突变蛋白的折叠缺陷和快速降解是遗传疾病中常见的疾病机制。

Defective folding and rapid degradation of mutant proteins is a common disease mechanism in genetic disorders.

作者信息

Gregersen N, Bross P, Jørgensen M M, Corydon T J, Andresen B S

机构信息

Research Unit for Molecular Medicine, Aarhus University Hospital, Skejby Sygehus, Denmark.

出版信息

J Inherit Metab Dis. 2000 Jul;23(5):441-7. doi: 10.1023/a:1005663728291.

DOI:10.1023/a:1005663728291

PMID:10947197

Abstract

Many disease-causing point mutations do not seriously compromise synthesis of the affected polypeptide but rather exert their effects by impairing subsequent protein folding or stability of the folded protein. This often results in rapid degradation of the affected protein. The concepts of such 'conformational disease' are illustrated by reference to cystic fibrosis, phenylketonuria and short-chain acyl-CoA dehydrogenase deficiency. Other cellular components such as chaperones and proteases, as well as environmental factors, may combine to modulate the phenotype of such disorders and this may open up new therapeutic approaches.

摘要

许多致病点突变不会严重损害受影响多肽的合成，而是通过损害后续蛋白质折叠或折叠后蛋白质的稳定性来发挥作用。这通常会导致受影响蛋白质的快速降解。通过参考囊性纤维化、苯丙酮尿症和短链酰基辅酶A脱氢酶缺乏症来说明这种“构象性疾病”的概念。其他细胞成分如伴侣蛋白和蛋白酶，以及环境因素，可能共同调节这些疾病的表型，这可能会开辟新的治疗方法。

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突变蛋白的折叠缺陷和快速降解是遗传疾病中常见的疾病机制。

Defective folding and rapid degradation of mutant proteins is a common disease mechanism in genetic disorders.

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