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Identification of Cardiac-Specific Myosin Light Chain Kinase

机译:心脏特异性肌球蛋白轻链激酶的鉴定

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摘要

Two myosin light chain (MLC) kinase (MLCK) proteins, smooth muscle (encoded by mylk1 gene) and skeletal (encoded by mylk2 gene) MLCK, have been shown to be expressed in mammals. Even though phosphorylation of its putative substrate, MLC2, is recognized as a key regulator of cardiac contraction, a MLCK that is preferentially expressed in cardiac muscle has not yet been identified. In this study, we characterized a new kinase encoded by a gene homologous to mylk1 and -2, named cardiac MLCK, which is specifically expressed in the heart in both atrium and ventricle. In fact, expression of cardiac MLCK is highly regulated by the cardiac homeobox protein Nkx2-5 in neonatal cardiomyocytes. The overall structure of cardiac MLCK protein is conserved with skeletal and smooth muscle MLCK; however, the amino terminus is quite unique, without significant homology to other known proteins, and its catalytic activity does not appear to be regulated by Ca2+/calmodulin in vitro. Cardiac MLCK is phosphorylated and the level of phosphorylation is increased by phenylephrine stimulation accompanied by increased level of MLC2v phosphorylation. Both overexpression and knockdown of cardiac MLCK in cultured cardiomyocytes revealed that cardiac MLCK is likely a new regulator of MLC2 phosphorylation, sarcomere organization, and cardiomyocyte contraction.
机译:两种肌球蛋白轻链(MLC)激酶(MLCK)蛋白,平滑肌(由mylk1基因编码)和骨骼肌(由mylk2基因编码)MLCK已显示在哺乳动物中表达。尽管公认的底物MLC2的磷酸化被认为是心脏收缩的关键调节剂,但尚未鉴定出在心肌中优先表达的MLCK。在这项研究中,我们表征了一种新的激酶,该激酶由与mylk1和-2同源的基因编码,称为心脏MLCK,在心脏的心房和心室中均特异性表达。实际上,新生儿心肌细胞中心脏ML的表达受心脏同源盒蛋白Nkx2-5的高度调节。心脏MLCK蛋白的总体结构与骨骼和平滑肌MLCK保守。然而,氨基末端非常独特,与其他已知蛋白质没有显着同源性,并且其催化活性似乎在体外不受Ca 2 + /钙调蛋白的调节。心脏MLCK被磷酸化,并且通过去氧肾上腺素刺激增加了磷酸化水平,同时增加了MLC2v磷酸化水平。在培养的心肌细胞中心脏MLCK的过表达和敲低都表明,心脏MLCK可能是MLC2磷酸化,肌节组织和心肌细胞收缩的新调节剂。

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