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涡虫作为一种新的模型系统,用于理解干细胞多能性和分化的表观遗传调控。

Planarian flatworms as a new model system for understanding the epigenetic regulation of stem cell pluripotency and differentiation.

机构信息

Department of Zoology, South Parks Road, University of Oxford, OX1 3PS, UK.

Department of Zoology, South Parks Road, University of Oxford, OX1 3PS, UK.

出版信息

Semin Cell Dev Biol. 2019 Mar;87:79-94. doi: 10.1016/j.semcdb.2018.04.007. Epub 2018 Apr 27.

Abstract

Planarian flatworms possess pluripotent stem cells (neoblasts) that are able to differentiate into all cell types that constitute the adult body plan. Consequently, planarians possess remarkable regenerative capabilities. Transcriptomic studies have revealed that gene expression is coordinated to maintain neoblast pluripotency, and ensure correct lineage specification during differentiation. But as yet they have not revealed how this regulation of expression is controlled. In this review, we propose that planarians represent a unique and effective system to study the epigenetic regulation of these processes in an in vivo context. We consolidate evidence suggesting that although DNA methylation is likely present in some flatworm lineages, it does not regulate neoblast function in Schmidtea mediterranea. A number of phenotypic studies have documented the role of histone modification and chromatin remodelling complexes in regulating distinct neoblast processes, and we focus on four important examples of planarian epigenetic regulators: Nucleosome Remodeling Deacetylase (NuRD) complex, Polycomb Repressive Complex (PRC), the SET1/MLL methyltransferases, and the nuclear PIWI/piRNA complex. Given the recent advent of ChIP-seq in planarians, we propose future avenues of research that will identify the genomic targets of these complexes allowing for a clearer picture of how neoblast processes are coordinated at the epigenetic level. These insights into neoblast biology may be directly relevant to mammalian stem cells and disease. The unique biology of planarians will also allow us to investigate how extracellular signals feed into epigenetic regulatory networks to govern concerted neoblast responses during regenerative polarity, tissue patterning, and remodelling.

摘要

涡虫拥有多能干细胞(成体干细胞),能够分化为构成成体身体结构的所有细胞类型。因此,涡虫具有显著的再生能力。转录组学研究表明,基因表达是协调一致的,以维持成体干细胞的多能性,并确保在分化过程中正确的谱系特化。但迄今为止,它们还没有揭示这种表达调控是如何控制的。在这篇综述中,我们提出涡虫代表了一个独特而有效的系统,可以在体内环境中研究这些过程的表观遗传调控。我们整合了一些证据,表明尽管 DNA 甲基化可能存在于某些扁形动物谱系中,但它并不调节 Schmidtea mediterranea 中的成体干细胞功能。许多表型研究记录了组蛋白修饰和染色质重塑复合物在调节不同成体干细胞过程中的作用,我们重点关注了四个重要的涡虫表观遗传调节剂:核小体重塑去乙酰化酶(NuRD)复合物、多梳抑制复合物(PRC)、SET1/MLL 甲基转移酶和核 PIWI/piRNA 复合物。鉴于最近在涡虫中出现了 ChIP-seq,我们提出了未来的研究途径,这些途径将确定这些复合物的基因组靶点,从而更清楚地了解成体干细胞过程如何在表观遗传水平上协调。这些对成体干细胞生物学的深入了解可能与哺乳动物干细胞和疾病直接相关。涡虫的独特生物学也将使我们能够研究细胞外信号如何进入表观遗传调控网络,以在再生极性、组织模式和重塑过程中协调成体干细胞的反应。

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