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Dive into the research topics where Horng H. Chen is active.

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Featured researches published by Horng H. Chen.


Journal of Cardiac Failure | 1998

Neutral endopeptidase inhibition potentiates the natriuretic actions of adrenomedullin

Ondrej Lisy; M Jougaski; John A. Schirger; Horng H. Chen; Pt Barclay; John C. Burnett

Lisy, Ondrej, Michihisa Jougasaki, John A. Schirger, Horng H. Chen, Paul T. Barclay, and John C. Burnett, Jr. Neutral endopeptidase inhibition potentiates the natriuretic actions of adrenomedullin. Am. J. Physiol. 275 (Renal Physiol. 44): F410–F414, 1998.—Adrenomedullin (ADM) is a potent renal vasodilating and natriuretic peptide possessing a six amino acid disulfide ring. Neutral endopeptidase 24.11 (NEP) is localized in greatest abundance in the kidney and cleaves endogenous peptides like atrial natriuretic peptide, which also possesses a disulfide ring. We hypothesized that NEP inhibition potentiates the natriuretic actions of exogenous ADM in anesthetized dogs (n 5 6). We therefore investigated renal function in which one kidney received intrarenal infusion of ADM (1 ng·kg21 ·min21) while the contralateral kidney served as control before and during the systemic infusion of a NEP inhibitor (Candoxatrilat, 8 μg·kg21 ·min21; Pfizer). In response to ADM, glomerular filtration rate (GFR) in the ADM kidney did not change, whereas renal blood flow, urine flow (UV), and urinary sodium excretion (UNaV) increased from baseline. Proximal and distal fractional reabsorption of sodium decreased in the ADM-infused kidney. In response to systemic NEP inhibition, UNaV and UV increased further in the ADM kidney. Indeed, DUNaV and DUV were markedly greater in the ADM kidney compared with the control kidney. Plasma ADM was unchanged during ADM infusion but increased during NEP inhibition. In conclusion, the present investigation is the first to demonstrate that NEP inhibition potentiates the natriuretic and diuretic responses to intrarenal ADM. This potentiation occurs secondary to a decrease in tubular sodium reabsorption. Lastly, the increase in plasma ADM during systemic NEP inhibition supports the conclusion that ADM is a substrate for NEP.


American Journal of Cardiology | 2006

Association of B-Type Natriuretic Peptide Activation to Left Ventricular End-Systolic Remodeling in Organic and Functional Mitral Regurgitation

Delphine Detaint; David Messika-Zeitoun; Horng H. Chen; A. Rossi; Jean-François Avierinos; Christopher G. Scott; John C. Burnett; Maurice Enriquez-Sarano


Archive | 2009

Natriuretic polypeptides for reducing or preventing restenosis

John C. Burnett; Horng H. Chen; Ondrej Lisy


Archive | 2009

Chimeric natriuretic polypeptides and methods for inhibiting cardiac remodeling

John C. Burnett; Horng H. Chen; Ondrej Lisy


Archive | 2007

TYPE V PHOSPHODIESTERASE INHIBITORS AND NATRIURETIC POLYPEPTIDES

John C. Burnett; Horng H. Chen


Archive | 2007

Diuretic and natriuretic polypeptides lacking the blood pressure lowering property

Robert D. Simari; Shuchong Pan; John C. Burnett; Horng H. Chen


Archive | 2010

Natriuretic polypeptides having mutations within their disulfide rings

John C. Burnett; Horng H. Chen


Archive | 2012

Chimeric aquaretic and natriuretic polypeptides lacking vasodilatory activity

Horng H. Chen; John C. Burnett


Journal of Cardiac Failure | 1998

A new natriuretic peptide present in canine plasma and heart

Ondrej Lisy; Michihisa Jougasaki; Denise M. Heublein; John A. Schirger; Horng H. Chen; Pw Wennberg; John C. Burnett


Archive | 2013

Subcutaneous delivery of a long-acting natriuretic peptide

Horng H. Chen; John C. Burnett; Daniel J. McCormick

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Shuchong Pan

University of Rochester

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A. Rossi

University of Rochester

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