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针对K562细胞系的单克隆抗体可加速大颗粒淋巴细胞对靶细胞的杀伤作用。

Monoclonal antibody against K562 cell line accelerates killing of the target cells by large granular lymphocytes.

作者信息

Park M M, Brahmi Z

出版信息

Cell Immunol. 1984 Mar;84(1):94-103. doi: 10.1016/0008-8749(84)90080-7.

Abstract

A monoclonal antibody (MoAb 11-4) was raised against K562, a human erythroleukemia cell line sensitive to natural killer cell-mediated cytotoxicity (NK-CMC). Immunological analysis revealed MoAb to be IgG2b. Alone, the MoAb was not cytotoxic for K562 and did not bind to the effector cells, but the addition of this antibody to macrophage-depleted human peripheral blood lymphocytes increased killing of K562 in a 4-hr NK-CMC assay. The maximum increase in NK-CMC was observed when MoAb 11-4 was added to target cells prior to the formation of effector/target cell conjugates. This effect was dose dependent, was specific for K562, and, contrary to conventional antisera, occurred at very low concentrations of MoAb. When MoAb was added either to Percoll-purified large granular lymphocytes (LGL) or to LGL-depleted lymphocytes, only the latter demonstrated a significant increase in the killing of K562 in a 4-hr chromium release assay. Kinetics studies revealed that although the overall LGL-mediated lysis was only slightly increased at 4 hr, the maximum lytic activity was reached within 2 hr. These studies suggest that (1) human LGL and LGL-depleted cell populations bear Fc receptors for mouse IgG2b and (2) although the cytotoxic activities of both cell populations are increased by treatment with MoAb 11-4, the kinetics of this increase are different.

摘要

制备了一种针对K562的单克隆抗体(MoAb 11 - 4),K562是一种对自然杀伤细胞介导的细胞毒性(NK - CMC)敏感的人红白血病细胞系。免疫分析显示该单克隆抗体为IgG2b。单独使用时,该单克隆抗体对K562无细胞毒性,也不与效应细胞结合,但在4小时的NK - CMC试验中,将这种抗体添加到去除巨噬细胞的人外周血淋巴细胞中可增强对K562的杀伤作用。当在效应细胞/靶细胞结合物形成之前将MoAb 11 - 4添加到靶细胞中时,观察到NK - CMC的最大增加。这种效应具有剂量依赖性,对K562具有特异性,并且与传统抗血清相反,在非常低的单克隆抗体浓度下就会出现。当将单克隆抗体添加到经Percoll纯化的大颗粒淋巴细胞(LGL)或去除LGL的淋巴细胞中时,只有后者在4小时的铬释放试验中显示出对K562杀伤作用的显著增加。动力学研究表明,虽然在4小时时LGL介导的总体裂解仅略有增加,但最大裂解活性在2小时内达到。这些研究表明:(1)人LGL和去除LGL的细胞群体带有小鼠IgG2b的Fc受体;(2)虽然用MoAb 11 - 4处理后这两种细胞群体的细胞毒性活性均增加,但这种增加的动力学不同。

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