Disruption of Apical-Basal Polarity of Human Embryonic Stem Cells Enhances Hematoendothelial Differentiation

doi:10.1634/stemcells.2007-0230

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First published online June 14, 2007
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Submitted on March 28, 2007
Accepted on June 7, 2007

EMBRYONIC STEM CELLS

Disruption of Apical-Basal Polarity of Human Embryonic Stem Cells Enhances Hematoendothelial Differentiation

Ana Krtolica ¹, Olga Genbacev ², Carmen Escobedo ³, Tamara Zdravkovic ², Adam Nordstrom ², Diana Vabuena ³, Aneel Nath ², Carlos Simon ³, Keith Mostov ⁴, Susan J. Fisher ⁵^*

¹ Lawrence Berkeley National Laboratory, Berkeley, California
² Departments of Cell and Tissue Biology, University of California San Francisco, San Francisco, California
³ Stem Cell Bank, Prince Felipe Research Center and IVI Foundation, University of Valencia, Valencia, Spain
⁴ Anatomy, University of California San Francisco, San Francisco, California
⁵ Departments of Cell and Tissue Biology, Anatomy, and Pharmaceutical Chemistry, University of California San Francisco, San Francisco, California

^* To whom correspondence should be addressed. E-mail: sfisher{at}cgl.ucsf.edu.

Abstract

During murine development, the formation of tight junctionsand acquisition of polarity is associated with allocation ofthe blastomeres on the outer surface of the embryo to the trophoblastlineage, whereas the absence of polarization directs cells tothe inner cell mass (ICM). Here we report the results of ultrastructuralanalyses that suggest a similar link between polarization andcell fate in human embryos. In contrast, the five human embryonicstem cell (hESC) lines displayed apical-basal, epithelial-typepolarity, with electron-dense tight junctions, apical microvilli,and asymmetric distribution of organelles. Consistent with thesefindings, molecules that are components of tight junctions orplay regulatory roles in polarization localized to the apicalregions of the hESCs at sites of cell-cell contact. The tightjunctions were functional, as shown by the ability of hESC coloniesto exclude the pericellular passage of a biotin compound. Depolarizationof hESCs produced multilayered aggregates of rapidly proliferatingcells that continued to express transcription factors that arerequired for pluripotency at the same level as control cells.However, during embryoid body formation, depolarized cells differentiatedpredominantly along mesenchymal lineage and spontaneously producedhematoendothelial precursors more efficiently than control ESC.Our findings have numerous implications with regard to strategiesfor deriving, propagating and differentiating hESC.

Key Words. human embryonic stem cells, inner cell mass, apical-basal polarity, embryoid body formation, hematoendothelial differentiation

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