Koh Ara, Park Dohyun, Jeong Heeyoon, Lee Jiyoun, Lee Mi Nam, Suh Pann-Ghill, Ryu Sung Ho
Department of Life Sciences, Pohang University of Science and Technology, Pohang 790-784, South Korea.
School of Nano-Biotechnology and Chemical Engineering, Ulsan National Institute of Science and Technology, Ulsan 689-798, South Korea.
Cell Signal. 2014 Nov;26(11):2470-80. doi: 10.1016/j.cellsig.2014.07.033. Epub 2014 Aug 4.
C1-Ten is a member of the tensin family of focal adhesion molecules but recent studies suggest it plays a more active role in many biological processes because of its potential association with diabetes and cancers. However, relatively little is known about the regulation of C1-Ten, such as changes in its protein level or cellular localization. The cellular localization of C1-Ten is unique because it is expressed in cytoplasmic puncta but nothing is known about these puncta. Here, we show that p62 sequestrates C1-Ten into puncta, making C1-Ten diffuse into the cytoplasm upon p62 depletion. More importantly, p62-mediated C1-Ten sequestration promoted C1-Ten ubiquitination and proteasomal degradation. p62-mediated protein reduction was specific to C1-Ten, and not other tensins such as tensin1 and tensin3. Thus, our results link cellular localization of C1-Ten to an off-switch site for C1-Ten. Additionally, p62 expression increased but C1-Ten protein decreased during muscle differentiation, supporting a role for p62 as a physiological regulator of C1-Ten.
C1-Ten是粘着斑分子张力蛋白家族的一员,但最近的研究表明,由于其与糖尿病和癌症的潜在关联,它在许多生物学过程中发挥着更积极的作用。然而,关于C1-Ten的调控,如蛋白质水平或细胞定位的变化,人们了解得相对较少。C1-Ten的细胞定位很独特,因为它在细胞质斑点中表达,但对这些斑点却一无所知。在这里,我们表明p62将C1-Ten隔离到斑点中,使得在p62缺失时C1-Ten扩散到细胞质中。更重要的是,p62介导的C1-Ten隔离促进了C1-Ten的泛素化和蛋白酶体降解。p62介导的蛋白质减少对C1-Ten具有特异性,而对其他张力蛋白如张力蛋白1和张力蛋白3则没有影响。因此,我们的结果将C1-Ten的细胞定位与C1-Ten的一个关闭位点联系起来。此外,在肌肉分化过程中p62表达增加而C1-Ten蛋白减少,这支持了p62作为C1-Ten生理调节因子的作用。
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