金标记槲寄生凝集素I及其亚基和免疫毒素在小鼠l1210白血病细胞内化的比较研究。

Acta histochemica. Supplementband Pub Date : 1991-01-01
L Jonas, H Walzel
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引用次数: 0

摘要

采用预包埋电镜技术,研究了金标记槲寄生凝集素I (ML I)及其A (ML I-A)和B (ML I-B)亚基,以及由抗l1210单克隆抗体和l1210细胞毒A链组成的免疫毒素在小鼠l1210白血病细胞上的结合和内化。我们发现受体介导的内吞作用在整个凝集素、其亚基和免疫毒素之间有显著差异。而ML I,其A链以及免疫毒素通过包被的凹坑/包被的囊泡或与未包被的膜结合被内化,B链则通过未包被的细胞膜深内陷被完全内吞。考虑到与细胞骨架运动相关的配体-受体复合物的结合和内化动力学,讨论了通过网格蛋白包被或未包被的囊泡的内吞作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Comparative studies on internalization of gold-labelled mistletoe lectin I, its subunits, as well as of an immunotoxin in murine L 1210 leukemia cells.

The binding and internalization of gold-labelled mistletoe lectin I (ML I), its A (ML I-A) and B (ML I-B) subunits, as well as of an immunotoxin consisting of an monoclonal anti L 1210 antibody and the cytotoxic A chains of ML I, were studied on murine L 1210 leukemia cells by a preembedding electron microscopic technique. We found that receptor-mediated endocytosis differs remarkably between the whole lectin, its subunits, and the immunotoxin. Whereas ML I, its A chain, as well as the immunotoxin are internalized by coated pits/coated vesicles or in combination with uncoated membranes, the B chain is exclusively endocytosed via uncoated deep invaginations of the cell membrane. The endocytosis via clathrin-coated or uncoated vesicles is discussed taking into account the binding and internalization kinetics of ligand-receptor complexes related with the movement by the cytoskeleton.

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