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Understanding the complexity of retina and pluripotent stem cell derived retinal organoids with single cell RNA sequencing: current progress, remaining challenges and future prospective

机译:了解视网膜和多能干细胞衍生视网膜器官的复杂性,用单细胞RNA测序:目前的进展,剩余挑战和未来的前瞻性

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摘要

Single-cell sequencing technologies have emerged as a revolutionary tool with transformative new methods to profile genetic, epigenetic, spatial, and lineage information in individual cells. Single-cell RNA sequencing (scRNA-Seq) allows researchers to collect large datasets detailing the transcriptomes of individual cells in space and time and is increasingly being applied to reveal cellular heterogeneity in retinal development, normal physiology, and disease, and provide new insights into cell-type specific markers and signaling pathways. In recent years, scRNA-Seq datasets have been generated from retinal tissue and pluripotent stem cell-derived retinal organoids. Their cross-comparison enables staging of retinal organoids, identification of specific cells in developing and adult human neural retina and provides deeper insights into cell-type sub-specification and geographical differences. In this article, we review the recent rapid progress in scRNA-Seq analyses of retina and retinal organoids, the questions that remain unanswered and the technical challenges that need to be overcome to achieve consistent results that reflect the complexity, functionality, and interactions of all retinal cell types.
机译:单细胞测序技术已成为具有转型性新方法的革命性工具,用于在单个细胞中概况遗传,表观遗传,空间和谱系信息。单细胞RNA测序(ScRNA-SEQ)允许研究人员收集细节在空间和时间中单个细胞的转录组的大型数据集,并且越来越多地应用于视网膜发育,正常生理学和疾病中的细胞异质性,并提供新的见解细胞类型特定标记和信号通路。近年来,ScRNA-SEQ数据集已从视网膜组织和多能干细胞衍生的视网膜器体产生。它们的交叉比较使视网膜有机体的分期,鉴定在开发和成人人类神经视网膜中的特异性细胞,并提供更深入的洞察细胞型子规范和地理差异。在本文中,我们审查了Retina和视网膜器有机体的Scrna-SEQ分析的最新进展情况,仍未得到答复的问题以及需要克服的技术挑战,以实现反映所有人的复杂性,功能和相互作用的一致结果视网膜细胞类型。

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