Insights into the sperm chromatin and implications for male infertility from a protein perspective.

IF 4.6 3区 医学 Q2 MEDICINE, RESEARCH & EXPERIMENTAL
Alberto de la Iglesia, Meritxell Jodar, Rafael Oliva, Judit Castillo
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引用次数: 6

Abstract

Male germ cells undergo an extreme but fascinating process of chromatin remodeling that begins in the testis during the last phase of spermatogenesis and continues through epididymal sperm maturation. Most of the histones are replaced by small proteins named protamines, whose high basicity leads to a tight genomic compaction. This process is epigenetically regulated at many levels, not only by posttranslational modifications, but also by readers, writers, and erasers, in a context of a highly coordinated postmeiotic gene expression program. Protamines are key proteins for acquiring this highly specialized chromatin conformation, needed for sperm functionality. Interestingly, and contrary to what could be inferred from its very specific DNA-packaging function across protamine-containing species, human sperm chromatin contains a wide spectrum of protamine proteoforms, including truncated and posttranslationally modified proteoforms. The generation of protamine knock-out models revealed not only chromatin compaction defects, but also collateral sperm alterations contributing to infertile phenotypes, evidencing the importance of sperm chromatin protamination toward the generation of a new individual. The unique features of sperm chromatin have motivated its study, applying from conventional to the most ground-breaking techniques to disentangle its peculiarities and the cellular mechanisms governing its successful conferment, especially relevant from the protein point of view due to the important epigenetic role of sperm nuclear proteins. Gathering and contextualizing the most striking discoveries will provide a global understanding of the importance and complexity of achieving a proper chromatin compaction and exploring its implications on postfertilization events and beyond. This article is categorized under: Reproductive System Diseases > Genetics/Genomics/Epigenetics Reproductive System Diseases > Molecular and Cellular Physiology.

Abstract Image

Abstract Image

从蛋白质的角度深入了解精子染色质及其对男性不育的影响。
男性生殖细胞经历了一个极端而迷人的染色质重塑过程,这个过程始于精子发生的最后阶段,一直持续到附睾精子成熟。大多数组蛋白被称为精蛋白的小蛋白质所取代,其高碱度导致基因组紧密压实。在减数分裂后基因表达程序高度协调的背景下,这一过程在许多水平上受到表观遗传调控,不仅通过翻译后修饰,还通过读取器、写入器和擦除器。精氨酸是获得这种高度特化的染色质构象的关键蛋白质,是精子功能所必需的。有趣的是,与从含有鱼精蛋白的物种中其非常特殊的dna包装功能推断的相反,人类精子染色质含有广泛的鱼精蛋白蛋白形式,包括截断和翻译后修饰的蛋白质形式。鱼精蛋白敲除模型的产生不仅揭示了染色质压实缺陷,而且还揭示了导致不育表型的附带精子改变,证明了精子染色质蛋白化对新个体产生的重要性。精子染色质的独特特征激发了它的研究,从传统到最具突破性的技术来解开它的特性和控制其成功授予的细胞机制,特别是从蛋白质的角度来看,由于精子核蛋白的重要表观遗传作用。收集和背景下最引人注目的发现将提供实现适当的染色质压实的重要性和复杂性的全球理解,并探索其对受精后事件和超越的影响。本文分类如下:生殖系统疾病>遗传学/基因组学/表观遗传学生殖系统疾病>分子和细胞生理学。
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
WIREs Mechanisms of Disease
WIREs Mechanisms of Disease MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
11.40
自引率
0.00%
发文量
45
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