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Dissection of distinct human immunoregulatory T-cell subsets by a monoclonal antibody recognizing a cell surface antigen with wide tissue distribution.

机译:通过识别具有广泛组织分布的细胞表面抗原的单克隆抗体解剖不同的人体免疫调节性T细胞亚群。

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摘要

A monoclonal antibody, PVR-11, was obtained after hybridization of X63Ag8.653 murine myeloma cells with spleen cells from a mouse immunized with human lymphocytes. It recognizes a 175,000- to 185,000-dalton surface antigen present on approximately 80% of normal human peripheral T lymphocytes, 50% of non-T non-B cells, and less than 10% of B cells as determined by complement-dependent microcytotoxicity. It is also present on various leukemia T cells, on some but not all T lymphoblastoid cell lines, and on a small fraction of some B lymphoblastoid cell lines. Some B-cell chronic lymphocytic leukemia cells also express the PVR-11 antigen. Functional analysis of normal human T lymphocytes demonstrated that the PVR-11-depleted T-cell subset contains the precursors of both cytotoxic and suppressor cells but lacks helper cells. On the other hand, cytotoxic effector T cells express the PVR-11 antigen. These results demonstrate that antigenic determinants with relatively wide tissue distribution can dissect functionally distinct human immunoregulatory T-cell subsets.
机译:X63Ag8.653鼠骨髓瘤细胞与来自用人淋巴细胞免疫的小鼠的脾细胞杂交后,获得了单克隆抗体PVR-11。通过补体依赖性微细胞毒性测定,它可识别约80%的正常人外周血T淋巴细胞,50%的非T非B细胞和少于10%的B细胞上存在的175,000至185,000道尔顿表面抗原。它也存在于各种白血病T细胞,一些但不是全部T淋巴母细胞系中以及一小部分B淋巴母细胞系中。一些B细胞慢性淋巴细胞性白血病细胞也表达PVR-11抗原。正常人T淋巴细胞的功能分析表明,耗尽PVR-11-的T细胞亚群包含细胞毒性和抑制细胞的前体,但缺少辅助细胞。另一方面,细胞毒性效应T细胞表达PVR-11抗原。这些结果证明具有相对宽的组织分布的抗原决定簇可以解剖功能上不同的人类免疫调节T细胞亚群。

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