Department of Organismic and Evolutionary Biology, Museum of Comparative Zoology, Harvard University, Cambridge, MA, 02138, USA.
Biodiversity Research Center, Academia Sinica, Taipei, Taiwan.
Nat Commun. 2023 May 5;14(1):2612. doi: 10.1038/s41467-023-38016-4.
Adult pluripotent stem cell (aPSC) populations underlie whole-body regeneration in many distantly-related animal lineages, but how the underlying cellular and molecular mechanisms compare across species is unknown. Here, we apply single-cell RNA sequencing to profile transcriptional cell states of the acoel worm Hofstenia miamia during postembryonic development and regeneration. We identify cell types shared across stages and their associated gene expression dynamics during regeneration. Functional studies confirm that the aPSCs, also known as neoblasts, are the source of differentiated cells and reveal transcription factors needed for differentiation. Subclustering of neoblasts recovers transcriptionally distinct subpopulations, the majority of which are likely specialized to differentiated lineages. One neoblast subset, showing enriched expression of the histone variant H3.3, appears to lack specialization. Altogether, the cell states identified in this study facilitate comparisons to other species and enable future studies of stem cell fate potentials.
成体多能干细胞(aPSC)是许多亲缘关系较远的动物谱系全身再生的基础,但不同物种之间潜在的细胞和分子机制如何比较尚不清楚。在这里,我们应用单细胞 RNA 测序来描绘后生动物 Hofstenia miamia 在胚胎后发育和再生过程中的转录细胞状态。我们确定了在再生过程中共享的细胞类型及其相关的基因表达动态。功能研究证实,也被称为成体干细胞的 aPSC 是分化细胞的来源,并揭示了分化所需的转录因子。成体干细胞的亚群聚类恢复了转录上不同的亚群,其中大多数可能专门针对分化谱系。一个成体干细胞亚群,表现出组蛋白变体 H3.3 的富集表达,似乎缺乏专业化。总的来说,本研究中确定的细胞状态有助于与其他物种进行比较,并为未来的干细胞命运潜力研究提供便利。
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