Kyungsun Heo
University of Rochester
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Publication
Featured researches published by Kyungsun Heo.
Circulation Research | 2013
Kyungsun Heo; Eugene B. Chang; Nhat-Tu Le; Hannah J. Cushman; Edward T.H. Yeh; Keigi Fujiwara; Jun Ichi Abe
Rationale: Disturbed flow induces proinflammatory and apoptotic responses in endothelial cells, causing them to become dysfunctional and subsequently proatherogenic. Objective: Although a possible link between SUMOylation of p53 and ERK5 detected during endothelial apoptosis and inflammation has been suggested, the mechanistic insights, especially under the proatherogenic flow condition, remain largely unknown. Methods and Results: SUMOylation of p53 and ERK5 was induced by disturbed flow but not by steady laminar flow. To examine the role of the disturbed flow–induced p53 and ERK5 SUMOylation, we used de-SUMOylation enzyme of sentrin/Small Ubiquitin-like MOdifier (SUMO)-specific protease 2 deficiency (Senp2+/−) mice and observed a significant increase in endothelial apoptosis and adhesion molecule expression both in vitro and in vivo. These increases, however, were significantly inhibited in endothelial cells overexpressing p53 and ERK5 SUMOylation site mutants. Senp2+/− mice exhibited increased leukocyte rolling along the endothelium, and accelerated formation of atherosclerotic lesions was observed in Senp2+/−/Ldlr−/−, but not in Senp2+/+/Ldlr−/−, mice fed a high-cholesterol diet. Notably, the extent of lesion size in the aortic arch of Senp2+/−/Ldlr−/− mice was much larger than that in the descending aorta, also suggesting a crucial role of the disturbed flow–induced SUMOylation of proteins, including p53 and ERK5 in atherosclerosis formation. Conclusions: These data show the unique role of sentrin/SUMO-specific protease 2 on endothelial function under disturbed flow and suggest that SUMOylation of p53 and ERK5 by disturbed flow contributes to the atherosclerotic plaque formation. Molecules involved in this newly discovered signaling will be useful targets for controlling endothelial cells dysfunction and consequently atherosclerosis formation.
Circulation Research | 2012
Yuichiro Takei; Nhat-Tu Le; Hakjoo Lee; Kyungsun Heo; Cheryl Hurley; Alan V. Smrcka; Benjamin L. Miller; Kyung Ae Ko; Craing Morrell; Keigi Fujiwara; Masashi Akaike; Jun Ichi Abe
Circulation | 2018
Meera V. Singh; Sivareddy Kotla; Nhat-Tu Le; Kyung Ae Ko; Kyungsun Heo; Yin Wang; Yuka Fujii; Hang Thi Vu; Elena McBeath; Tamlyn Thomas; Young-Jin Gi; Yunting Tao; Jan L. Medina; Jack Taunton; Nancy Carson; Vikram S. Dogra; Marvin M. Doyley; Alicia Tyrell; Wang Lu; Xing Qiu; Nicole E. Stirpe; Kathleen Gates; Christine Hurley; Keigi Fujiwara; Sanjay B. Maggirwar; Giovanni Schifitto; Jun Ichi Abe
Circulation | 2014
Kyungsun Heo; Massashi Akaike; Jack Taunton; Keigi Fujiwara; Jun Ichi Abe
Arteriosclerosis, Thrombosis, and Vascular Biology | 2014
Kyungsun Heo; Masashi Akike; Jack Taunton; Keigi Fujiwara; Jun Ichi Abe
Circulation | 2013
Kyungsun Heo; Nhat-Tu Le; Hannah J. Cushman; Carolyn J. Giancursio; Eugene B. Chang; Chang-Hoon Woo; Jack Taunton; Edward T.H. Yeh; Keigi Fujiwara; Jun Ichi Abe
Arteriosclerosis, Thrombosis, and Vascular Biology | 2013
Kyungsun Heo; Hannah J. Cushman; Chang-Hoon Woo; Masashi Akaike; Xin Wang; Craig N. Morrell; Keigi Fujiwara; Jun Ichi Abe
Circulation | 2012
Kyungsun Heo; Eugene B. Chang; Nhat-Tu Le; Hannah J. Cushman; Edward T.H. Yeh; Keigi Fujiwara; Jun Ichi Abe
Circulation | 2010
Eugene B. Chang; Kyungsun Heo; Chang-Hoon Woo; Keigi Fujiwara; Jun Ichi Abe
Circulation | 2010
Kyungsun Heo; Hakjoo Lee; Nhat-Tu Le; Chang-Hoon Woo; Eugene B. Chang; Carolyn McClain; Craig N. Morrell; Keigi Fujiwara; Ja Abe
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