Stem Cell Research (Jul 2014)

SIRPA, VCAM1 and CD34 identify discrete lineages during early human cardiovascular development

  • Rhys J.P. Skelton,
  • Magdaline Costa,
  • David J. Anderson,
  • Freya Bruveris,
  • Ben W. Finnin,
  • Katerina Koutsis,
  • Deevina Arasaratnam,
  • Anthony J. White,
  • Arash Rafii,
  • Elizabeth S. Ng,
  • Andrew G. Elefanty,
  • Edouard G. Stanley,
  • Colin W. Pouton,
  • John M. Haynes,
  • Reza Ardehali,
  • Richard P. Davis,
  • Christine L. Mummery,
  • David A. Elliott

DOI
https://doi.org/10.1016/j.scr.2014.04.016
Journal volume & issue
Vol. 13, no. 1
pp. 172 – 179

Abstract

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The study of human cardiogenesis would benefit from a detailed cell lineage fate map akin to that established for the haematopoietic lineages. Here we sought to define cell lineage relationships based on the expression of NKX2-5 and the cell surface markers VCAM1, SIRPA and CD34 during human cardiovascular development. Expression of NKX2-5GFP was used to identify cardiac progenitors and cardiomyocytes generated during the differentiation of NKX2-5GFP/w human embryonic stem cells (hESCs). Cardiovascular cell lineages sub-fractionated on the basis of SIRPA, VCAM1 and CD34 expression were assayed for differentiation potential and gene expression. The NKX2-5posCD34pos population gave rise to endothelial cells that rapidly lost NKX2-5 expression in culture. Conversely, NKX2-5 expression was maintained in myocardial committed cells, which progressed from being NKX2-5posSIRPApos to NKX2-5posSIRPAposVCAM1pos. Up-regulation of VCAM1 was accompanied by the expression of myofilament markers and reduced clonal capacity, implying a restriction of cell fate potential. Combinatorial expression of NKX2-5, SIRPA, VCAM1 and CD34 can be used to define discrete stages of cardiovascular cell lineage differentiation. These markers identify specific stages of cardiomyocyte and endothelial lineage commitment and, thus provide a scaffold for establishing a fate map of early human cardiogenesis.