The genetics of cardiomyocyte polyploidy.

2区 生物学 Q1 Biochemistry, Genetics and Molecular Biology
Current Topics in Developmental Biology Pub Date : 2024-01-01 Epub Date: 2024-02-06 DOI:10.1016/bs.ctdb.2024.01.008
Tyler Buddell, Alexandra L Purdy, Michaela Patterson
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引用次数: 0

Abstract

The regulation of ploidy in cardiomyocytes is a complex and tightly regulated aspect of cardiac development and function. Cardiomyocyte ploidy can range from diploid (2N) to 8N or even 16N, and these states change during key stages of development and disease progression. Polyploidization has been associated with cellular hypertrophy to support normal growth of the heart, increased contractile capacity, and improved stress tolerance in the heart. Conversely, alterations to ploidy also occur during cardiac pathogenesis of diseases, such as ischemic and non-ischemic heart failure and arrhythmia. Therefore, understanding which genes control and modulate cardiomyocyte ploidy may provide mechanistic insight underlying cardiac growth, regeneration, and disease. This chapter summarizes the current knowledge regarding the genes involved in the regulation of cardiomyocyte ploidy. We discuss genes that have been directly tested for their role in cardiomyocyte polyploidization, as well as methodologies used to identify ploidy alterations. These genes encode cell cycle regulators, transcription factors, metabolic proteins, nuclear scaffolding, and components of the sarcomere, among others. The general physiological and pathological phenotypes in the heart associated with the genetic manipulations described, and how they coincide with the respective cardiomyocyte ploidy alterations, are further discussed in this chapter. In addition to being candidates for genetic-based therapies for various cardiac maladies, these genes and their functions provide insightful evidence regarding the purpose of widespread polyploidization in cardiomyocytes.

心肌细胞多倍体的遗传学。
心肌细胞倍性的调节是心脏发育和功能的一个复杂而严格的方面。心肌细胞倍性的范围从二倍体(2N)到 8N 甚至 16N,这些状态在发育和疾病进展的关键阶段会发生变化。多倍体化与细胞肥大有关,可支持心脏的正常生长、增强收缩能力并改善心脏的应激耐受性。相反,倍性的改变也发生在心脏疾病的发病过程中,如缺血性和非缺血性心力衰竭和心律失常。因此,了解哪些基因可控制和调节心肌细胞倍性,可从机理上揭示心脏生长、再生和疾病的根本原因。本章总结了目前有关参与调控心肌细胞倍性的基因的知识。我们讨论了已直接检测其在心肌细胞多倍体化中作用的基因,以及用于鉴定多倍体改变的方法。这些基因编码细胞周期调节因子、转录因子、代谢蛋白、核支架和肌节成分等。本章将进一步讨论与所述基因操作相关的心脏一般生理和病理表型,以及这些表型如何与相应的心肌细胞倍性改变相吻合。这些基因及其功能除了可作为治疗各种心脏疾病的基因疗法的候选基因外,还为心肌细胞广泛多倍体化的目的提供了深刻的证据。
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
CiteScore
6.00
自引率
0.00%
发文量
91
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