Pablo A Mendoza, Patricio Silva, Jorge Díaz, Cecilia Arriagada, Jimena Canales, Oscar Cerda, Vicente A Torres
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引用次数: 8
Abstract
The early endosome protein Rab5 was recently shown to promote cell migration by enhancing focal adhesion disassembly through mechanisms that remain elusive. Focal adhesion disassembly is associated to proteolysis of talin, in a process that requires calpain2. Since calpain2 has been found at vesicles and endosomal compartments, we hypothesized that Rab5 stimulates calpain2 activity, leading to enhanced focal adhesion disassembly in migrating cells. We observed that calpain2 co-localizes with EEA1-positive early endosomes and co-immunoprecipitates with EEA1 and Rab5 in A549 lung carcinoma cells undergoing spreading, whereas Rab5 knock-down decreased the accumulation of calpain2 at early endosomal-enriched fractions. In addition, Rab5 silencing decreased calpain2 activity, as shown by cleavage of the fluorogenic substrate tBOC-LM-CMAC and the endogenous substrate talin. Accordingly, Rab5 promoted focal adhesion disassembly in a calpain2-dependent manner, as expression of GFP-Rab5 accelerated focal adhesion disassembly in nocodazole-synchronized cells, whereas pharmacological inhibition of calpain2 with N-acetyl-Leu-Leu-Met prevented both focal adhesion disassembly and cell migration induced by Rab5. In summary, these data uncover Rab5 as a novel regulator of calpain2 activity and focal adhesion proteolysis leading to cell migration.
早期核内体蛋白Rab5最近被证明通过增强局灶黏附分解来促进细胞迁移,其机制尚不明确。局灶性黏附解体与talin的蛋白水解有关,这一过程需要calpain2。由于在囊泡和内体腔室中发现了calpain2,我们假设Rab5刺激calpain2活性,导致迁移细胞中局灶性黏附分解增强。我们观察到,在A549肺癌细胞扩散过程中,calpain2与EEA1阳性的早期内体共定位,与EEA1和Rab5共免疫沉淀,而Rab5敲除减少了早期内体富集部分calpain2的积累。此外,Rab5的沉默降低了calpain2的活性,这可以从荧光底物tBOC-LM-CMAC和内源性底物talin的裂解中得到证实。因此,Rab5以依赖于calpain2的方式促进了局灶性粘附的破坏,因为GFP-Rab5的表达加速了nocodazole同步细胞的局灶性粘附的破坏,而n -乙酰- leu - leu - met对calpain2的药理学抑制既阻止了Rab5诱导的局灶性粘附的破坏,也阻止了Rab5诱导的细胞迁移。总之,这些数据揭示了Rab5作为calpain2活性和局灶黏附蛋白水解导致细胞迁移的新调节剂。