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The pyruvate kinase model system a cautionary tale for the use of osmolyte perturbations to support conformational equilibria in allostery

机译:丙酮酸激酶模型系统使用渗透压微扰来支持构象构象平衡的警示性故事

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摘要

In the study of rabbit muscle pyruvate kinase (M1-PYK), proline has previously been used as an osmolyte in an attempt to determine a role for preexisting conformational equilibria in allosteric regulation. In this context, osmolytes are small molecules assumed to have no direct interaction with the protein. In contrast to proline's proposed role as an osmolyte, the structure of M1PYK-Mn-pyruvate-proline complex reported herein demonstrates that proline binds specifically to the allosteric site of M1-PYK. Therefore, this amino acid is an allosteric effector rather than a benign osmolyte. Other compounds often used as osmolytes (polyethyleneglycol and glycerol) are also present in the structure, suggesting an interaction with the protein that would, in turn, prevent the usefulness of these compounds in the study of this and most likely other proteins. These findings highlight the need to verify that compounds used as osmolytes to perturb preexisting conformational equilibrium do not directly interact with the protein, a consideration not commonly addressed in the past.
机译:在兔肌肉丙酮酸激酶(M1-PYK)的研究中,脯氨酸先前已用作渗透压剂,试图确定构象平衡中已存在的构象平衡的作用。在这种情况下,渗透压剂是假定与蛋白质没有直接相互作用的小分子。与脯氨酸提议的渗透压作用相反,本文报道的M1PYK-Mn-丙酮酸-脯氨酸复合物的结构证明脯氨酸特异性结合M1-PYK的变构位点。因此,该氨基酸是变构效应物,而不是良性渗透压物质。结构中还存在其他通常用作渗透液的化合物(聚乙二醇和甘油),这表明与该蛋白质的相互作用反过来又会阻止这些化合物在研究该蛋白质以及最可能的其他蛋白质中的有用性。这些发现凸显了需要验证用作渗透物以扰乱预先存在的构象平衡的化合物不会直接与蛋白质相互作用的问题,而这在过去是不常见的。

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