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通过HIV-1感染谱在脑中上调Fas和Fas配体的表达。

Upregulated expression of Fas and Fas ligand in brain through the spectrum of HIV-1 infection.

作者信息

Elovaara I, Sabri F, Gray F, Alafuzoff I, Chiodi F

机构信息

Microbiology and Tumorbiology Center, Karolinska Institute, Stockholm, Sweden.

出版信息

Acta Neuropathol. 1999 Oct;98(4):355-62. doi: 10.1007/s004010051094.

Abstract

Apoptosis of neurons and glial cells has been shown to occur in the brain of patients with the acquired immune deficiency syndrome (AIDS) and was postulated as contributing to brain atrophy and white matter damage in these patients. Since apoptotic events may be induced by the Fas-Fas ligand (FasL) system, we analyzed the relevance of these molecules to cell depletion in eight brains from HIV-1-infected patients and nine HIV-1-negative controls all of whom were analyzed histopathologically. The presence of Fas and FasL in brain tissue was analyzed by PCR amplification using Fas- and FasL-specific oligonucleotide primers and immunohistochemistry. The visualization of DNA fragmentation was used to evaluate apoptosis. Fas transcripts were detected in brains from each of four AIDS patients, each of three asymptomatic HIV-1 carriers and each of two HIV-1-negative controls. In the brains from AIDS patients the level of Fas expression was higher than in asymptomatic carriers and uninfected controls. FasL transcripts were seen in three of seven HIV-1-infected brains, two AIDS cases and one asymptomatic HIV-1 carrier. The predominant Fas-expressing cells were reactive astrocytes seen in each of two AIDS patients and one pre-AIDS case, but not in HIV-1-negative controls. Occasional Fas-positive oligodendrocyte-like cells were also seen in AIDS and pre-AIDS cases. No significant expression of Fas and FasL was seen in neurons. Fas-positive reactive astrocytes were more frequent in foci of HIV-1 encephalitis (HIVE). In the same area reactive apoptotic astrocytes were seen in close vicinity to FasL-expressing CD3 T lymphocytes, suggesting that apoptosis of astrocytes is mediated by Fas-FasL. The Fas expression on glial cells in asymptomatic HIV-1 infection may indicate apoptosis already in the asymptomatic stage of HIV-1 disease. In AIDS brains expression of Fas and FasL may contribute to the loss of glial cells and indirectly to the loss of neurons.

摘要

神经元和胶质细胞凋亡已被证实在获得性免疫缺陷综合征(AIDS)患者的大脑中发生,并被认为是导致这些患者脑萎缩和白质损伤的原因。由于凋亡事件可能由Fas-Fas配体(FasL)系统诱导,我们分析了这些分子与8例HIV-1感染患者及9例HIV-1阴性对照者脑内细胞减少的相关性,所有这些患者均进行了组织病理学分析。使用Fas和FasL特异性寡核苷酸引物通过PCR扩增及免疫组织化学分析脑组织中Fas和FasL的存在情况。通过DNA片段化的可视化来评估凋亡。在4例AIDS患者、3例无症状HIV-1携带者及2例HIV-1阴性对照者的大脑中均检测到Fas转录本。AIDS患者大脑中的Fas表达水平高于无症状携带者和未感染对照者。在7例HIV-1感染的大脑中有3例、2例AIDS病例及1例无症状HIV-1携带者中可见FasL转录本。主要表达Fas的细胞是在2例AIDS患者及1例AIDS前期病例中均可见的反应性星形胶质细胞,但在HIV-1阴性对照者中未见。在AIDS和AIDS前期病例中也偶尔可见Fas阳性的少突胶质细胞样细胞。在神经元中未见Fas和FasL的显著表达。Fas阳性反应性星形胶质细胞在HIV-1脑炎(HIVE)病灶中更为常见。在同一区域,可见反应性凋亡星形胶质细胞紧邻表达FasL的CD3 T淋巴细胞,提示星形胶质细胞凋亡由Fas-FasL介导。无症状HIV-1感染时胶质细胞上的Fas表达可能表明在HIV-1疾病的无症状阶段就已发生凋亡。在AIDS患者大脑中,Fas和FasL的表达可能导致胶质细胞丢失,并间接导致神经元丢失。

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