Seok Hyung Kim scite author profile

FLK1-expressing (FLK1(+)) mesoderm generates blood and vessels. Here, we show that combined BMP, Notch, and Wnt signaling is necessary for efficient FLK1(+) mesoderm formation from embryonic stem cells (ESCs). Inhibition of BMP, Notch, and Wnt signaling pathways greatly decreased the generation of FLK1(+) mesoderm and expression of the Ets transcription factor Er71. Enforced expression of ER71 in ESCs resulted in a robust induction of FLK1(+) mesoderm; rescued the generation of FLK1(+) mesoderm when blocked by BMP, Notch, and Wnt inhibition; and enhanced hematopoietic and endothelial cell generation. Er71-deficient mice had greatly reduced FLK1 expression, died early in gestation, and displayed severe blood and vessel defects that are highly reminiscent of the Flk1 null mouse phenotype. Collectively, we provide compelling evidence that ER71 functions downstream of BMP, Notch, and Wnt signals and regulates FLK1(+) mesoderm, blood, and vessel development.

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Zebrafish TRPA1 Channels Are Required for Chemosensation But Not for Thermosensation or Mechanosensory Hair Cell Function

Prober¹,

Zimmerman²,

Myers³

et al. 2008

J. Neurosci.

164

157

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Cyclooxygenase-1-derived PGE₂ promotes cell motility via the G-protein-coupled EP4 receptor during vertebrate gastrulation

Yong¹,

Kim²,

Sepich³

et al. 2006

Genes Dev.

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Gastrulation is a fundamental process during embryogenesis that shapes proper body architecture and establishes three germ layers through coordinated cellular actions of proliferation, fate specification, and movement. Although many molecular pathways involved in the specification of cell fate and polarity during vertebrate gastrulation have been identified, little is known of the signaling that imparts cell motility. Here we show that prostaglandin E 2 (PGE 2 ) production by microsomal PGE 2 synthase (Ptges) is essential for gastrulation movements in zebrafish. Furthermore, PGE 2 signaling regulates morphogenetic movements of convergence and extension as well as epiboly through the G-protein-coupled PGE 2 receptor (EP4) via phosphatidylinositol 3-kinase (PI3K)/Akt. EP4 signaling is not required for proper cell shape or persistence of migration, but rather it promotes optimal cell migration speed during gastrulation. This work demonstrates a critical requirement of PGE 2 signaling in promoting cell motility through the COX-1-Ptges-EP4 pathway, a previously unrecognized role for this biologically active lipid in early animal development.[Keywords: Cancer; cell motility; cyclooxygenase; development; prostaglandin; zebrafish] Supplemental material is available at http://www.genesdev.org.

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Seok Hyung Kim

Lineage-dependent gene expression programs influence the immune landscape of colorectal cancer

ER71 Acts Downstream of BMP, Notch, and Wnt Signaling in Blood and Vessel Progenitor Specification

Zebrafish TRPA1 Channels Are Required for Chemosensation But Not for Thermosensation or Mechanosensory Hair Cell Function

Cyclooxygenase-1-derived PGE₂ promotes cell motility via the G-protein-coupled EP4 receptor during vertebrate gastrulation

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Seok Hyung Kim

Lineage-dependent gene expression programs influence the immune landscape of colorectal cancer

ER71 Acts Downstream of BMP, Notch, and Wnt Signaling in Blood and Vessel Progenitor Specification

Zebrafish TRPA1 Channels Are Required for Chemosensation But Not for Thermosensation or Mechanosensory Hair Cell Function

Cyclooxygenase-1-derived PGE2 promotes cell motility via the G-protein-coupled EP4 receptor during vertebrate gastrulation

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Cyclooxygenase-1-derived PGE₂ promotes cell motility via the G-protein-coupled EP4 receptor during vertebrate gastrulation