TGF-beta1 enhances cardiomyogenic differentiation of skeletal muscle-derived adult primitive cells

TGF-β1增强骨骼肌来源的成体原始细胞向心肌细胞分化。

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作者：Abdel-Latif,Ahmed,Zuba-Surma,Ewa K,Case,Jamie,Tiwari,Sumit,Hunt,Greg,Ranjan,Smita,Vincent,Robert J,Srour,Edward F,Bolli,Roberto,Dawn,Buddhadeb

期刊：	Basic Research in Cardiology	影响因子：	8.000
时间：	2008	起止号：	2008 Nov;103(6):514-24
doi：	10.1007/s00395-008-0729-9	靶点：	TGF-β1
研究方向：	细胞生物学

Abstract

The optimal medium for cardiac differentiation of adult primitive cells remains to be established. We quantitatively compared the efficacy of IGF-1, dynorphin B, insulin, oxytocin, bFGF, and TGF-beta1 in inducing cardiomyogenic differentiation. Adult mouse skeletal muscle-derived Sca1+/CD45-/c-kit-/Thy-1+ (SM+) and Sca1-/CD45-/c-kit-/Thy-1+ (SM-) cells were cultured in basic medium (BM; DMEM, FBS, IGF-1, dynorphin B) alone and BM supplemented with insulin, oxytocin, bFGF, or TGF-beta1. Cardiac differentiation was evaluated by the expression of cardiac-specific markers at the mRNA (qRT-PCR) and protein (immunocytochemistry) levels. BM+TGF-beta1 upregulated mRNA expression of Nkx2.5 and GATA-4 after 4 days and Myl2 after 9 days. After 30 days, BM+TGF-beta1 induced the greatest extent of cardiac differentiation (by morphology and expression of cardiac markers) in SM- cells. We conclude that TGF-beta1 enhances cardiomyogenic differentiation in skeletal muscle-derived adult primitive cells. This strategy may be utilized to induce cardiac differentiation as well as to examine the cardiomyogenic potential of adult tissue-derived stem/progenitor cells.

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