肌球蛋白-IIA 重链 S1943 磷酸化调节肿瘤转移。
Myosin-IIA heavy chain phosphorylation on S1943 regulates tumor metastasis.
机构信息
Department of Biochemistry, Albert Einstein College of Medicine, 1300 Morris Park Avenue, Bronx, NY 10461, United States.
Department of Anatomy and Structural Biology, Albert Einstein College of Medicine, 1300 Morris Park Avenue, Bronx, NY 10461, United States.
出版信息
Exp Cell Res. 2018 Sep 15;370(2):273-282. doi: 10.1016/j.yexcr.2018.06.028. Epub 2018 Jun 25.
Abstract
Nonmuscle myosin-IIA (NMHC-IIA) heavy chain phosphorylation has gained recognition as an important feature of myosin-II regulation. In previous work, we showed that phosphorylation on S1943 promotes myosin-IIA filament disassembly in vitro and enhances EGF-stimulated lamellipod extension of breast tumor cells. However, the contribution of NMHC-IIA S1943 phosphorylation to the modulation of invasive cellular behavior and metastasis has not been examined. Stable expression of phosphomimetic (S1943E) or non-phosphorylatable (S1943A) NMHC-IIA in breast cancer cells revealed that S1943 phosphorylation enhances invadopodia function, and is critical for matrix degradation in vitro and experimental metastasis in vivo. These studies demonstrate a novel link between NMHC-IIA S1943 phosphorylation, the regulation of extracellular matrix degradation and tumor cell invasion and metastasis.
摘要
非肌肉肌球蛋白-IIA(NMHC-IIA)重链磷酸化已被认为是肌球蛋白-II 调节的一个重要特征。在之前的工作中,我们表明 S1943 的磷酸化促进了体外肌球蛋白-IIA 纤维的解体,并增强了 EGF 刺激的乳腺癌细胞片状伪足的延伸。然而,NMHC-IIA S1943 磷酸化对侵袭性细胞行为和转移的调节作用尚未得到检验。在乳腺癌细胞中稳定表达磷酸模拟物(S1943E)或非磷酸化(S1943A)NMHC-IIA 表明,S1943 磷酸化增强了侵袭小窝的功能,对于体外基质降解和体内实验性转移是至关重要的。这些研究表明 NMHC-IIA S1943 磷酸化、细胞外基质降解和肿瘤细胞侵袭转移之间存在新的联系。
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