色氨酸800处平滑肌肌球蛋白轻链激酶的突变体。
Mutants of smooth muscle myosin light chain kinase at tryptophan 800.
作者信息
Matsushima S, Huang Y P, Dudas C V, Guerriero V, Hartshorne D J
机构信息
Muscle Biology Group, University of Arizona, Tucson 85721.
出版信息
Biochem Biophys Res Commun. 1994 Aug 15;202(3):1329-36. doi: 10.1006/bbrc.1994.2076.
The importance of Trp 800 in the calmodulin-binding site of myosin light chain kinase was investigated. Truncation mutants from Leu 447 to the C-terminus were expressed in E. coli and these were modified by point mutations of Trp 800 to Gly, Cys, Leu and Tyr. Trp at this position was more effective than any of the other residues. The Leu mutant was partially active and its Km for calmodulin decreased from about 10 nM to 175 nM. The Tyr mutant had detectable activity but the other two mutants were inactive and did not bind calmodulin. Thus Trp at position 800 is critical. The activity of the Leu mutant at high calmodulin concentrations was less than the wild-type mutant, about 20%. This suggests that the binding of calmodulin does not release inhibition in an all-or-none mechanism and that other intramolecular interactions are important.
研究了色氨酸800在肌球蛋白轻链激酶钙调蛋白结合位点中的重要性。从亮氨酸447到C端的截短突变体在大肠杆菌中表达,并通过将色氨酸800点突变为甘氨酸、半胱氨酸、亮氨酸和酪氨酸对其进行修饰。该位置的色氨酸比其他任何残基都更有效。亮氨酸突变体具有部分活性,其对钙调蛋白的Km值从约10 nM降至175 nM。酪氨酸突变体具有可检测到的活性,但其他两个突变体无活性且不结合钙调蛋白。因此,800位的色氨酸至关重要。亮氨酸突变体在高钙调蛋白浓度下的活性低于野生型突变体,约为20%。这表明钙调蛋白的结合并非以全或无的机制解除抑制,其他分子内相互作用也很重要。
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