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用人白细胞共同抗原的一种主要为B淋巴细胞特异性决定簇的单克隆抗体进行鉴定。人白细胞共同分子结构和可能功能多样性的证据。

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.

作者信息

Dalchau R, Fabre J W

出版信息

J Exp Med. 1981 Apr 1;153(4):753-65. doi: 10.1084/jem.153.4.753.

Abstract

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.

摘要

本文所述的针对单克隆抗体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,仅与一小部分胸腺细胞和外周T淋巴细胞微弱反应。这一情况与针对白细胞共同(LC)抗原的单克隆抗体所见的情况完全不同,在后者中,上述所有白细胞群体100%呈阳性。利用用3H标记唾液酸残基的去污剂溶解膜进行的生化研究表明,带有F8-11-13决定簇的分子是一种分子量为215,000的糖蛋白,并且F8-11-13单克隆抗体亲和柱耗尽的峰对应于先前已显示被针对LC抗原的单克隆抗体(F10-89-4)亲和柱完全耗尽的宽峰的高分子量区域。通过用亲和柱纯化和耗尽的材料进行交叉抑制研究,证实了F8-11-13决定簇在一些LC分子上表达。在功能上离散的淋巴细胞群体的LC分子上选择性表达血清学可识别的构象或其他结构变化这一发现,对于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相关。

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