巨核细胞生成的变化及其在健康和疾病中的意义。

Changes in megakaryopoiesis over ontogeny and their implications in health and disease.

机构信息

Division of Newborn Medicine, Boston Children's Hospital and Harvard Medical School , Boston, MA, USA.

出版信息

Platelets. 2020 Aug 17;31(6):692-699. doi: 10.1080/09537104.2020.1742879. Epub 2020 Mar 21.

DOI:10.1080/09537104.2020.1742879

PMID:32200697

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8006558/

Abstract

A growing body of research has made it increasingly clear that there are substantial biological differences between fetal/neonatal and adult megakaryopoiesis. Over the last decade, studies revealed a developmentally unique uncoupling of proliferation, polyploidization, and cytoplasmic maturation in neonatal MKs that results in the production of large numbers of small, low ploidy, but mature MKs during this period of development, and identified substantial molecular differences between fetal/neonatal and adult MKs. This review will summarize our current knowledge on the developmental differences between fetal/neonatal and adult MKs, and recent advances in our understanding of the underlying molecular mechanisms, including newly described developmentally regulated pathways and miRNAs. We will also discuss the implications of these findings on the ways MKs interact with the environment, the response of neonates to thrombocytopenia, the pathogenesis of Down syndrome-transient myeloproliferative disorder (TMD), and the developmental stage specific-manifestations of congenital amegakaryocytic thrombocytopenia.

摘要

越来越多的研究表明，胎儿/新生儿和成人巨核细胞生成之间存在显著的生物学差异。在过去的十年中，研究揭示了新生儿巨核细胞增殖、多倍体形成和细胞质成熟的发育独特解耦，导致在此发育阶段产生大量小而低倍体但成熟的巨核细胞，并确定了胎儿/新生儿和成人巨核细胞之间存在大量分子差异。这篇综述将总结我们目前对胎儿/新生儿和成人巨核细胞发育差异的认识，以及我们对潜在分子机制理解的最新进展，包括新描述的发育调控途径和 miRNA。我们还将讨论这些发现对巨核细胞与环境相互作用方式、新生儿对血小板减少症的反应、唐氏综合征-短暂性骨髓增生异常（TMD）发病机制以及先天性无巨核细胞性血小板减少症的发育阶段特异性表现的影响。

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