta-chemokines. Finally, anti-beta-chemokine-neutralizing antibodies caused a more rapid release of HIV by CD4+ T cells naturally infected by NSI, but not SI, viruses indicating that endogenously produced chemokines can affect HIV production in culture. These findings suggest that beta-chemokines may affect HIV replication when an NSI virus is involved, but provide little evidence that they substantially influence HIV infection and pathogenesis.

摘要

评估了β趋化因子在HIV感染中的作用。受刺激的T淋巴细胞产生正常T细胞表达和分泌的、巨噬细胞炎性蛋白-1α和巨噬细胞炎性蛋白1β的动力学,在HIV感染(无症状和患艾滋病)和未感染的受试者之间没有显著差异。被激活的外周血细胞产生这些β趋化因子的最大值,在感染个体中高于未感染个体,但在健康感染受试者和艾滋病患者之间未观察到显著差异。对HIV复制对β趋化因子产生的影响的评估表明,用非合胞体诱导(NSI)病毒急性感染CD4+T细胞通常会使β趋化因子的产生增加2至8倍,而用合胞体诱导(SI)毒株感染则导致产生减少。个体病毒对β趋化因子介导的抑制的敏感性与NSI病毒表型和健康临床状态相关。然而,50%的艾滋病患者的NSI病毒对β趋化因子敏感。最后,抗β趋化因子中和抗体导致被NSI而非SI病毒自然感染的CD4+T细胞更快地释放HIV,这表明内源性产生的趋化因子可影响培养中的HIV产生。这些发现表明,当涉及NSI病毒时,β趋化因子可能影响HIV复制,但几乎没有证据表明它们会对HIV感染和发病机制产生实质性影响。