Literature DB >> 19910576

The cellular prion protein identifies bipotential cardiomyogenic progenitors.

Kyoko Hidaka1, Manabu Shirai, Jong-Kook Lee, Takanari Wakayama, Itsuo Kodama, Michael D Schneider, Takayuki Morisaki.   

Abstract

RATIONALE: The paucity of specific surface markers for cardiomyocytes and their progenitors has impeded the development of embryonic or pluripotent stem cell-based transplantation therapy. Identification of relevant surface markers may also enhance our understanding of the mechanisms underlying differentiation.
OBJECTIVE: Here, we show that cellular prion protein (PrP) serves as an effective surface marker for isolating nascent cardiomyocytes as well as cardiomyogenic progenitors. METHODS AND
RESULTS: Embryonic stem (or embryo-derived) cells were analyzed using flow cytometry to detect surface expression of PrP and intracellular myosin heavy chain (Myhc) proteins. Sorted cells were then analyzed for their differentiation potential.
CONCLUSIONS: PrP+ cells from beating embryoid bodies (EBs) frequently included nascent Myhc+ cardiomyocytes. Cultured PrP+ cells further differentiated, giving rise to cardiac troponin I+ definitive cardiomyocytes with either an atrial or a ventricular identity. These cells were electrophysiologically functional and able to survive in vivo after transplantation. Combining PrP with a second marker, platelet-derived growth factor receptor (PDGFR)alpha, enabled us to identify an earlier cardiomyogenic population from prebeating EBs, the PrP+PDGFRalpha+ (PRa) cells. The Myhc- PRa cells expressed cardiac transcription factors, such as Nkx2.5, T-box transcription factor 5, and Isl1 (islet LIM homeobox 1), although they were not completely committed. In mouse embryos, PRa cells in cardiac crescent at the 1 to 2 somite stage were Myhc+, whereas they were Myhc- at headfold stages. PRa cells clonally expanded in methlycellulose cultures. Furthermore, single Myhc- PRa cell-derived colonies contained both cardiac and smooth muscle cells. Thus, PrP demarcates a population of bipotential cardiomyogenic progenitor cells that can differentiate into cardiac or smooth muscle cells.

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Year:  2009        PMID: 19910576     DOI: 10.1161/CIRCRESAHA.109.209478

Source DB:  PubMed          Journal:  Circ Res        ISSN: 0009-7330            Impact factor:   17.367


  15 in total

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Review 3.  Embryonic template-based generation and purification of pluripotent stem cell-derived cardiomyocytes for heart repair.

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4.  Prion Protein and Stage Specific Embryo Antigen 1 as Selection Markers to Enrich the Fraction of Murine Embryonic Stem Cell-Derived Cardiomyocytes.

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9.  Human neonatal cardiovascular progenitors: unlocking the secret to regenerative ability.

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Review 10.  PrP(C) from stem cells to cancer.

Authors:  Séverine Martin-Lannerée; Théo Z Hirsch; Julia Hernandez-Rapp; Sophie Halliez; Jean-Luc Vilotte; Jean-Marie Launay; Sophie Mouillet-Richard
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