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白细胞介素3依赖的自然细胞毒性细胞的形态学与溶解机制:肿瘤坏死因子作为一种可能的介质

Morphology and lytic mechanisms of interleukin 3-dependent natural cytotoxic cells: tumor necrosis factor as a possible mediator.

作者信息

Jadus M R, Schmunk G, Djeu J Y, Parkman R

出版信息

J Immunol. 1986 Nov 1;137(9):2774-83.

PMID:2428873
Abstract

Populations of interleukin 3 (IL 3)-dependent cells can be derived from mouse bone marrow that display natural cytotoxicity (NC) against Wehi-164 target cells but do not display natural killing against YAC-1 cells. These bone marrow-derived NC cells cultured up to 2 mo in IL 3 do not contain rearranged T cell receptor beta-chain genes. They appear to be mast-like cells by electron microscopy and contain heterogeneous type granules. The molecules that mediate NC appear to be contained in these granules and are preformed because protein synthesis inhibitors have no effect on the capacity of IL 3-dependent NC cells to lyse Wehi-164 target cells. In addition to the IL 3-dependent bone marrow-derived cells, the basophilic leukemia cells, RBL-1, but not P815 mastocytoma cells were found to mediate NC against Wehi-164 cells. Both bone marrow-derived NC and RBL-1 cells can lyse L929 cells in 18 hr, suggesting that the putative NC mediator may be related to lymphotoxin/tumor necrosis factor (TNF). Recombinant human TNF displayed identical properties as NC cells; both entities possessed the same target cell specificity and had similar kinetics of target cell killing. The use of polyclonal rabbit antimouse TNF antibody blocked the actions of NC cells. Thus we believe that the mediation of NC is through the actions of a TNF-like molecule.

摘要

白细胞介素3(IL-3)依赖细胞群体可从小鼠骨髓中获得,这些细胞对Wehi-164靶细胞具有天然细胞毒性(NC),但对YAC-1细胞无天然杀伤作用。这些在IL-3中培养长达2个月的骨髓来源的NC细胞不包含重排的T细胞受体β链基因。通过电子显微镜观察,它们似乎是类肥大细胞,并含有异质性颗粒。介导NC的分子似乎包含在这些颗粒中,并且是预先形成的,因为蛋白质合成抑制剂对IL-3依赖的NC细胞裂解Wehi-164靶细胞的能力没有影响。除了IL-3依赖的骨髓来源细胞外,还发现嗜碱性白血病细胞RBL-1,但不是P815肥大细胞瘤细胞,可介导对Wehi-164细胞的NC作用。骨髓来源的NC细胞和RBL-1细胞均可在18小时内裂解L929细胞,这表明假定的NC介质可能与淋巴毒素/肿瘤坏死因子(TNF)有关。重组人TNF表现出与NC细胞相同的特性;两者都具有相同的靶细胞特异性,并且具有相似的靶细胞杀伤动力学。使用多克隆兔抗小鼠TNF抗体可阻断NC细胞的作用。因此,我们认为NC的介导是通过一种TNF样分子的作用。

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