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Effect of antisense peptide binding on the dimerization of human cystatin C — gel electrophoresis and molecular modeling studies

机译:反义肽结合对人胱抑素C凝胶电泳二聚化的影响及分子模型研究

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摘要

Human cystatin C (HCC) shows a tendency to dimerize. This process is particularly easy in the case of the L68Q HCC mutant and might lead to formation of amyloid deposits in brain arteries of young adults. Our purpose was to find ligands of monomeric HCC that can prevent its dimerization. Eleven antisense peptide ligands of monomeric HCC were designed and synthesized. The influence of these ligands on HCC dimerization was studied using gel electrophoresis and molecular modeling methods. The results suggest that all the designed peptides interact with monomeric HCC facilitating its dimerization rather than preventing it.
机译:人胱抑素C(HCC)显示出二聚化趋势。对于L68Q HCC突变体,此过程特别容易,并且可能导致年轻人脑动脉中淀粉样蛋白沉积物的形成。我们的目的是找到可以阻止其二聚化的单体HCC的配体。设计并合成了11种单体HCC的反义肽配体。使用凝胶电泳和分子建模方法研究了这些配体对HCC二聚化的影响。结果表明,所有设计的肽均与单体HCC相互作用,促进其二聚而不是阻止其形成。

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