论文信息 - Direct Reprogramming of Human Fibroblasts toward a Cardiomyocyte-like State

Direct Reprogramming of Human Fibroblasts toward a Cardiomyocyte-like State

Summary Direct reprogramming of adult somatic cells into alternative cell types has been shown for several lineages. We previously showed that GATA4, MEF2C, and TBX5 (GMT) directly reprogrammed nonmyocyte mouse heart cells into induced cardiomyocyte-like cells (iCMs) in vitro and in vivo. However, GMT alone appears insufficient in human fibroblasts, at least in vitro. Here, we show that GMT plus ESRRG and MESP1 induced global cardiac gene-expression and phenotypic shifts in human fibroblasts derived from embryonic stem cells, fetal heart, and neonatal skin. Adding Myocardin and ZFPM2 enhanced reprogramming, including sarcomere formation, calcium transients, and action potentials, although the efficiency remained low. Human iCM reprogramming was epigenetically stable. Furthermore, we found that transforming growth factor β signaling was important for, and improved the efficiency of, human iCM reprogramming. These findings demonstrate that human fibroblasts can be directly reprogrammed toward the cardiac lineage, and lay the foundation for future refinements in vitro and in vivo.

[1] A. McCulloch,et al. Lentiviral Vectors and Protocols for Creation of Stable hESC Lines for Fluorescent Tracking and Drug Resistance Selection of Cardiomyocytes , 2009, PloS one.

[2] Shinsuke Yuasa,et al. Induction of human cardiomyocyte-like cells from fibroblasts by defined factors , 2013, Proceedings of the National Academy of Sciences.

[3] M. Blanchette,et al. Genome-wide Orchestration of Cardiac Functions by the Orphan Nuclear Receptors ERRα and γ , 2007 .

[4] V. Vedantham,et al. Direct Reprogramming of Fibroblasts into Functional Cardiomyocytes by Defined Factors , 2010, Cell.

[5] Jonathan C. Cohen,et al. GATA4 mutations cause human congenital heart defects and reveal an interaction with TBX5 , 2003, Nature.

[6] E. Svensson,et al. A syndrome of tricuspid atresia in mice with a targeted mutation of the gene encoding Fog-2 , 2000, Nature Genetics.

[7] Gordon K Smyth,et al. Linear Models and Empirical Bayes Methods for Assessing Differential Expression in Microarray Experiments , 2004, Statistical applications in genetics and molecular biology.

[8] Xiaoxia Qi,et al. Heart repair by reprogramming non-myocytes with cardiac transcription factors , 2012, Nature.

[9] D. Srivastava,et al. Cardiac fibroblasts regulate myocardial proliferation through beta1 integrin signaling. , 2009, Developmental cell.

[10] E. A. Packham,et al. Physical Interaction between TBX5 and MEF2C Is Required for Early Heart Development , 2009, Molecular and Cellular Biology.

[11] Jian Li,et al. Myocardin is required for cardiomyocyte survival and maintenance of heart function , 2009, Proceedings of the National Academy of Sciences.

[12] J. Thomson,et al. Embryonic stem cell lines derived from human blastocysts. , 1998, Science.

[13] H. Weintraub,et al. Expression of a single transfected cDNA converts fibroblasts to myoblasts , 1987, Cell.

[14] R. Jaenisch,et al. A drug-inducible system for direct reprogramming of human somatic cells to pluripotency. , 2008, Cell stem cell.

[15] Michael Kyba,et al. Mesp1 acts as a master regulator of multipotent cardiovascular progenitor specification. , 2008, Cell stem cell.

[16] M. Jinnin,et al. Characterization of SIS3, a Novel Specific Inhibitor of Smad3, and Its Effect on Transforming Growth Factor-β1-Induced Extracellular Matrix Expression , 2006, Molecular Pharmacology.

[17] E. Finch,et al. MicroRNA-Mediated In Vitro and In Vivo Direct Reprogramming of Cardiac Fibroblasts to Cardiomyocytes , 2012, Circulation research.

[18] R. Rosenfeld. Nature , 2009, Otolaryngology--head and neck surgery : official journal of American Academy of Otolaryngology-Head and Neck Surgery.

[19] S. Orkin,et al. FOG-2, a Cofactor for GATA Transcription Factors, Is Essential for Heart Morphogenesis and Development of Coronary Vessels from Epicardium , 2000, Cell.

[20] R. Schwartz,et al. Transcription factors ETS2 and MESP1 transdifferentiate human dermal fibroblasts into cardiac progenitors , 2012, Proceedings of the National Academy of Sciences.

[21] Wenjun Guo,et al. Induction of pluripotent stem cells by defined factors is greatly improved by small-molecule compounds , 2008, Nature Biotechnology.

[22] Sheng Ding,et al. A chemical platform for improved induction of human iPSCs , 2009, Nature Methods.

[23] Mathieu Blanchette,et al. Genome-wide orchestration of cardiac functions by the orphan nuclear receptors ERRalpha and gamma. , 2007, Cell metabolism.

[24] S Nattel,et al. Delayed rectifier outward current and repolarization in human atrial myocytes. , 1993, Circulation research.

[25] A. B. Lyons,et al. Flow cytometric analysis of cell division history using dilution of carboxyfluorescein diacetate succinimidyl ester, a stably integrated fluorescent probe. , 2001, Methods in cell biology.

[26] Da-Zhi Wang,et al. Activation of Cardiac Gene Expression by Myocardin, a Transcriptional Cofactor for Serum Response Factor , 2001, Cell.

[27] Jeffrey W. Streb,et al. Myocardin: a component of a molecular switch for smooth muscle differentiation. , 2002, Journal of molecular and cellular cardiology.

[28] D. Lindemann,et al. A new approach to transcription factor screening for reprogramming of fibroblasts to cardiomyocyte-like cells. , 2012, Journal of molecular and cellular cardiology.

[29] Thomas Vierbuchen,et al. Direct conversion of fibroblasts to functional neurons by defined factors , 2010, Nature.

[30] P. Couture,et al. Thy-1 expression by cardiac fibroblasts: lack of association with myofibroblast contractile markers. , 2007, Journal of molecular and cellular cardiology.