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通过酶组织化学、单克隆抗体和流式细胞术分析豚鼠T淋巴细胞发育。

Guinea pig T lymphocyte development analyzed by enzyme histocytochemistry, monoclonal antibodies, and flow cytometry.

作者信息

Elias J M, Chiba J, Shevach E M, Godfrey H P

出版信息

Lab Invest. 1985 Mar;52(3):270-7.

PMID:2579290
Abstract

Studies of T (thymus-derived) lymphocyte ontogeny in the guinea pig have been hampered by the lack of suitable antigenic or other markers for various T cell subpopulations in this species. Monoclonal antibodies that recognize three distinct surface proteins of guinea pig T cells and react with all peripheral T cells have been used in combination with membrane alkaline phosphatase (AP) to characterize stages of guinea pig T cell development and to determine anatomical localization of different T cell subpopulations. Flow cytofluorographic analysis of thymus, spleen, and lymph node lymphocytes was used to characterize monoclonal antibody specificity. Cortical thymocytes in tissue sections expressed membrane AP activity and contained nuclear terminal deoxynucleotidyl transferase; medullary thymocytes reacted strongly with one of the monoclonal antibodies (8BE6), minimally with a second (5CD2), and not at all with a third (11AE3). In contrast, polyclonal rabbit antiguinea pig T cell antiserum reacted with both cortical and medullary thymocytes. Staining of tissue sections of lymph node and spleen revealed AP+ lymphocytes to be present peripheral to the mantle region of lymph node follicles and to be randomly scattered throughout the splenic red pulp. T cells reactive with monoclonal antibodies were located primarily in paracortical regions of lymph node and the central region around the periarteriolar regions of the spleen. Dual staining of frozen sections and cell suspension of guinea pig lymphoid tissues for AP activity and surface proteins unique to T cells showed that AP+ cells lacked T cell markers. Dual staining for AP activity and surface immunoglobulins or esterase activity showed that AP+ cells are not likely to be derived from either B cell or monocyte-macrophage lineages. AP+ cells in guinea pig secondary lymphoid tissue may represent a unique subset of lymphocytes of unknown function.

摘要

豚鼠中T(胸腺衍生)淋巴细胞个体发生的研究因缺乏该物种各种T细胞亚群合适的抗原或其他标志物而受阻。识别豚鼠T细胞三种不同表面蛋白并与所有外周T细胞发生反应的单克隆抗体已与膜碱性磷酸酶(AP)结合使用,以表征豚鼠T细胞发育阶段并确定不同T细胞亚群的解剖定位。利用胸腺、脾脏和淋巴结淋巴细胞的流式细胞荧光分析来表征单克隆抗体的特异性。组织切片中的皮质胸腺细胞表达膜AP活性并含有核末端脱氧核苷酸转移酶;髓质胸腺细胞与一种单克隆抗体(8BE6)强烈反应,与第二种单克隆抗体(5CD2)反应较弱,与第三种单克隆抗体(11AE3)完全不反应。相比之下,多克隆兔抗豚鼠T细胞抗血清与皮质和髓质胸腺细胞均发生反应。淋巴结和脾脏组织切片的染色显示,AP+淋巴细胞存在于淋巴结滤泡套区外周,且随机散布于脾红髓中。与单克隆抗体反应的T细胞主要位于淋巴结的副皮质区和脾脏动脉周围区域的中央区域。对豚鼠淋巴组织的冰冻切片和细胞悬液进行AP活性和T细胞特有的表面蛋白的双重染色显示,AP+细胞缺乏T细胞标志物。对AP活性与表面免疫球蛋白或酯酶活性进行双重染色显示,AP+细胞不太可能来源于B细胞或单核细胞-巨噬细胞谱系。豚鼠二级淋巴组织中的AP+细胞可能代表功能未知的独特淋巴细胞亚群。

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