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诱导人多能干细胞分化为胚胎起源的特定血管平滑肌亚型。

Directed differentiation of embryonic origin-specific vascular smooth muscle subtypes from human pluripotent stem cells.

机构信息

Institute of Molecular and Cell Biology, Agency for Science, Technology and Research, Singapore.

The Anne McLaren Laboratory for Regenerative Medicine and Wellcome Trust-Medical Research Council Cambridge Stem Cell Institute, University of Cambridge, Cambridge, UK.

出版信息

Nat Protoc. 2014 Apr;9(4):929-38. doi: 10.1038/nprot.2014.059. Epub 2014 Mar 27.

Abstract

Vascular smooth muscle cells (SMCs) arise from diverse developmental origins. Regional distribution of vascular diseases may, in part, be attributed to this inherent heterogeneity in SMC lineage. Therefore, systems for generating human SMC subtypes of distinct embryonic origins would represent useful platforms for studying the influence of SMC lineage on the spatial specificity of vascular disease. Here we describe how human pluripotent stem cells can be differentiated into distinct populations of SMC subtypes under chemically defined conditions. The initial stage (days 0-5 or 0-7) begins with the induction of three intermediate lineages: neuroectoderm, lateral plate mesoderm and paraxial mesoderm. Subsequently, these precursor lineages are differentiated into contractile SMCs (days 5-19+). At key stages, the emergence of lineage-specific markers confirms recapitulation of embryonic developmental pathways and generation of functionally distinct SMC subtypes. The ability to derive an unlimited supply of human SMCs will accelerate applications in regenerative medicine and disease modeling.

摘要

血管平滑肌细胞(SMCs)起源于不同的发育来源。血管疾病的区域分布可能部分归因于 SMC 谱系的这种固有异质性。因此,生成具有不同胚胎起源的人类 SMC 亚型的系统将代表用于研究 SMC 谱系对血管疾病空间特异性影响的有用平台。在这里,我们描述了如何在化学定义条件下将人类多能干细胞分化为不同的 SMC 亚型群体。初始阶段(第 0-5 天或 0-7 天)始于诱导三个中间谱系:神经外胚层、侧板中胚层和轴旁中胚层。随后,这些前体细胞系分化为收缩型 SMC(第 5-19+天)。在关键阶段,谱系特异性标志物的出现证实了胚胎发育途径的再现和功能不同的 SMC 亚型的产生。获得无限供应的人类 SMC 的能力将加速再生医学和疾病建模中的应用。

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