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携带人Fc受体的淋巴细胞与抗原-抗体复合物的黏附。II. 底物诱导的形态学改变。

The adherence of human Fc receptor-bearing lymphocytes to antigen-antibody complexes. II. Morphologic alterations induced by the substrate.

作者信息

Alexander E, Henkart P

出版信息

J Exp Med. 1976 Feb 1;143(2):329-47. doi: 10.1084/jem.143.2.329.

DOI:10.1084/jem.143.2.329
PMID:814196
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2190128/
Abstract

The adhesion of human Fc receptor-bearing lymphocytes to immobilized antigen-antibody complexes is accompanied by marked alterations in cell shape, resulting in flattening of greater than 90% of the adherent cells. In addition, about 65% of the adherent cells become elongated, with distinct uropods being present in about 1/3 of these cells. Scanning electron microscopy demonstrates that most of the surface microvilli are lost, while ruffled membranes and long microextensions are formed during the shape change. Time-lapse cinematography shows that the major shape changes occur within a few minutes after contact with the substrate, and that the adherent cells undergo translational motility. Both flattening and elongation of the adherent cells are inhibited by low temperature, chelating agents, cytochalasin B, and vinblastine, while sodium azide selectively inhibits elongation and uropod formation. It is argued that these morphological changes result from an active response of the cell to the immobilized complexes, and that such alterations may be related mechanistically to the ability of the cells to kill antibody-coated target cells.

摘要

携带人Fc受体的淋巴细胞与固定化抗原-抗体复合物的黏附伴随着细胞形态的显著改变,导致超过90%的黏附细胞变扁平。此外,约65%的黏附细胞会伸长,其中约1/3的细胞会出现明显的尾足。扫描电子显微镜显示,大多数表面微绒毛消失,而在形态变化过程中会形成褶皱膜和长微延伸。延时摄影显示,主要的形态变化发生在与底物接触后的几分钟内,并且黏附细胞会进行平移运动。黏附细胞的变扁平及伸长均受到低温、螯合剂、细胞松弛素B和长春碱的抑制,而叠氮化钠选择性地抑制伸长和尾足形成。有人认为,这些形态变化是细胞对固定化复合物的主动反应所致,并且这种改变在机制上可能与细胞杀伤抗体包被靶细胞的能力有关。

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The adherence of human Fc receptor-bearing lymphocytes to antigen-antibody complexes. II. Morphologic alterations induced by the substrate.携带人Fc受体的淋巴细胞与抗原-抗体复合物的黏附。II. 底物诱导的形态学改变。
J Exp Med. 1976 Feb 1;143(2):329-47. doi: 10.1084/jem.143.2.329.
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