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HIV-1 脑炎中 T 细胞的免疫细胞化学鉴定:对中枢神经系统疾病发病机制的意义

Immunocytochemical identification of T-cells in HIV-1 encephalitis: implications for pathogenesis of CNS disease.

作者信息

Weidenheim K M, Epshteyn I, Lyman W D

机构信息

Department of Pathology (Neuropathology), Albert Einstein College of Medicine, Bronx, New York.

出版信息

Mod Pathol. 1993 Mar;6(2):167-74.

PMID:8483886
Abstract

T-lymphocytes enter the brain in viral encephalitides. The monoclonal antibodies UCHL1 and Leu22 are widely used to identify these cells; however, both antibodies cross-react with peripheral blood monocytes, cells ontologically related to brain macrophages and microglia. This study examines the nature of UCHL1- and Leu22-positive cells in HIV-1 encephalitis, and investigates whether they carry the gp41 epitope of HIV-1. Formalin-fixed sections of brain from eight AIDS patients were double-stained using combinations of UCHL1 and Leu22 antibodies with the lectin Ricinus communis agglutinin (RCA), a lectin that binds to microglia, macrophages, and multinucleated giant cells (MNGC), or antibody to the gp41 transmembrane protein of HIV-1 and UCHL1. Some sections were also stained with the OPD4 antibody to helper/inducer T-cells. Small round cells were single-stained for UCHL1 and Leu22 in all cases. A few cells having morphologic characteristics of microglia, macrophages, and MNGC were observed using double stains employing UCHL1 or Leu22 and RCA, or UCHL1 or Leu22 and anti-gp41. Small round cells positive for both UCHL1 or Leu22 and gp41 could represent either macrophages or lymphocytes. The presence of small round cells positive only for UCHL1 or Leu22 in double-stained sections strongly suggests that T-cells are present in the brain in HIV encephalitis. Only a few of these cells were positive with OPD4 antibody for T-helper cells. Inability to demonstrate unequivocally HIV-1-infected T-cells suggests that microglia and macrophages, not T-cells, are the more important reservoirs of retrovirus in the brain.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在病毒性脑炎中,T淋巴细胞会进入大脑。单克隆抗体UCHL1和Leu22被广泛用于识别这些细胞;然而,这两种抗体都会与外周血单核细胞发生交叉反应,外周血单核细胞在本体上与脑巨噬细胞和小胶质细胞相关。本研究检测了HIV-1脑炎中UCHL1和Leu22阳性细胞的性质,并研究它们是否携带HIV-1的gp41表位。对8例艾滋病患者的脑福尔马林固定切片,使用UCHL1和Leu22抗体与凝集素蓖麻凝集素(RCA,一种与小胶质细胞、巨噬细胞和多核巨细胞(MNGC)结合的凝集素)的组合,或HIV-1的gp41跨膜蛋白抗体与UCHL1进行双重染色。一些切片还用辅助/诱导性T细胞的OPD4抗体染色。在所有病例中,小圆形细胞均被UCHL1和Leu22单染色。使用UCHL1或Leu22与RCA,或UCHL1或Leu22与抗gp41的双重染色观察到一些具有小胶质细胞、巨噬细胞和MNGC形态特征的细胞。UCHL1或Leu22以及gp41均呈阳性的小圆形细胞可能代表巨噬细胞或淋巴细胞。在双重染色切片中仅UCHL1或Leu22呈阳性的小圆形细胞的存在强烈表明在HIV脑炎患者的大脑中存在T细胞。这些细胞中只有少数对T辅助细胞的OPD4抗体呈阳性。无法明确证明HIV-1感染的T细胞表明,在大脑中,小胶质细胞和巨噬细胞而非T细胞是逆转录病毒更重要的储存库。(摘要截短于250字)

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