Endothelin-1 supports clonal derivation and expansion of cardiovascular progenitors derived from human embryonic stem cells

Boon Seng Soh; Shi Yan Ng; Hao Wu; Kristina Buac; Joo Hye C. Park; Xiaojun Lian; Jiejia Xu; Kylie S. Foo; Ulrika Felldin; Xiaobing He; Massimo Nichane; Henry Yang; Lei Bu; Ronald A. Li; Bing Lim; Kenneth R. Chien

doi:10.1038/ncomms10774

Endothelin-1 supports clonal derivation and expansion of cardiovascular progenitors derived from human embryonic stem cells

Boon Seng Soh, Shi Yan Ng, Hao Wu, Kristina Buac, Joo Hye C. Park, Xiaojun Lian, Jiejia Xu, Kylie S. Foo, Ulrika Felldin, Xiaobing He, Massimo Nichane, Henry Yang, Lei Bu, Ronald A. Li, Bing Lim, Kenneth R. Chien

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18 Scopus citations

Abstract

Coronary arteriogenesis is a central step in cardiogenesis, requiring coordinated generation and integration of endothelial cell and vascular smooth muscle cells. At present, it is unclear whether the cell fate programme of cardiac progenitors to generate complex muscular or vascular structures is entirely cell autonomous. Here we demonstrate the intrinsic ability of vascular progenitors to develop and self-organize into cardiac tissues by clonally isolating and expanding second heart field cardiovascular progenitors using WNT3A and endothelin-1 (EDN1) human recombinant proteins. Progenitor clones undergo long-term expansion and differentiate primarily into endothelial and smooth muscle cell lineages in vitro, and contribute extensively to coronary-like vessels in vivo, forming a functional human-mouse chimeric circulatory system. Our study identifies EDN1 as a key factor towards the generation and clonal derivation of ISL1⁺ vascular intermediates, and demonstrates the intrinsic cell-autonomous nature of these progenitors to differentiate and self-organize into functional vasculatures in vivo.

Original language	English (US)
Article number	10774
Journal	Nature communications
Volume	7
DOIs	https://doi.org/10.1038/ncomms10774
State	Published - Mar 8 2016

All Science Journal Classification (ASJC) codes

Chemistry(all)
Biochemistry, Genetics and Molecular Biology(all)
Physics and Astronomy(all)

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Soh, B. S., Ng, S. Y., Wu, H., Buac, K., Park, J. H. C., Lian, X., Xu, J., Foo, K. S., Felldin, U., He, X., Nichane, M., Yang, H., Bu, L., Li, R. A., Lim, B., & Chien, K. R. (2016). Endothelin-1 supports clonal derivation and expansion of cardiovascular progenitors derived from human embryonic stem cells. Nature communications, 7, Article 10774. https://doi.org/10.1038/ncomms10774

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title = "Endothelin-1 supports clonal derivation and expansion of cardiovascular progenitors derived from human embryonic stem cells",

abstract = "Coronary arteriogenesis is a central step in cardiogenesis, requiring coordinated generation and integration of endothelial cell and vascular smooth muscle cells. At present, it is unclear whether the cell fate programme of cardiac progenitors to generate complex muscular or vascular structures is entirely cell autonomous. Here we demonstrate the intrinsic ability of vascular progenitors to develop and self-organize into cardiac tissues by clonally isolating and expanding second heart field cardiovascular progenitors using WNT3A and endothelin-1 (EDN1) human recombinant proteins. Progenitor clones undergo long-term expansion and differentiate primarily into endothelial and smooth muscle cell lineages in vitro, and contribute extensively to coronary-like vessels in vivo, forming a functional human-mouse chimeric circulatory system. Our study identifies EDN1 as a key factor towards the generation and clonal derivation of ISL1+ vascular intermediates, and demonstrates the intrinsic cell-autonomous nature of these progenitors to differentiate and self-organize into functional vasculatures in vivo.",

author = "Soh, {Boon Seng} and Ng, {Shi Yan} and Hao Wu and Kristina Buac and Park, {Joo Hye C.} and Xiaojun Lian and Jiejia Xu and Foo, {Kylie S.} and Ulrika Felldin and Xiaobing He and Massimo Nichane and Henry Yang and Lei Bu and Li, {Ronald A.} and Bing Lim and Chien, {Kenneth R.}",

note = "Funding Information: This work was supported in part by the Research Grant Council of HKSAR (T13-706/ 11).",

year = "2016",

month = mar,

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doi = "10.1038/ncomms10774",

language = "English (US)",

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journal = "Nature communications",

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T1 - Endothelin-1 supports clonal derivation and expansion of cardiovascular progenitors derived from human embryonic stem cells

AU - Soh, Boon Seng

AU - Ng, Shi Yan

AU - Wu, Hao

AU - Buac, Kristina

AU - Park, Joo Hye C.

AU - Lian, Xiaojun

AU - Xu, Jiejia

AU - Foo, Kylie S.

AU - Felldin, Ulrika

AU - He, Xiaobing

AU - Nichane, Massimo

AU - Yang, Henry

AU - Bu, Lei

AU - Li, Ronald A.

AU - Lim, Bing

AU - Chien, Kenneth R.

N1 - Funding Information: This work was supported in part by the Research Grant Council of HKSAR (T13-706/ 11).

PY - 2016/3/8

Y1 - 2016/3/8

N2 - Coronary arteriogenesis is a central step in cardiogenesis, requiring coordinated generation and integration of endothelial cell and vascular smooth muscle cells. At present, it is unclear whether the cell fate programme of cardiac progenitors to generate complex muscular or vascular structures is entirely cell autonomous. Here we demonstrate the intrinsic ability of vascular progenitors to develop and self-organize into cardiac tissues by clonally isolating and expanding second heart field cardiovascular progenitors using WNT3A and endothelin-1 (EDN1) human recombinant proteins. Progenitor clones undergo long-term expansion and differentiate primarily into endothelial and smooth muscle cell lineages in vitro, and contribute extensively to coronary-like vessels in vivo, forming a functional human-mouse chimeric circulatory system. Our study identifies EDN1 as a key factor towards the generation and clonal derivation of ISL1+ vascular intermediates, and demonstrates the intrinsic cell-autonomous nature of these progenitors to differentiate and self-organize into functional vasculatures in vivo.

AB - Coronary arteriogenesis is a central step in cardiogenesis, requiring coordinated generation and integration of endothelial cell and vascular smooth muscle cells. At present, it is unclear whether the cell fate programme of cardiac progenitors to generate complex muscular or vascular structures is entirely cell autonomous. Here we demonstrate the intrinsic ability of vascular progenitors to develop and self-organize into cardiac tissues by clonally isolating and expanding second heart field cardiovascular progenitors using WNT3A and endothelin-1 (EDN1) human recombinant proteins. Progenitor clones undergo long-term expansion and differentiate primarily into endothelial and smooth muscle cell lineages in vitro, and contribute extensively to coronary-like vessels in vivo, forming a functional human-mouse chimeric circulatory system. Our study identifies EDN1 as a key factor towards the generation and clonal derivation of ISL1+ vascular intermediates, and demonstrates the intrinsic cell-autonomous nature of these progenitors to differentiate and self-organize into functional vasculatures in vivo.

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Endothelin-1 supports clonal derivation and expansion of cardiovascular progenitors derived from human embryonic stem cells

Abstract

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