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人和小鼠自然杀伤系统中的靶效应器相互作用:可溶性自然杀伤靶结构复合物的特异性和异种反应性及其在体细胞杂种中的丧失

Target-effector interaction in the human and murine natural killer system: specificity and xenogeneic reactivity of the solubilized natural killer-target structure complex and its loss in a somatic cell hybrid.

作者信息

Roder J C, Ahrlund-Richter L, Jondal M

出版信息

J Exp Med. 1979 Sep 19;150(3):471-81. doi: 10.1084/jem.150.3.471.

Abstract

Preincubation of natural killer (NK) cells with electrophoresis purified proteins from a variety of NK-sensitive murine and human tumor cells specifically prevented subsequent binding to the intact, homologous target cell. The NK-target structures (NK-TS) consisted of some or all of four characteristic molecular species, tentatively assigned molecular weights of 140K, 160K, 190K, and 240K (+/-10K) based on electrophoretic mobility in sodium dodecyl sulfate-polyacrylamide gels. When these NK-TS molecules were compared in cross-inhibition assays, the large 240K molecule most often carried the unique NK specificity, whereas the smaller 140K molecules cross-reacted between YAC, 136-6 and X-63 in the mouse and between Molt-4 and K562 in the human. Mouse NK cells recognised a different spectrum of NK-TS molecules than human NK cells. The control of NK-TS expression was partially revealed in a cloned, somatic cell hybrid bwtween an NK sensitive (YAC-IR) and insensitive (A9HT) cell line. The hybrid did not express NK-TS and did not bind to NK cells which is in accordance with negative NK cytolytic results previously reported. Although unique specificities are carried by some of the multiple NK-TS protein molecules, cross-reactions were widespread. These observations taken together suggest that the NK cell is polyspecific and has some heterogeneity in the recognition structure although much less than would be expected of an antibody-combining site.

摘要

将自然杀伤(NK)细胞与来自多种对NK敏感的鼠类和人类肿瘤细胞经电泳纯化的蛋白质进行预孵育,可特异性地阻止随后与完整的同源靶细胞结合。NK-靶结构(NK-TS)由四种特征性分子种类中的部分或全部组成,根据其在十二烷基硫酸钠-聚丙烯酰胺凝胶中的电泳迁移率,初步确定其分子量分别为140K、160K、190K和240K(±10K)。在交叉抑制试验中比较这些NK-TS分子时,较大的240K分子最常携带独特的NK特异性,而较小的140K分子在小鼠的YAC、136-6和X-63之间以及人类的Molt-4和K562之间发生交叉反应。小鼠NK细胞识别的NK-TS分子谱与人类NK细胞不同。在一个由对NK敏感的(YAC-IR)和不敏感的(A9HT)细胞系构建的克隆体细胞杂交体中,部分揭示了NK-TS表达的调控情况。该杂交体不表达NK-TS,也不与NK细胞结合,这与先前报道的阴性NK细胞溶解结果一致。尽管多个NK-TS蛋白分子中的一些具有独特的特异性,但交叉反应广泛存在。综合这些观察结果表明,NK细胞具有多特异性,并且在识别结构上存在一些异质性,尽管比预期的抗体结合位点要少得多。

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