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PAK4和αPIX通过局部肌动蛋白调节来决定巨噬细胞中足体的大小和数量。

PAK4 and alphaPIX determine podosome size and number in macrophages through localized actin regulation.

作者信息

Gringel Alexandra, Walz Daniel, Rosenberger Georg, Minden Audrey, Kutsche Kerstin, Kopp Petra, Linder Stefan

机构信息

Institut für Prophylaxe und Epidemiologie der Kreislaufkrankheiten, Pettenkoferstr, München, Germany.

出版信息

J Cell Physiol. 2006 Nov;209(2):568-79. doi: 10.1002/jcp.20777.

DOI:10.1002/jcp.20777
PMID:16897755
Abstract

Podosomes are actin-rich adhesion structures typical for monocytic cells and are implicated in migration and invasion. Major modes of podosome regulation include RhoGTPase signaling and actin regulatory pathways. However, it is not clearly understood how these signals induce highly localized changes in podosome formation and dynamics. Here, we show that the RhoGTPase effector PAK4, a member of the p21 associated kinase family, and its regulator alphaPIX (PAK-interacting exchange factor), are central to podosome formation in primary human macrophages. Immunofluorescence, biochemical and microarray data indicate that PAK4 acts as physiological regulator of podosomes in this system. Accordingly, transfection of a specific shRNA, as well as expression of PAK4 truncation mutants, resulted in reduced numbers of podosomes per cell. Moreover, expression of kinase active or inactive PAK4 mutants enhanced or reduced the size of individual podosomes, respectively, indicating a modulatory influence of PAK4 kinase activity on podosome size. Similar to the results gained with PAK4, cellular/overexpressed PIX was shown to be closely associated with podosomes. Moreover, both overexpression of alphaPIX wt and a mutant lacking the SH3 domain led to coalescence of podosomes. In sum, we propose that PAK4 and alphaPIX can induce highly localized changes in actin dynamics and thereby regulate size and number of podosomes in primary human macrophages.

摘要

足体是富含肌动蛋白的粘附结构,是单核细胞的典型特征,与迁移和侵袭有关。足体调节的主要模式包括RhoGTPase信号传导和肌动蛋白调节途径。然而,目前尚不清楚这些信号如何诱导足体形成和动态变化中的高度局部化改变。在这里,我们表明RhoGTPase效应器PAK4(p21相关激酶家族的成员)及其调节因子alphaPIX(PAK相互作用交换因子)是原代人巨噬细胞中足体形成的核心。免疫荧光、生化和微阵列数据表明PAK4在该系统中作为足体的生理调节因子起作用。因此,转染特异性短发夹RNA以及PAK4截短突变体的表达导致每个细胞中足体数量减少。此外,激酶活性或无活性的PAK4突变体的表达分别增加或减少了单个足体的大小,表明PAK4激酶活性对足体大小有调节作用。与PAK4的结果相似,细胞内/过表达的PIX被证明与足体密切相关。此外,alphaPIX野生型和缺乏SH3结构域的突变体的过表达均导致足体融合。总之,我们提出PAK4和alphaPIX可以诱导肌动蛋白动力学的高度局部化变化,从而调节原代人巨噬细胞中足体的大小和数量。

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J Cell Physiol. 2006 Nov;209(2):568-79. doi: 10.1002/jcp.20777.
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