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人类诱导多能干细胞(iPSC)系的建立和多能性的机制:历史视角和最新进展。

Derivation of Human Induced Pluripotent Stem Cell (iPSC) Lines and Mechanism of Pluripotency: Historical Perspective and Recent Advances.

机构信息

Department of Medicine, University of Connecticut Health Center (UConn Health), Farmington, CT, 06030, USA.

出版信息

Stem Cell Rev Rep. 2017 Dec;13(6):757-773. doi: 10.1007/s12015-017-9766-9.

Abstract

Derivation of human embryonic stem cell (hES) lines in 1998 was not only a major technological breakthrough in the field of regenerative medicine; it also triggered a passionate debate about the ethical issues associated with the utilization of human embryos for derivation of hESC lines. Successful derivation of induced pluripotent stem cell (iPS) lines from human somatic cells with defined reprogramming factors by Shinya Yamanaka`s group in 2007 was another breakthrough that generated enormous excitement and hope for the development of donor-specific personalized cell replacement therapies (CRT) without the ethical dilemma associated with it. As we approach twentieth anniversary of derivation of hESC lines and the tenth anniversary of isolation of donor-specific iPSC lines, this manuscript summarizes the key advances in pluripotent stem cell (PSC) research field that led to derivation of human iPSC lines, different methodologies for derivation iPSC lines and characterization of the mechanism of reprogramming. We will also review progress towards generating donor-specific somatic cell lineages from iPSC lines, especially the functional immune cell lineages, and progress towards advancing these findings to the clinic. Finally, we will discuss the challenges, such as genome instability and inherent immunogenicity of hPSC lines that need to be addressed to develop safe and effective iPSC-based CRT.

摘要

人胚胎干细胞(hESC)系于 1998 年的成功建立不仅是再生医学领域的重大技术突破,也引发了关于利用人类胚胎建立 hESC 系的相关伦理问题的激烈争论。2007 年,Shinya Yamanaka 小组利用定义明确的重编程因子成功地从人体细胞中诱导出多能干细胞(iPS)系,这是另一个突破,为开发供体特异性的个性化细胞替代疗法(CRT)带来了巨大的兴奋和希望,而不会带来与之相关的伦理困境。随着我们接近 hESC 系建立二十周年和供体特异性 iPSC 系建立十周年,本文总结了多能干细胞(PSC)研究领域的关键进展,这些进展导致了人类 iPSC 系的建立、不同的 iPSC 系建立方法以及重编程机制的特征。我们还将回顾从 iPSC 系生成供体特异性体细胞谱系的进展,特别是功能性免疫细胞谱系,以及将这些发现推进到临床应用的进展。最后,我们将讨论一些挑战,如 hPSC 系的基因组不稳定性和固有免疫原性,这些问题需要解决,以开发安全有效的基于 iPSC 的 CRT。

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