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Rho是人类单核细胞铺展的负调节因子。

Rho is a negative regulator of human monocyte spreading.

作者信息

Aepfelbacher M, Essler M, Huber E, Czech A, Weber P C

机构信息

Institute for Prevention of Cardiovascular Diseases, University of Munich, Germany.

出版信息

J Immunol. 1996 Dec 1;157(11):5070-5.

PMID:8943416
Abstract

Monocyte spreading is a sequential series of events including cell flattening, formation of new actin structures and focal adhesions, as well as development of cytoplasmic projections. To investigate the involvement of the GTP-binding protein Rho in spreading, we treated human blood monocytes or PMA-stimulated U937 or THP1 cells with Clostridium botulinum C3-transferase (C3), which ADP-ribosylates and inactivates Rho in intact cells. The C3 treatment caused 1) a four- to fivefold increase in the number of THP1 cells that spread on fibronectin within 24 h of PMA stimulation, 2) a greater area covered by the spread cells, and 3) accelerated and enhanced development of macrophage-like filopodial and pseudopodial projections. Similar results were obtained with PMA-stimulated U937 cells and human blood monocytes. Furthermore, cell staining revealed disorganization of subcortical actin in C3-treated THP1 cells, whereas circular actin formations at the substrate-attached part of the cells and vinculin-containing focal complexes/adhesions were unaffected. Finally, we found a decrease in membrane-associated RhoA in normal spreading THP1 cells, which suggests endogenous inactivation of Rho and might provide an explanation for the acceleration of spreading caused by the C3-transferase. In conclusion, these results indicate that active Rho is an important, negative regulator of human monocyte spreading by maintaining cell tension and cortical actin organization.

摘要

单核细胞铺展是一系列连续的事件,包括细胞扁平化、新肌动蛋白结构和粘着斑的形成以及细胞质突起的发育。为了研究GTP结合蛋白Rho在铺展过程中的作用,我们用肉毒杆菌C3转移酶(C3)处理人血单核细胞或经佛波酯(PMA)刺激的U937或THP-1细胞,C3可使完整细胞中的Rho ADP核糖基化并使其失活。C3处理导致:1)在PMA刺激后24小时内,在纤连蛋白上铺展的THP-1细胞数量增加了4至5倍;2)铺展细胞覆盖的面积更大;3)加速并增强了巨噬细胞样丝状伪足和片状伪足突起的发育。用PMA刺激的U937细胞和人血单核细胞也得到了类似的结果。此外,细胞染色显示C3处理的THP-1细胞皮层肌动蛋白紊乱,而细胞与底物附着部分的圆形肌动蛋白结构以及含纽蛋白的粘着斑复合物/粘着斑未受影响。最后,我们发现正常铺展的THP-1细胞中膜相关RhoA减少,这表明Rho的内源性失活,可能解释了C3转移酶导致的铺展加速现象。总之,这些结果表明,活性Rho通过维持细胞张力和皮层肌动蛋白组织,是人类单核细胞铺展的重要负调节因子。

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1
Rho is a negative regulator of human monocyte spreading.Rho是人类单核细胞铺展的负调节因子。
J Immunol. 1996 Dec 1;157(11):5070-5.
2
Rho regulates association of both the ERM family and vinculin with the plasma membrane in MDCK cells.Rho调节MDCK细胞中ERM家族和纽蛋白与质膜的结合。
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ADP-ribosylation of Rho-proteins with botulinum C3 exoenzyme inhibits invasion and shape changes of T-lymphoma cells.肉毒杆菌C3外毒素对Rho蛋白的ADP核糖基化作用可抑制T淋巴瘤细胞的侵袭和形态变化。
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Translocation of activated Rho from the cytoplasm to membrane ruffling area, cell-cell adhesion sites and cleavage furrows.活化的Rho从细胞质转位至膜皱褶区域、细胞间黏附位点和分裂沟。
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Regulation of TNF-alpha-induced reorganization of the actin cytoskeleton and cell-cell junctions by Rho, Rac, and Cdc42 in human endothelial cells.Rho、Rac和Cdc42对人内皮细胞中肿瘤坏死因子-α诱导的肌动蛋白细胞骨架重组和细胞间连接的调节作用
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Studies on the function of rho A protein in cardiac myofibrillogenesis.Rho A蛋白在心肌纤维生成中的功能研究。
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Invasion of T-lymphoma cells: cooperation between Rho family GTPases and lysophospholipid receptor signaling.T淋巴瘤细胞的侵袭:Rho家族GTP酶与溶血磷脂受体信号传导之间的协同作用
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