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使用 MeCP2 E1 和 E2 异构体中的相关 Rett 突变来测试 PEST 假说。

Testing the PEST hypothesis using relevant Rett mutations in MeCP2 E1 and E2 isoforms.

机构信息

Department of Biochemistry and Microbiology, University of Victoria, 3800 Finnerty Rd, Victoria, BC V8W 2Y2, Canada.

Department of Biology, University of Victoria, 3800 Finnerty Rd, Victoria, BC V8W 2Y2, Canada.

出版信息

Hum Mol Genet. 2024 Nov 5;33(21):1833-1845. doi: 10.1093/hmg/ddae119.

Abstract

Mutations in methyl-CpG binding protein 2 (MeCP2), such as the T158M, P152R, R294X, and R306C mutations, are responsible for most Rett syndrome (RTT) cases. These mutations often result in altered protein expression that appears to correlate with changes in the nuclear size; however, the molecular details of these observations are poorly understood. Using a C2C12 cellular system expressing human MeCP2-E1 isoform as well as mouse models expressing these mutations, we show that T158M and P152R result in a decrease in MeCP2 protein, whereas R306C has a milder variation, and R294X resulted in an overall 2.5 to 3 fold increase. We also explored the potential involvement of the MeCP2 PEST domains in the proteasome-mediated regulation of MeCP2. Finally, we used the R294X mutant to gain further insight into the controversial competition between MeCP2 and histone H1 in the chromatin context. Interestingly, in R294X, MeCP2 E1 and E2 isoforms were differently affected, where the E1 isoform contributes to much of the overall protein increase observed, while E2 decreases by half. The modes of MeCP2 regulation, thus, appear to be differently regulated in the two isoforms.

摘要

甲基化 CpG 结合蛋白 2(MeCP2)中的突变,如 T158M、P152R、R294X 和 R306C 突变,是大多数雷特综合征(RTT)病例的原因。这些突变通常导致蛋白表达的改变,似乎与核大小的变化相关;然而,这些观察结果的分子细节尚不清楚。使用表达人类 MeCP2-E1 异构体的 C2C12 细胞系统以及表达这些突变的小鼠模型,我们表明 T158M 和 P152R 导致 MeCP2 蛋白减少,而 R306C 则有较轻的变化,R294X 则导致总体增加 2.5 到 3 倍。我们还探讨了 MeCP2 PEST 结构域在蛋白酶体介导的 MeCP2 调节中的潜在作用。最后,我们使用 R294X 突变体进一步深入了解在染色质背景下 MeCP2 和组蛋白 H1 之间有争议的竞争。有趣的是,在 R294X 中,MeCP2 E1 和 E2 异构体受到不同的影响,其中 E1 异构体对观察到的大部分总体蛋白增加有贡献,而 E2 则减少了一半。因此,MeCP2 的调节方式似乎在两种异构体中受到不同的调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/277a/11540922/a59b66e45e6d/ddae119f1.jpg

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