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由双突变R217Q/R402Q导致的人重组酪氨酸酶不稳定化。

Human recombinant tyrosinase destabilization caused by the double mutation R217Q/R402Q.

作者信息

Toay Sarah, Sheri Narin, MacDonald Ian, Sergeev Yuri V

机构信息

Protein Biochemistry and Molecular Modeling Group, OGVFB, National Eye Institute, National Institutes of Health, Bethesda, Maryland, USA.

Department of Ophthalmology & Visual Sciences, University of Alberta, Edmonton, Canada.

出版信息

Protein Sci. 2025 Feb;34(2):e70029. doi: 10.1002/pro.70029.

Abstract

Oculocutaneous albinism is an autosomal recessive inherited disorder associated with mutations in the TYR gene. A single missense change in the tyrosinase (Tyr) could result in partial or complete loss of catalytic activity. The effect of two genetic mutations in the same Tyr as the molecule is less studied. Here, we study single mutation variants, R217Q, R402Q, and a double mutant variant, R217Q/R402Q, to establish a link between alterations at the level of the atomic model of the protein and the disease phenotype. Human recombinant intra-melanosomal Tyr domains of Tyr and three mutant variants were expressed in T. ni. Larvae were purified using the combination of IMAC and SEC, and diphenolase activities were measured. The Tyr homology model was equilibrated using 100 ns molecular dynamics and analyzed using computational methods. The purified R217Q and R217Q/R402Q variants show decreased catalytic activities compared to those of the Tyr and R402Q variants. The R217Q/R402Q variant has the lowest protein activity and is significantly reduced.

摘要

眼皮肤白化病是一种常染色体隐性遗传性疾病,与酪氨酸酶(TYR)基因突变有关。酪氨酸酶(Tyr)中的单个错义变化可能导致催化活性部分或完全丧失。对同一Tyr分子中两个基因突变的影响研究较少。在这里,我们研究单突变变体R217Q、R402Q和双突变变体R217Q/R402Q,以建立蛋白质原子模型水平的改变与疾病表型之间的联系。Tyr和三个突变变体的人重组黑素体内Tyr结构域在烟草天蛾中表达。幼虫通过IMAC和SEC组合进行纯化,并测量双酚酶活性。使用100 ns分子动力学对Tyr同源模型进行平衡,并使用计算方法进行分析。与Tyr和R402Q变体相比,纯化的R217Q和R217Q/R402Q变体显示出催化活性降低。R217Q/R402Q变体的蛋白质活性最低,且显著降低。

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