Review |
From the National Institutes of Health (K.R.B., D.T., H.-T.Y., S.V.A.), National Institute on Aging, Baltimore, Md, and the Institute of Plant Genetics (J.C., A.M.W.), Gatersleben, Germany. Dr Yang is now at the Health Science Center, Shanghai Institutes of Biological Sciences, Chinese Academy of Sciences and Shanghai Second Medical University, Shanghai, China.
Correspondence to Kenneth R. Boheler, PhD, Laboratory of Cardiovascular Science, Gerontology Research Center, NIH, NIA, 5600 Nathan Shock Dr, Baltimore, MD 21224. E-mail bohelerk{at}grc.nia.nih.gov
Embryonic stem (ES) cells have been established as permanent lines of undifferentiated pluripotent cells from early mouse embryos. ES cells provide a unique system for the genetic manipulation and the creation of knockout strains of mice through gene targeting. By cultivation in vitro as 3D aggregates called embryoid bodies, ES cells can differentiate into derivatives of all 3 primary germ layers, including cardiomyocytes. Protocols for the in vitro differentiation of ES cells into cardiomyocytes representing all specialized cell types of the heart, such as atrial-like, ventricular-like, sinus nodallike, and Purkinje-like cells, have been established. During differentiation, cardiac-specific genes as well as proteins, receptors, and ion channels are expressed in a developmental continuum, which closely recapitulates the developmental pattern of early cardiogenesis. Exploitation of ES cellderived cardiomyocytes has facilitated the analysis of early cardiac development and has permitted in vitro "gain-of-function" or "loss-of-function" genetic studies. Recently, human ES cell lines have been established that can be used to investigate cardiac development and the function of human heart cells and to determine the basic strategies of regenerative cell therapy. This review summarizes the current state of ES cellderived cardiogenesis and provides an overview of how genomic strategies coupled with this in vitro differentiation system can be applied to cardiac research.
Key Words: embryonic stem embryonic carcinoma embryonic germ in vitro differentiation cardiomyocytes
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