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多能胚胎isl1+祖细胞可导致心脏、平滑肌和内皮细胞多样化。

Multipotent embryonic isl1+ progenitor cells lead to cardiac, smooth muscle, and endothelial cell diversification.

作者信息

Moretti Alessandra, Caron Leslie, Nakano Atsushi, Lam Jason T, Bernshausen Alexandra, Chen Yinhong, Qyang Yibing, Bu Lei, Sasaki Mika, Martin-Puig Silvia, Sun Yunfu, Evans Sylvia M, Laugwitz Karl-Ludwig, Chien Kenneth R

机构信息

Massachusetts General Hospital - Cardiovascular Research Center, Charles River Plaza/CPZN 3208, 185 Cambridge Street, Boston, MA 02114, USA.

出版信息

Cell. 2006 Dec 15;127(6):1151-65. doi: 10.1016/j.cell.2006.10.029. Epub 2006 Nov 22.


DOI:10.1016/j.cell.2006.10.029
PMID:17123592
Abstract

Cardiogenesis requires the generation of endothelial, cardiac, and smooth muscle cells, thought to arise from distinct embryonic precursors. We use genetic fate-mapping studies to document that isl1(+) precursors from the second heart field can generate each of these diverse cardiovascular cell types in vivo. Utilizing embryonic stem (ES) cells, we clonally amplified a cellular hierarchy of isl1(+) cardiovascular progenitors, which resemble the developmental precursors in the embryonic heart. The transcriptional signature of isl1(+)/Nkx2.5(+)/flk1(+) defines a multipotent cardiovascular progenitor, which can give rise to cells of all three lineages. These studies document a developmental paradigm for cardiogenesis, where muscle and endothelial lineage diversification arises from a single cell-level decision of a multipotent isl1(+) cardiovascular progenitor cell (MICP). The discovery of ES cell-derived MICPs suggests a strategy for cardiovascular tissue regeneration via their isolation, renewal, and directed differentiation into specific mature cardiac, pacemaker, smooth muscle, and endothelial cell types.

摘要

心脏发生需要生成内皮细胞、心肌细胞和平滑肌细胞,这些细胞被认为起源于不同的胚胎前体细胞。我们利用基因命运图谱研究来证明,来自第二心脏区域的isl1(+)前体细胞能够在体内生成这些不同类型的心血管细胞。利用胚胎干细胞,我们克隆扩增了isl1(+)心血管祖细胞的细胞谱系,这些祖细胞类似于胚胎心脏中的发育前体细胞。isl1(+)/Nkx2.5(+)/flk1(+)的转录特征定义了一种多能心血管祖细胞,它可以产生所有三个谱系的细胞。这些研究记录了心脏发生的一种发育模式,即肌肉和内皮谱系的分化源于多能isl1(+)心血管祖细胞(MICP)在单细胞水平上的决定。胚胎干细胞衍生的MICP的发现提示了一种通过分离、更新并将其定向分化为特定成熟的心肌、起搏、平滑肌和内皮细胞类型来进行心血管组织再生的策略。

相似文献

[1]
Multipotent embryonic isl1+ progenitor cells lead to cardiac, smooth muscle, and endothelial cell diversification.

Cell. 2006-12-15

[2]
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[4]
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[5]
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[6]
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[7]
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[8]
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[10]
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