Modeling X chromosome inactivation using t5iLA naive human pluripotent stem cells

IF 4.4 1区 生物学 Q1 BIOLOGY BMC Biology Pub Date : 2024-09-18 DOI:10.1186/s12915-024-01994-y
Yudan Shang, Nannan Wang, Haoyi Wang, Chenrui An, Wen Sun
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Abstract

X chromosome inactivation (XCI) is a critical epigenetic event for dosage compensation of X-linked genes in female mammals, ensuring developmental stability. A robust in vitro model is required for mimicking XCI during the early stages of embryonic development. This methodology article introduces an advanced framework for the in-depth study of XCI using human pluripotent stem cells (hPSCs). By focusing on the transition between naive and primed pluripotent states, we highlight the role of long non-coding RNA X-inactive specific transcript (XIST) and epigenetic alterations in mediating XCI. Our methodology enables the distinction between naive and primed hESCs based on XIST expression and the activity of X-linked reporters, facilitating the investigation of XCI initiation and maintenance. Through detailed experimental procedures, we demonstrate the utility of our hESC lines in modeling the process of human XCI, including the establishment of conditions for random XCI induction and the analysis of X chromosome reactivation. The study outlines a comprehensive approach for characterizing the X chromosome status in hPSCs, employing dual fluorescent reporter hESC lines. These reporter lines enable real-time tracking of XCI dynamics through differentiation processes. We detailed protocols for the induction of X chromosome reactivation and inactivation, as well as the X status characterization methods including cultivation of hESCs, flow cytometric analysis, RNA fluorescence in situ hybridization (FISH), and transcriptome sequencing, providing a step-by-step guide for researchers to investigate XCI mechanisms in vitro. This article provides a detailed, reproducible methodology for studying XCI mechanisms in vitro, employing hPSCs as a model system. It presents a significant advance in our ability to investigate XCI, offering potential applications in developmental biology, disease modeling, and regenerative medicine. By facilitating the study of XCI dynamics, this methodological framework paves the way for deeper understanding and manipulation of this fundamental biological process.
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利用 t5iLA 天真的人类多能干细胞模拟 X 染色体失活
X 染色体失活(XCI)是雌性哺乳动物 X 连锁基因剂量补偿的关键表观遗传事件,可确保发育的稳定性。在胚胎发育的早期阶段,需要一个强大的体外模型来模拟 XCI。这篇方法论文章介绍了利用人体多能干细胞(hPSCs)深入研究 XCI 的先进框架。通过关注天真多能状态和原始多能状态之间的过渡,我们强调了长非编码 RNA X-非活性特异性转录本(XIST)和表观遗传学改变在介导 XCI 中的作用。我们的方法能够根据 XIST 的表达和 X 连锁报告因子的活性来区分幼稚和激活的 hESC,从而促进对 XCI 启动和维持的研究。通过详细的实验过程,我们证明了我们的 hESC 株系在模拟人类 XCI 过程中的实用性,包括建立随机 XCI 诱导条件和分析 X 染色体再活化。该研究采用双荧光报告基因 hESC 株系,概述了表征 hPSC 中 X 染色体状态的综合方法。这些报告基因可通过分化过程实时跟踪 XCI 动态。我们详细介绍了诱导 X 染色体再激活和失活的方案,以及 X 状态表征方法,包括培养 hESCs、流式细胞分析、RNA 荧光原位杂交(FISH)和转录组测序,为研究人员研究体外 XCI 机制提供了逐步指导。本文以 hPSCs 为模型系统,为体外研究 XCI 机制提供了详细、可重复的方法。它大大提高了我们研究 XCI 的能力,为发育生物学、疾病建模和再生医学提供了潜在的应用前景。通过促进 XCI 动态研究,该方法框架为深入了解和操纵这一基本生物过程铺平了道路。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
BMC Biology
BMC Biology 生物-生物学
CiteScore
7.80
自引率
1.90%
发文量
260
审稿时长
3 months
期刊介绍: BMC Biology is a broad scope journal covering all areas of biology. Our content includes research articles, new methods and tools. BMC Biology also publishes reviews, Q&A, and commentaries.
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