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与先天性红细胞生成性卟啉症相关的尿卟啉原III合酶突变确定了蛋白质稳定性的关键螺旋。

Uroporphyrinogen III synthase mutations related to congenital erythropoietic porphyria identify a key helix for protein stability.

作者信息

Fortian Arola, Castaño David, Ortega Gabriel, Laín Ana, Pons Miquel, Millet Oscar

机构信息

Structural Biology Unit, CIC bioGUNE, Bizkaia Technology Park, Building 800, 48160 Derio, Spain.

出版信息

Biochemistry. 2009 Jan 20;48(2):454-61. doi: 10.1021/bi801731q.

Abstract

In the present study we have investigated deleterious mutants in the uroporphyrinogen III synthase (UROIIIS) that are related to the congenital erythropoietic porphyria (CEP). The 25 missense mutants found in CEP patients have been cloned, expressed, and purified. Their enzymatic activities have been measured relative to wild-type UROIIIS activity. All mutants retain measurable activity, consistent with the recessive character of the disease. Most of the mutants with a significant decrease in activity involve residues likely associated in binding. However, other mutants are fully active, indicating that different mechanisms may contribute to enzyme missfunction. UROIIIS is a thermolabile enzyme undergoing irreversible denaturation. The unfolding kinetics of wild-type UROIIIS and the suite of mutants have been monitored by circular dichroism. This analysis allowed the identification of a helical region in the molecule, essential to retain the kinetic stability of the folded conformation. C73R is found in one-third of CEP patients, and Cys73 is part of this helix. The integrated analysis of the enzymatic activity and kinetic stability data is used to gain insight in the relationship between defects in UROIIIS sequence and CEP.

摘要

在本研究中,我们研究了与先天性红细胞生成性卟啉症(CEP)相关的尿卟啉原III合酶(UROIIIS)中的有害突变体。已克隆、表达并纯化了在CEP患者中发现的25个错义突变体。已相对于野生型UROIIIS活性测量了它们的酶活性。所有突变体均保留可测量的活性,这与该疾病的隐性特征一致。大多数活性显著降低的突变体涉及可能与结合相关的残基。然而,其他突变体具有完全活性,表明不同的机制可能导致酶功能异常。UROIIIS是一种热不稳定酶,会发生不可逆变性。通过圆二色性监测了野生型UROIIIS和一系列突变体的解折叠动力学。该分析确定了分子中的一个螺旋区域,该区域对于保持折叠构象的动力学稳定性至关重要。在三分之一的CEP患者中发现了C73R,并且半胱氨酸73是该螺旋的一部分。酶活性和动力学稳定性数据的综合分析用于深入了解UROIIIS序列缺陷与CEP之间的关系。

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