SLC25A1 regulates placental development to ensure embryonic heart morphogenesis.

IF 3.7 2区 生物学 Q1 DEVELOPMENTAL BIOLOGY
Development Pub Date : 2024-11-15 Epub Date: 2024-11-26 DOI:10.1242/dev.204290
Wenli Fan, Zixuan Li, Xueke He, Xiaodong Wang, Ming Sun, Zhongzhou Yang
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引用次数: 0

Abstract

22q11.2 deletion syndrome (22q11.2DS) is the most common chromosomal microdeletion syndrome. Congenital heart defects are prevalent in 22q11.2DS but the etiology is still poorly understood. In this study, we aimed to gain mechanistic insights into the heart defects that result from 22q11.2 deletion, with a focus on Slc25a1, which is located in the deletion segment. Whereas global knockout of Slc25a1 in mice produced a variety of heart malformations, cardiac deletion of Slc25a1 had little effect on heart development. We then found that trophoblast-specific Slc25a1 deletion recapitulated heart anomalies in the global knockout mice. Further study identified SLC25A1 as a regulator of trophoblast and placental development through modulation of histone H3K27 acetylation at the promoters and enhancers of key genes involved in trophoblast differentiation. Finally, administration of recombinant human pregnancy-specific glycoprotein 1 (PSG1), a trophoblast-derived secretory glycoprotein, partially corrected placental and embryonic heart defects. This study defines the role of SLC25A1 in heart development by regulating placental development, and provides new insights to understand the etiology of 22q11.2DS.

SLC25A1 调节胎盘发育,确保胚胎心脏的形态形成。
22q11.2 缺失综合征(22q11.2DS)是最常见的染色体微缺失综合征。先天性心脏缺陷在 22q11.2DS 中很常见,但对其病因仍知之甚少。在这项研究中,我们旨在从机理上深入了解 22q11.2 缺失导致的心脏缺陷,重点是位于缺失区段的 Slc25a1。在小鼠体内全面敲除 Slc25a1 会导致多种心脏畸形,而心脏缺失 Slc25a1 对心脏发育几乎没有影响。我们随后发现,滋养层特异性 Slc25a1 基因缺失再现了全基因敲除小鼠的心脏畸形。进一步的研究发现,SLC25A1 通过调节参与滋养层分化的关键基因启动子和增强子上的组蛋白 H3K27 乙酰化,成为滋养层和胎盘发育的调控因子。最后,服用重组人妊娠特异性糖蛋白1(PSG1)--一种滋养层来源的分泌性糖蛋白--可部分纠正胎盘和胚胎心脏缺陷。这项研究确定了SLC25A1通过调节胎盘发育在心脏发育中的作用,并为了解22q11.2DS的病因提供了新的见解。
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来源期刊
Development
Development 生物-发育生物学
CiteScore
6.70
自引率
4.30%
发文量
433
审稿时长
3 months
期刊介绍: Development’s scope covers all aspects of plant and animal development, including stem cell biology and regeneration. The single most important criterion for acceptance in Development is scientific excellence. Research papers (articles and reports) should therefore pose and test a significant hypothesis or address a significant question, and should provide novel perspectives that advance our understanding of development. We also encourage submission of papers that use computational methods or mathematical models to obtain significant new insights into developmental biology topics. Manuscripts that are descriptive in nature will be considered only when they lay important groundwork for a field and/or provide novel resources for understanding developmental processes of broad interest to the community. Development includes a Techniques and Resources section for the publication of new methods, datasets, and other types of resources. Papers describing new techniques should include a proof-of-principle demonstration that the technique is valuable to the developmental biology community; they need not include in-depth follow-up analysis. The technique must be described in sufficient detail to be easily replicated by other investigators. Development will also consider protocol-type papers of exceptional interest to the community. We welcome submission of Resource papers, for example those reporting new databases, systems-level datasets, or genetic resources of major value to the developmental biology community. For all papers, the data or resource described must be made available to the community with minimal restrictions upon publication. To aid navigability, Development has dedicated sections of the journal to stem cells & regeneration and to human development. The criteria for acceptance into these sections is identical to those outlined above. Authors and editors are encouraged to nominate appropriate manuscripts for inclusion in one of these sections.
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