Zscan4 as a candidate conveyor of early developmental defects in O-GlcNAc transferase intellectual disability.

IF 5.5 2区生物学 Q1 BIOCHEMICAL RESEARCH METHODS

Molecular & Cellular Proteomics Pub Date : 2025-09-29 DOI:10.1016/j.mcpro.2025.101077

Veronica M Pravata, Hao Jiang, Andrew T Ferenbach, Angus Lamond, Daan M F van Aalten

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引用次数: 0

Abstract

Variants in the human β-N-acetylglucosamine (O-GlcNAc) transferase (OGT) gene give rise to an intellectual disability (ID) syndrome termed OGT congenital disorder of glycosylation (OGT-CDG). The mechanisms by which loss of OGT and/or protein O-GlcNAcylation lead to this syndrome are not understood, but symptoms associated with the syndrome suggest a developmental origin. Here, we establish and characterise two lines of mouse embryonic stem cells carrying different patient mutations and show that these mutations lead to disrupted O-GlcNAc homeostasis. Using quantitative proteomics on these cells in the pluripotent state, we identify candidate proteins/pathways that could underpin this syndrome. In addition to the increased levels of OGT and decreased levels of OGA reflecting disrupted O-GlcNAc homeostasis, we find that expression of the ID gene Zscan4 is upregulated. This is associated with increased levels of the OGT:Ten Eleven (Tet) - protein complex that regulates DNA methylation and Zscan4 expression. These data uncover a potential mechanism contributing to the developmental aspects of OGT-CDG.

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Zscan4作为O-GlcNAc转移酶智力残疾早期发育缺陷的候选传送带。

人类β- n -乙酰氨基葡萄糖（O-GlcNAc）转移酶（OGT）基因的变异导致一种称为OGT先天性糖基化障碍（OGT- cdg）的智力残疾（ID）综合征。OGT和/或o - glcn酰化蛋白缺失导致该综合征的机制尚不清楚，但与该综合征相关的症状提示其发育起源。在这里，我们建立并表征了携带不同患者突变的两种小鼠胚胎干细胞系，并表明这些突变导致O-GlcNAc稳态被破坏。在这些多能状态的细胞上使用定量蛋白质组学，我们确定了可能支持这种综合征的候选蛋白质/途径。除了OGT水平的升高和OGA水平的降低反映了O-GlcNAc稳态的破坏外，我们还发现ID基因Zscan4的表达上调。这与调节DNA甲基化和Zscan4表达的OGT:Ten - 11 （Tet）蛋白复合物水平升高有关。这些数据揭示了促进OGT-CDG发育方面的潜在机制。

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

Molecular & Cellular Proteomics 生物-生化研究方法

CiteScore

11.50

自引率

4.30%

发文量

131

审稿时长

84 days

期刊介绍： The mission of MCP is to foster the development and applications of proteomics in both basic and translational research. MCP will publish manuscripts that report significant new biological or clinical discoveries underpinned by proteomic observations across all kingdoms of life. Manuscripts must define the biological roles played by the proteins investigated or their mechanisms of action. The journal also emphasizes articles that describe innovative new computational methods and technological advancements that will enable future discoveries. Manuscripts describing such approaches do not have to include a solution to a biological problem, but must demonstrate that the technology works as described, is reproducible and is appropriate to uncover yet unknown protein/proteome function or properties using relevant model systems or publicly available data. Scope: -Fundamental studies in biology, including integrative "omics" studies, that provide mechanistic insights -Novel experimental and computational technologies -Proteogenomic data integration and analysis that enable greater understanding of physiology and disease processes -Pathway and network analyses of signaling that focus on the roles of post-translational modifications -Studies of proteome dynamics and quality controls, and their roles in disease -Studies of evolutionary processes effecting proteome dynamics, quality and regulation -Chemical proteomics, including mechanisms of drug action -Proteomics of the immune system and antigen presentation/recognition -Microbiome proteomics, host-microbe and host-pathogen interactions, and their roles in health and disease -Clinical and translational studies of human diseases -Metabolomics to understand functional connections between genes, proteins and phenotypes