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平滑肌肌球蛋白激酶需要磷酸化位点羧基末端一侧的残基。肽类抑制剂。

Smooth muscle myosin kinase requires residues on the COOH-terminal side of the phosphorylation site. Peptide inhibitors.

作者信息

Pearson R B, Misconi L Y, Kemp B E

出版信息

J Biol Chem. 1986 Jan 5;261(1):25-7.

PMID:3941075
Abstract

The COOH-terminal residue in peptide analogs of the phosphorylation site sequence in smooth muscle myosin light chains, Lys11-Lys12-Arg13-Ala-Ala-Arg16-Ala-Thr-Ser19 -(P)Asn20-Val21-Phe22-Ala23, were shown to have a strong influence on the kinetics of peptide phosphorylation. The peptides 11-19, 11-20, 11-21, 11-22, and 11-23 were all phosphorylated by the myosin light chain kinase with similar apparent Km values in the range 11-17 microM. The Vmax varied 40-fold, with the peptides 11-19, 11-20, 11-21, 11-22, and 11-23 having Vmax values of 0.035, 0.045, 0.32, 1.74, and 1.43 mumol X min-1 X mg-1 respectively. These results indicated that Ala23 was not essential whereas Phe22 and Val21 had a strong influence on the Vmax of peptide phosphorylation. This series of peptides competitively inhibited myosin light chain phosphorylation with Ki values similar to their respective Km values. Peptide 11-19 had a Ki value of approximately 10 microM and a Vmax less than 0.1% of the value with myosin light chains and is therefore an effective inhibitor of the smooth muscle myosin kinase.

摘要

平滑肌肌球蛋白轻链磷酸化位点序列肽类似物中的羧基末端残基,即Lys11-Lys12-Arg13-Ala-Ala-Arg16-Ala-Thr-Ser19-(P)Asn20-Val21-Phe22-Ala23,已显示对肽磷酸化动力学有强烈影响。肽11-19、11-20、11-21、11-22和11-23均被肌球蛋白轻链激酶磷酸化,其表观Km值相似,范围为11-17微摩尔。Vmax变化了40倍,肽11-19、11-20、11-21、11-22和11-23的Vmax值分别为0.035、0.045、0.32、1.74和1.43微摩尔·分钟-1·毫克-1。这些结果表明Ala23并非必需,而Phe22和Val21对肽磷酸化的Vmax有强烈影响。这一系列肽竞争性抑制肌球蛋白轻链磷酸化,其Ki值与其各自的Km值相似。肽11-19的Ki值约为10微摩尔,Vmax小于肌球蛋白轻链值的0.1%,因此是平滑肌肌球蛋白激酶的有效抑制剂。

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