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Identification with a monoclonal antibody of a predominantly B lymphocyte-specific determinant of the human leukocyte common antigen. Evidence for structural and possible functional diversity of the human leukocyte common molecule

机译:用单克隆抗体鉴定人白细胞共同抗原的主要是B淋巴细胞特异性决定簇。人类白细胞共同分子的结构和可能的功能多样性的证据

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摘要

Initial studies with the monoclonal antibody F8-11-13 described in this paper showed that it reacted strongly with B lymphocytes, did not react at all with granulocytes, and reacted only weakly with a small subpopulation of thymocytes and peripheral T lymphocytes. This picture was entirely different from that seen with monoclonal antibodies to the leukocyte common (LC) antigen, where 100% of all the above-mentioned leukocyte populations were positive. Biochemical studies using detergent solubilized membranes labeled with 3H at the sialic acid residues showed that the molecule bearing the F8-11-13 determinant was a glycoprotein of 215,000 mol wt, and that the peak depleted by F8-11- 13 monoclonal antibody affinity columns corresponded to the high molecular weight region of a broad peak previously shown to be completely depleted by monoclonal antibody (F10-89-4) affinity columns directed at the LC antigen. Proof that the F8-11-13 determinant was expressed on some LC molecules was established by cross-inhibition studies with affinity-column-purified and depleted material. This finding of a serologically identifiable conformational or other structural change selectively expressed on the LC molecule of a functionally discrete population of lymphocytes has interesting implications for the structure and function of the LC molecule, and might be relevant to functional consideration of other membrane molecules.
机译:本文描述的单克隆抗体F8-11-13的初步研究表明,它与B淋巴细胞强烈反应,与粒细胞完全不反应,仅与少量的胸腺细胞和外周T淋巴细胞亚群反应。这张图片与白细胞常见(LC)抗原的单克隆抗体所看到的完全不同,在该抗体中,所有上述白细胞群体均为100%呈阳性。使用唾液酸残基标记有3H的去污剂溶解膜的生化研究表明,带有F8-11-13决定簇的分子是215,000 mol wt的糖蛋白,并且被F8-11- 13单克隆抗体亲和柱消耗的峰对应之前显示被针对LC抗原的单克隆抗体(F10-89-4)亲和柱完全耗尽了宽峰的高分子量区域。 F8-11-13决定簇在某些LC分子上表达的证据是通过与亲和柱纯化和消耗的物质进行交叉抑制研究确定的。在功能上离散的淋巴细胞群的LC分子上选择性表达的血清学上可识别的构象或其他结构变化的发现,对LC分子的结构和功能具有有趣的意义,并且可能与其他膜分子的功能考虑有关。

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