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库尔洛夫细胞的自然杀伤和凝集素依赖性细胞毒性活性:靶细胞选择性、共轭形成和钙离子依赖性。

Natural killer and lectin-dependent cytotoxic activities of Kurloff cells: target cell selectivity, conjugate formation, and Ca++ dependency.

作者信息

Pouliot N, Maghni K, Blanchette F, Cironi L, Sirois P, Stankova J, Rola-Pleszczynski M

机构信息

Department of Pediatrics, Faculty of Medicine, Université de Sherbrooke, QC, Canada.

出版信息

Inflammation. 1996 Dec;20(6):647-71. doi: 10.1007/BF01488802.

Abstract

Kurloff cells may represent a major component of NK cell activity in the guinea pig. We have pursued to characterize the mechanism of their action. Using murine target cells, we found Kurloff cell cytotoxicity to be selective for the NK-sensitive YAC-1 target cell, with minimal activity against the NK-resistant P815 target cell. In the presence of PHA, but not ConA, cytotoxicity was markedly augmented against both YAC-1 and P815. While effector-target conjugate formation was observed with YAC-1 cells but not P815 cells in control cultures, it was augmented with both target cell types in cultures with PHA. Pretreatment alone with PHA was ineffective, however. NK cell activity of Kurloff cells was dependent on extracellular Ca++ and entry of Ca++ into the effector cells, as demonstrated by abrogation of cytotoxicity when extracellular Ca++ was chelated with EDTA or EGTA, or following treatment with the Ca++ channel blockers verapamil and diltiazem. Furthermore, inhibition of PKC by H7 resulted in significant reduction of Kurloff cell-mediated NK activity, while pretreatment of effector cells with the PKC activator TPA enhanced NK activity. Kurloff cells could also be stimulated to produce serine esterases by contact with target cells or treatment with phorbol ester and ionophore. Finally, a majority of Kurloff cells, identified by the monoclonal antibody 14D1, reacted with the human NK cell marker CD56. Taken together, these data suggest that Kurloff cells have NK-like characteristics and activity, with target cell selectivity, and that their lytic mechanisms involve influx of extracellular Ca++, PKC activation and serine esterase production.

摘要

库尔洛夫细胞可能是豚鼠自然杀伤(NK)细胞活性的主要组成部分。我们一直在努力阐明其作用机制。使用鼠类靶细胞,我们发现库尔洛夫细胞的细胞毒性对NK敏感的YAC-1靶细胞具有选择性,而对NK抗性的P815靶细胞的活性最小。在有PHA但没有ConA的情况下,对YAC-1和P815的细胞毒性均显著增强。在对照培养物中,观察到YAC-1细胞能形成效应细胞-靶细胞共轭物,而P815细胞则不能,但在含有PHA的培养物中,两种靶细胞类型都能增强共轭物的形成。然而,单独用PHA预处理是无效的。库尔洛夫细胞的NK细胞活性依赖于细胞外Ca++以及Ca++进入效应细胞,当用EDTA或EGTA螯合细胞外Ca++时,或在用Ca++通道阻滞剂维拉帕米和地尔硫卓处理后,细胞毒性被消除就证明了这一点。此外,H7对蛋白激酶C(PKC)的抑制导致库尔洛夫细胞介导的NK活性显著降低,而用PKC激活剂佛波酯(TPA)预处理效应细胞则增强了NK活性。库尔洛夫细胞也可以通过与靶细胞接触或用佛波酯和离子载体处理来刺激产生丝氨酸酯酶。最后,通过单克隆抗体14D1鉴定的大多数库尔洛夫细胞与人NK细胞标志物CD56发生反应。综上所述,这些数据表明库尔洛夫细胞具有类似NK细胞的特征和活性,具有靶细胞选择性,并且它们的裂解机制涉及细胞外Ca++内流、PKC激活和丝氨酸酯酶产生。

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