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衰老与凋亡:哺乳动物发育的构建者

Senescence and Apoptosis: Architects of Mammalian Development.

作者信息

Wanner Emma, Thoppil Harikrishnan, Riabowol Karl

机构信息

Department of Biology, Faculty of Science, University of Calgary, Calgary, AB, Canada.

Department of Biochemistry and Molecular Biology, Cumming School of Medicine, University of Calgary, Calgary, AB, Canada.

出版信息

Front Cell Dev Biol. 2021 Jan 18;8:620089. doi: 10.3389/fcell.2020.620089. eCollection 2020.

Abstract

Mammalian development involves an exquisite choreography of cell division, differentiation, locomotion, programmed cell death, and senescence that directs the transformation of a single cell zygote to a mature organism containing on the order of 40 trillion cells in humans. How a single totipotent zygote undergoes the rapid stages of embryonic development to form over 200 different cell types is complex in the extreme and remains the focus of active research. Processes such as programmed cell death or apoptosis has long been known to occur during development to help sculpt organs and tissue systems. Other processes such as cellular senescence, long thought to only occur in pathologic states such as aging and tumorigenesis have been recently reported to play a vital role in development. In this review, we focus on apoptosis and senescence; the former as an integral mechanism that plays a critical role not only in mature organisms, but that is also essential in shaping mammalian development. The latter as a well-defined feature of aging for which some reports indicate a function in development. We will dissect the dual roles of major gene families, pathways such as Hox, Rb, p53, and epigenetic regulators such as the ING proteins in both early and the late stages and how they play antagonistic roles by increasing fitness and decreasing mortality early in life but contribute to deleterious effects and pathologies later in life.

摘要

哺乳动物的发育涉及细胞分裂、分化、运动、程序性细胞死亡和衰老的精妙编排,这些过程引导着单细胞受精卵转变为成熟的生物体,在人类中大约包含40万亿个细胞。单个全能受精卵如何经历胚胎发育的快速阶段,形成200多种不同的细胞类型,这极其复杂,仍然是活跃研究的焦点。诸如程序性细胞死亡或凋亡等过程长期以来已知在发育过程中发生,以帮助塑造器官和组织系统。其他过程,如细胞衰老,长期以来一直被认为只发生在诸如衰老和肿瘤发生等病理状态中,最近有报道称其在发育中起着至关重要的作用。在这篇综述中,我们聚焦于凋亡和衰老;前者作为一种不可或缺的机制,不仅在成熟生物体中起关键作用,而且在塑造哺乳动物发育过程中也至关重要。后者作为衰老的一个明确特征,一些报道表明其在发育中有功能。我们将剖析主要基因家族、诸如Hox、Rb、p53等信号通路以及诸如ING蛋白等表观遗传调节因子在早期和晚期的双重作用,以及它们如何通过在生命早期提高适应性和降低死亡率来发挥拮抗作用,但在生命后期会导致有害影响和病理状况。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/be05/7848110/29caba6dae69/fcell-08-620089-g001.jpg

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