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自然杀伤细胞(NK细胞)溶解作用的阻断是单克隆抗体的一种特性,这些单克隆抗体可与T-200的不同区域结合。

Blockade of NK cell lysis is a property of monoclonal antibodies that bind to distinct regions of T-200.

作者信息

Newman W, Fast L D, Rose L M

出版信息

J Immunol. 1983 Oct;131(4):1742-7.

PMID:6194213
Abstract

The previously described NK inhibitory monoclonal antibody 13.1 is shown to immunoprecipitate a series of high m.w. glycoproteins homologous with the murine T-200/Ly-5 molecules. Not all antibodies to the human T-200 molecule, however, have an inhibitory effect on NK cell function. A comparison is made between two noninhibitory anti-T-200 antibodies, 13.5 and 13.6, and two inhibitory anti-T-200 antibodies, 13.1 and 13.3. All antibodies are of the IgG1 subclass. Sequential immunoprecipitation experiments show that these antibodies react with the same set of molecules. The differences in NK-blocking activity could not be explained by the amount of antibody bound per cell in NK-enriched populations, nor by the avidity with which they bound. It is shown by competitive radiobinding assays that the 13.1 and 13.3 antibodies define a region, termed region A, distinct from that defined by the nonblocking antibodies 13.5 and 13.6, termed region B. Region B is shown to reside between the membrane and region A. These findings show that the inhibition of NK lysis by anti-T-200 antibodies is a function of the site on that molecule to which these antibodies bind. This may also explain the ability of antibodies to the A region of T-200 to block selectively the lysis of myeloid and erythroid tumor targets, with no effect on the lysis of T lymphoma targets.

摘要

先前描述的NK抑制性单克隆抗体13.1可免疫沉淀一系列与小鼠T-200/Ly-5分子同源的高分子量糖蛋白。然而,并非所有针对人T-200分子的抗体都对NK细胞功能具有抑制作用。对两种非抑制性抗T-200抗体13.5和13.6,以及两种抑制性抗T-200抗体13.1和13.3进行了比较。所有抗体均为IgG1亚类。连续免疫沉淀实验表明,这些抗体与同一组分子发生反应。NK阻断活性的差异既不能用富含NK的群体中每个细胞结合的抗体量来解释,也不能用它们结合的亲和力来解释。竞争性放射结合分析表明,13.1和13.3抗体界定了一个区域,称为A区,与非阻断性抗体13.5和13.6所界定的区域(称为B区)不同。已表明B区位于膜与A区之间。这些发现表明,抗T-200抗体对NK裂解的抑制作用是这些抗体所结合的该分子上位点的一种功能。这也可能解释了针对T-200 A区的抗体能够选择性地阻断髓系和红系肿瘤靶标的裂解,而对T淋巴瘤靶标的裂解没有影响的能力。

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