High-throughput natural compound library screening identified 15 substances with antiproliferative effects in human cardiac fibroblasts. Using multiple in vitro fibrosis assays and stringent selection algorithms, we identified the steroid bufalin (from Chinese toad venom) and the alkaloid lycorine (from Amaryllidaceae species) to be effective antifibrotic molecules both in vitro and in vivo, leading to improvement in diastolic function in 2 hypertension-dependent rodent models of cardiac fibrosis. Administration at effective doses did not change plasma damage markers or the morphology of kidney and liver, providing the first toxicological safety data. Using next-generation sequencing, we identified the conserved microRNA 671-5p and downstream the antifibrotic selenoprotein P1 as common effectors of the antifibrotic compounds

Alexander, Kevin M

Batkai, Sandor

Beaumont, Javier

Bock, Katharina

Braesen, Jan Hinrich

Brandenberger, Christina

Bähre, Heike

Bär, Christian

Dangwal, Seema

Diez, Javier

Do, Quoc-Tuan

Fiedler, Jan

Fisch, Sudeshna

Foinquinos, Ariana

Geffers, Robert

González, Arantxa

Grote-Levi, Lea

Hobuß, Lisa

Janssen-Peters, Heike

José, Gorka San

Jung, Mira

Just, Annette

Kaever, Volkhard

Kenneweg, Franziska

Kleemiss, Felix

Kreutzer, Fabian Philipp

Leonardy, Julia

Liao, Ronglih

López, Begoña

Müller, Dominik N

Ngoy, Soeun

Pfanne, Angelika

Piccoli, Maria-Teresa

Ravassa, Susana

Remke, Janet

Samolovac, Sabine

Santer, Laura

Scherf, Kristian

Schimmel, Katharina

Schmitz, Jessica

Thum, Thomas

Wertheim, Bradley M

Wilck, Nicola

Xiao, Ke

Zimmer, Karina

Circulation

BACKGROUND: Myocardial fibrosis is a hallmark of cardiac remodeling and functionally involved in heart failure (HF) development, a leading cause of deaths worldwide. Clinically there is no therapeutic strategy available that specifically attenuates maladaptive responses of cardiac fibroblasts, the effector cells of fibrosis in the heart. Therefore, we aimed at the development of novel anti-fibrotic therapeutics based on natural-derived substance library screens for the treatment of cardiac fibrosis. METHODS: Anti-fibrotic drug candidates were identified by functional screening of 480 chemically diverse natural compounds in primary human cardiac fibroblasts (HCFs), subsequent validation and mechanistic in vitro and in vivo studies. Hits were analyzed for dose-dependent inhibition of proliferation of HCFs, for modulation of apoptosis and extracellular matrix expression. In vitro findings were confirmed in vivo, using an angiotensin II (Ang II)-mediated murine model of cardiac fibrosis in both preventive and therapeutic settings, as well as in the Dahl salt sensitive rat model. To investigate the mechanism underlying the anti-fibrotic potential of the lead compounds, treatment-dependent changes in the noncoding RNAome in primary HCFs were analyzed by RNA-deep sequencing. RESULTS: High-throughput natural compound library screening identified 15 substances with antiproliferative effects in HCFs. Using multiple in vitro fibrosis assays and stringent selection algorithms we identified the steroid bufalin (from Chinese toad venom) and the alkaloid lycorine (from Amaryllidaceae species) to be effective anti-fibrotic molecules both in vitro and in vivo leading to improvement in diastolic function in two hypertension-dependent rodent models of cardiac fibrosis. Administration at effective doses did not change plasma damage markers nor the morphology of kidney and liver, providing first toxicological safety data. By next-generation sequencing we identified the conserved microRNA (miR) miR-671-5p and downstream the antifibrotic selenoprotein P1 (SEPP1) as common effectors of the anti-fibrotic compounds. CONCLUSION: We identified the molecules bufalin and lycorine as drug candidates for therapeutic applications in cardiac fibrosis and diastolic dysfunction

Schimmel, K.

Jung, M.

Foinquinos, A.

San José, G.

Beaumont, J.

Bock, K.

Grote-Levi, L.

Xiao, K.

Bär, C.

Pfanne, A.

Just, A.

Zimmer, K.

Ngoy, S.

López, B.

Ravassa, S.

Samolovac, S.

Janssen-Peters, H.

Remke, J.

Scherf, K.

Dangwal, S.

Piccoli, M.T.

Kleemiss, F.

Kreutzer, F.P.

Kenneweg, F.

Leonardy, J.

Hobuß, L.

Santer, L.

Do, Q.T.

Geffers, R.

Braesen, J.H.

Schmitz, J.

Brandenberger, C.

Müller, D.N.

Wilck, N.

Kaever, V.

Bähre, H.

Batkai, S.

Fiedler, J.

Alexander, K.M.

Wertheim, B.M.

Fisch, S.

Liao, R.

Diez, J.

González, A.

Thum, T.

MDC Repository

English

Natural compound library screening identifies new molecules for the treatment of cardiac fibrosis and diastolic dysfunction

Xu Y

Zhao H

Crossref

Natural Compound Library Screening Identifies New Molecules for the Treatment of Cardiac Fibrosis and Diastolic Dysfunction

Helmholtz Zentrum für Infektionsforschung Repository

Natural Compound Library Screening Identifies New Molecules for the Treatment of Cardiac Fibrosis and Diastolic Dysfunction.

http://edoc.mdc-berlin.de/18673/13/18673oa.pdf

Natural Compound Library Screening Identifies New Molecules for the Treatment of Cardiac Fibrosis and Diastolic Dysfunction.

Abstract

Similar works

Full text

Available Versions

MDC Repository

Crossref

Helmholtz Zentrum für Infektionsforschung Repository