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The epicardium is composed of a single cell layer that encapsulates the heart during embryogenesis. The epicardium also serves as a rich source of mesenchymal cells and growth factors that support both cardiomyocyte and coronary vasculature development. Although the function of the epicardium is invariably linked to the growth of the primitive coronary plexus, the cellular and molecular mechanisms that regulate cell autonomous and cell non-autonomous functions of the epicardium remain unclear. To facilitate the identification of the epicardium’s role in embryonic angiogenesis, our lab utilizes transgenic mouse models and single-cell transcriptomic sequencing to discover novel epicardium-directed guidance cues required for arterio-venous specification and maturation. As compared to the fetal heart, the adult myocardium is unable to undergo angiogenesis in response to ischemic injury, which ultimately leads to cardiac functional decline. By using information acquired from our studies during development, we are investigating the effects of secreted factors from the epicardium to promote angiogenesis and repair after ischemic injury in the adult heart.
The epicardium is composed of a single cell layer that encapsulates the heart during embryogenesis. The epicardium also serves as a rich source of mesenchymal cells and growth factors that support both cardiomyocyte and coronary vasculature development. Although the function of the epicardium is invariably linked to the growth of the primitive coronary plexus, the cellular and molecular mechanisms that regulate cell autonomous and cell non-autonomous functions of the epicardium remain unclear. To facilitate the identification of the epicardium’s role in embryonic angiogenesis, our lab utilizes transgenic mouse models and single-cell transcriptomic sequencing to discover novel epicardium-directed guidance cues required for arterio-venous specification and maturation. As compared to the fetal heart, the adult myocardium is unable to undergo angiogenesis in response to ischemic injury, which ultimately leads to cardiac functional decline. By using information acquired from our studies during development, we are investigating the effects of secreted factors from the epicardium to promote angiogenesis and repair after ischemic injury in the adult heart.
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Circulation Researchno. Suppl_1 (2024)
Zhen Li, Aline Zaparte,Xiaoming Fu,Xinmin Li,David Wong,Aaron Gibson,Kiersten Gorse, Zeneng Wong,Stanley Hazen,David Lefer,Pearl Quijada, Cat Makarewich,Thomas Sharp
CIRCULATION RESEARCH (2024)
CIRCULATION RESEARCH (2024)
Circulation researchno. 2 (2024): 353-371
Pearl Quijada,Shuin Park, Peng Zhao, Kamal S. S. Kolluri, David Wong, Kevin D. Shih, Kai Fang,Arash Pezhouman,Lingjun Wang,Ali Daraei, Matthew D. Tran, Elle M. Rathbun,Kimberly N. Burgos Villar,Maria L. Garcia-Hernandez, Thanh T. D. Pham, Charles J. Lowenstein, M. Luisa Iruela-Arispe, S. Thomas Carmichael,Eric M. Small,Reza Ardehali
JOURNAL OF CLINICAL INVESTIGATIONno. 10 (2023)
David E. Ebeid,Farid G. Khalafalla,Kathleen M. Broughton,Megan M. Monsanto,Carolina Y. Esquer,Veronica Sacchi,Nirmala Hariharan,Kelli Korski,Maryam Moshref,Jacqueline Emathinger,Christopher T. Cottage,Pearl J. Quijada,Jonathan H. Nguyen,Roberto Alvarez,Mirko Volkers,Mathias H. Konstandin,Bingyan J. Wang,Fareheh Firouzi,Julian M. Navarrete,Natalie A. Gude,Marie-Jose Goumans,Mark A. Sussman
Circulation Researchno. Suppl_1 (2020)
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#Papers: 86
#Citation: 2631
H-Index: 27
G-Index: 51
Sociability: 6
Diversity: 0
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