The alpha-kinases TRPM6 and TRPM7, but not eEF-2 kinase, phosphorylate the assembly domain of myosin IIA, IIB and IIC.

Clark K; Middelbeek J; Dorovkov MV; Figdor CG; Ryazanov AG; Lasonder E; van-Leeuwen FN

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The alpha-kinases TRPM6 and TRPM7, but not eEF-2 kinase, phosphorylate the assembly domain of myosin IIA, IIB and IIC.

机译：α激酶TRPM6和TRPM7而不是eEF-2激酶使肌球蛋白IIA，IIB和IIC的装配结构域磷酸化。

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摘要

TRPM6 and TRPM7 encode channel-kinases. While these channels share electrophysiological properties and cellular functions, TRPM6 and TRPM7 are non-redundant genes raising the possibility that the kinases have distinct substrates. Here, we demonstrate that TRPM6 and TRPM7 phosphorylate the assembly domain of myosin IIA, IIB and IIC on identical residues. Whereas phosphorylation of myosin IIA is restricted to the coiled-coil domain, TRPM6 and TRPM7 also phosphorylate the non-helical tails of myosin IIB and IIC. TRPM7 does not phosphorylate eukaryotic elongation factor-2 (eEF-2) and myosin II is a poor substrate for eEF-2 kinase. In conclusion, TRPM6 and TRPM7 share exogenous substrates among themselves but not with functionally distant alpha-kinases. STRUCTURED SUMMARY:

机译：TRPM6和TRPM7编码通道激酶。虽然这些通道共享电生理特性和细胞功能，但TRPM6和TRPM7是非冗余基因，增加了激酶具有不同底物的可能性。在这里，我们证明TRPM6和TRPM7磷酸化肌球蛋白IIA，IIB和IIC的装配结构域在相同的残基上。肌球蛋白IIA的磷酸化仅限于卷曲螺旋域，而TRPM6和TRPM7也会使肌球蛋白IIB和IIC的非螺旋尾部磷酸化。 TRPM7不会磷酸化真核延伸因子2（eEF-2），而肌球蛋白II是eEF-2激酶的较弱底物。总之，TRPM6和TRPM7之间共享外源底物，但功能上相距遥远的α激酶却不共享。结构总结：

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来源
《FEBS letters. 》 |2008年第20期| 共5页
作者
Clark K; Middelbeek J; Dorovkov MV; Figdor CG; Ryazanov AG; Lasonder E; van-Leeuwen FN;
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正文语种 eng
中图分类生物化学 ;
关键词
Myosins; Phosphotransferases; Financially poor; Cellular biology; 磷酸转移酶类;

机译：Myosins;Phosphotransferases;Financially poor;Cellular biology;磷酸转移酶类;

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1. The alpha-kinases TRPM6 and TRPM7, but not eEF-2 kinase, phosphorylate the assembly domain of myosin IIA, IIB and IIC. [J] . Clark K, Middelbeek J, Dorovkov MV, FEBS letters. . 2008 ,第20期

机译：α激酶TRPM6和TRPM7而不是eEF-2激酶使肌球蛋白IIA，IIB和IIC的装配结构域磷酸化。
2. Identification of dimer interactions required for the catalytic activity of the TRPM7 alpha-kinase domain [J] . Graham P. C?té, Scott W. Crawley The biochemical journal . 2009 ,第1期

机译：鉴定TRPM7α激酶结构域催化活性所需的二聚体相互作用
3. Identification of dimer interactions required for the catalytic activity of the TRPM7 alpha-kinase domain [J] . Crawley SW, Cote GP The Biochemical Journal . 2009 ,第1期

机译：鉴定TRPM7α激酶结构域催化活性所需的二聚体相互作用
4. The CrkRS/CDK12 kinase is activated by a novel isoform of Cyclin K and phosphorylates and the C-terminal domain of RNA Pol II [C] . Annie Moradian, S.-W. Grace Cheng, Michael Kuzyk, American Society for Mass Spectrometry Conference on Mass Spectrometry and Allied Topics . 2009

机译：CrKRS / CDK12激酶通过细胞周期蛋白K和磷酸化合物的新型同种型和RNA POL II的C末端结构域激活
5. The Myosin-Binding UCS Domain but not the Hsp90-Binding TPR Domain of the UNC-45 Chaperone is Essential for Myosin Accumulation and Assembly in Caenorhabditis elegans [D] . Ni, Weiming. 2011

机译：肌苷结合的UCS结构域但不是UNC-45伴侣的HSP90结合TPR结构域对于Caenorhabditis elegans中的肌球蛋白积累和组装是必不可少的
6. Elucidating the role of the TRPM7 alpha-kinase: TRPM7 kinase inactivation leads to magnesium deprivation resistance phenotype in mice [O] . Lillia V. Ryazanova, Zhixian Hu, Sayuri Suzuki, -1

机译：阐明TRPM7α激酶的作用：TRPM7激酶失活导致小鼠对镁缺乏的抵抗性表型
7. The α-kinases TRPM6 and TRPM7, but not eEF-2 kinase, phosphorylate the assembly domain of myosin IIA, IIB and IIC [O] . Clark Kristopher, Middelbeek Jeroen, Dorovkov Maxim V., 2008

机译：α激酶TRPM6和TRPM7而不是eEF-2激酶使肌球蛋白IIA，IIB和IIC的装配结构域磷酸化

The alpha-kinases TRPM6 and TRPM7, but not eEF-2 kinase, phosphorylate the assembly domain of myosin IIA, IIB and IIC.

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