Functional and in silico analysis of ATP8A2 and other P4-ATPase variants associated with human genetic diseases.

IF 4 3区 医学 Q2 CELL BIOLOGY
Disease Models & Mechanisms Pub Date : 2024-06-01 Epub Date: 2024-04-24 DOI:10.1242/dmm.050546
Eli Matsell, Jens Peter Andersen, Robert S Molday
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引用次数: 0

Abstract

P4-ATPases flip lipids from the exoplasmic to cytoplasmic leaflet of cell membranes, a property crucial for many biological processes. Mutations in P4-ATPases are associated with severe inherited and complex human disorders. We determined the expression, localization and ATPase activity of four variants of ATP8A2, the P4-ATPase associated with the neurodevelopmental disorder known as cerebellar ataxia, impaired intellectual development and disequilibrium syndrome 4 (CAMRQ4). Two variants, G447R and A772P, harboring mutations in catalytic domains, expressed at low levels and mislocalized in cells. In contrast, the E459Q variant in a flexible loop displayed wild-type expression levels, Golgi-endosome localization and ATPase activity. The R1147W variant expressed at 50% of wild-type levels but showed normal localization and activity. These results indicate that the G447R and A772P mutations cause CAMRQ4 through protein misfolding. The E459Q mutation is unlikely to be causative, whereas the R1147W may display a milder disease phenotype. Using various programs that predict protein stability, we show that there is a good correlation between the experimental expression of the variants and in silico stability assessments, suggesting that such analysis is useful in identifying protein misfolding disease-associated variants.

与人类遗传疾病相关的 ATP8A2 和其他 P4-ATP 酶变体的功能分析和 In-silico 分析。
P4-ATP 酶将脂质从细胞膜的外质小叶翻转到细胞质小叶,这一特性对许多生物过程至关重要。P4-ATP 酶的突变与严重的遗传性复杂人类疾病有关。我们确定了 ATP8A2 中四个变体的表达、定位和 ATP 酶活性,ATP8A2 是与小脑共济失调、智力迟钝和失衡综合征 4(CAMRQ4)相关的 P4-ATP 酶。Gly447Arg和Ala772Pro这两个变体的催化结构域发生了突变,它们在细胞中的表达量很低,而且定位错误。相反,柔性环中的 Glu459Gln 变体显示出野生型的表达水平、高尔基内体定位和 ATPase 活性。Arg1147Trp 变体的表达水平只有野生型的 50%,但定位和活性正常。这些结果表明,Gly447Arg 和 Ala772Pro 突变是通过蛋白质错误折叠引起 CAMRQ4 的。Glu459Gln 突变不太可能是致病因素,而 Arg1147Trp 突变可能表现出较轻的疾病表型。通过使用各种预测蛋白质稳定性的程序,我们发现变异体的实验表达与硅学稳定性评估之间存在良好的相关性,这表明此类分析有助于确定与疾病相关的错误折叠变异体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Disease Models & Mechanisms
Disease Models & Mechanisms 医学-病理学
CiteScore
6.60
自引率
7.00%
发文量
203
审稿时长
6-12 weeks
期刊介绍: Disease Models & Mechanisms (DMM) is an online Open Access journal focusing on the use of model systems to better understand, diagnose and treat human disease.
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