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溶酶体相关的p61Hck亚型的激活触发了足体的生物发生。

Activation of the lysosome-associated p61Hck isoform triggers the biogenesis of podosomes.

作者信息

Cougoule Céline, Carréno Sébastien, Castandet Jerôme, Labrousse Arnaud, Astarie-Dequeker Catherine, Poincloux Renaud, Le Cabec Véronique, Maridonneau-Parini Isabelle

机构信息

Institut de Pharmacologie et de Biologie Structurale - Centre National de la Recherche Scientifique UMR 5089, Département Mécanismes Moléculaires des Infections Mycobactériennes, 205 route de Narbonne, 31077 Toulouse cedex, France.

出版信息

Traffic. 2005 Aug;6(8):682-94. doi: 10.1111/j.1600-0854.2005.00307.x.

DOI:10.1111/j.1600-0854.2005.00307.x
PMID:15998323
Abstract

Haematopoietic cell kinase (Hck) is a protein tyrosine kinase of the Src family specifically expressed in phagocytes as two isoforms, p59Hck and p61Hck, present at the plasma membrane and lysosomes, respectively. We report that ectopic expression of a constitutively active mutant of p61Hck (p61Hck(ca)) triggered the de novo formation of actin-rich rings at the ventral face of the cells that we characterized as bona fide podosome rosettes, structures involved in cell migration. Their formation required the adaptor domains and the kinase activity of p61Hck, the integrity of microfilament and microtubule networks and concerted action of Cdc42, Rac and Rho. Podosome rosette formation was either abolished when p61Hck(ca) was readdressed from lysosomes to the cytosol or triggered when p59Hck(ca) was relocalized to lysosomes. Lysosomal markers were present at podosome rosettes. By stimulating exocytosis of p61Hck(ca) lysosomes with a calcium ionophore, the formation of podosome rosettes was enhanced. Interestingly, we confirm that, in human macrophages, Hck and lysosomal markers were present at podosomes which were spatially reorganized as clusters, a foregoing step to form rosettes, upon expression of p61Hck(ca). We propose that lysosomes, under the control of p61Hck, are involved in the biogenesis of podosomes, a key phenomenon in the migration of phagocytes.

摘要

造血细胞激酶(Hck)是Src家族的一种蛋白酪氨酸激酶,在吞噬细胞中特异性表达为两种异构体,即p59Hck和p61Hck,分别存在于质膜和溶酶体中。我们报告称,p61Hck的组成型活性突变体(p61Hck(ca))的异位表达触发了细胞腹侧富含肌动蛋白环的从头形成,我们将其鉴定为真正的足体玫瑰花结,这是一种参与细胞迁移的结构。它们的形成需要p61Hck的衔接结构域和激酶活性、微丝和微管网络的完整性以及Cdc42、Rac和Rho的协同作用。当p61Hck(ca)从溶酶体重新定位到细胞质时,足体玫瑰花结的形成被消除,而当p59Hck(ca)重新定位到溶酶体时则被触发。溶酶体标记物存在于足体玫瑰花结中。通过用钙离子载体刺激p61Hck(ca)溶酶体的胞吐作用,足体玫瑰花结的形成得到增强。有趣的是,我们证实,在人类巨噬细胞中,Hck和溶酶体标记物存在于足体中,在p61Hck(ca)表达后,足体会在空间上重新组织成簇,这是形成玫瑰花结的前一步。我们提出,在p61Hck的控制下,溶酶体参与了足体的生物发生,这是吞噬细胞迁移中的一个关键现象。

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