Natural Compound Library Screening Identifies New Molecules for the Treatment of Cardiac Fibrosis and Diastolic Dysfunction-Reference-Cited by-同舟云学术

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

Published:2020-03-03 Issue:9 Volume:141 Page:751-767
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Schimmel Katharina¹,Jung Mira¹,Foinquinos Ariana¹,José Gorka San²³,Beaumont Javier²³,Bock Katharina¹,Grote-Levi Lea¹,Xiao Ke¹,Bär Christian¹,Pfanne Angelika¹,Just Annette¹,Zimmer Karina¹,Ngoy Soeun⁴,López Begoña²³,Ravassa Susana²³,Samolovac Sabine¹,Janssen-Peters Heike¹,Remke Janet¹,Scherf Kristian¹⁵,Dangwal Seema¹⁵,Piccoli Maria-Teresa¹,Kleemiss Felix¹,Kreutzer Fabian Philipp¹,Kenneweg Franziska¹,Leonardy Julia¹,Hobuß Lisa¹,Santer Laura¹,Do Quoc-Tuan⁶,Geffers Robert⁷,Braesen Jan Hinrich⁸,Schmitz Jessica⁸,Brandenberger Christina⁹,Müller Dominik N.¹⁰,Wilck Nicola¹⁰¹¹,Kaever Volkhard¹²,Bähre Heike¹²,Batkai Sandor¹,Fiedler Jan¹,Alexander Kevin M.⁵,Wertheim Bradley M.¹³,Fisch Sudeshna⁴,Liao Ronglih⁵⁴,Diez Javier²³¹⁴,González Arantxa²³,Thum Thomas¹¹⁵^ORCID

Affiliation:

1. Institute of Molecular and Translational Therapeutic Strategies (K.S., M.J., A.F., K.B., L.G.-L., K.X., C. Bär, A.P., A.J., K.Z., S.S., H.J.-P., J.R., K.S., S.D., M.-T.P., F.K., F.P.K., F.K., J.L., L.H., L.S., S.B., J.F., T.T.), Hannover Medical School, Germany.

2. Program of Cardiovascular Diseases, CIMA Universidad de Navarra and IdiSNA, Pamplona, Spain (G.S.J., J.B., B.L., S.R., J.D., A.G.).

3. CIBERCV, Institute of Health Carlos III, Madrid, Spain (G.S.J., J.B., B.L., S.R., J.D., A.G.).

4. Department of Medicine, Divisions of Genetics and Cardiology (S.N., S.F., R.L.), Brigham and Women’s Hospital, Harvard Medical School, Boston, MA.

5. Cardiovascular Institute, Stanford University School of Medicine, CA (K.S., S.D., K.M.A., R.L.).

6. Greenpharma SAS, Department of Chemoinformatics, Orléans, France (Q.-T.D.).

7. Helmholtz Centre for Infection Research, Research Group Genome Analytics, Braunschweig, Germany (R.G.).

8. Institute for Pathology, Nephropathology Unit (J.H.B., J.S.), Hannover Medical School, Germany.

9. Institute of Functional and Applied Anatomy (C. Brandenberger), Hannover Medical School, Germany.

10. Experimental and Clinical Research Center, a cooperation of Charité-Universitätsmedizin Berlin and Max Delbrück Center for Molecular Medicine in the Helmholtz Association, Germany (D.N.M., N.W.).

11. Division of Nephrology and Internal Intensive Care Medicine, Charité-Universitätsmedizin Berlin, Germany (N.W.).

12. Research Core Unit Metabolomics, Institute of Pharmacology (V.K., H.B.), Hannover Medical School, Germany.

13. Department of Medicine, Division of Pulmonary and Critical Care Medicine (B.M.W.), Brigham and Women’s Hospital, Harvard Medical School, Boston, MA.

14. Department of Cardiology and Cardiac Surgery and Department of Nephrology, Clínica Universidad de Navarra, Pamplona, Spain (J.D.).

15. REBIRTH Center of Translational Regenerative Medicine (T.T.), Hannover Medical School, Germany.

Abstract

Background: Myocardial fibrosis is a hallmark of cardiac remodeling and functionally involved in heart failure development, a leading cause of deaths worldwide. Clinically, no therapeutic strategy is available that specifically attenuates maladaptive responses of cardiac fibroblasts, the effector cells of fibrosis in the heart. Therefore, our aim was to develop novel antifibrotic therapeutics based on naturally derived substance library screens for the treatment of cardiac fibrosis. Methods: Antifibrotic drug candidates were identified by functional screening of 480 chemically diverse natural compounds in primary human cardiac fibroblasts, subsequent validation, and mechanistic in vitro and in vivo studies. Hits were analyzed for dose-dependent inhibition of proliferation of human cardiac fibroblasts, modulation of apoptosis, and extracellular matrix expression. In vitro findings were confirmed in vivo with an angiotensin 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 antifibrotic potential of the lead compounds, treatment-dependent changes in the noncoding RNAome in primary human cardiac fibroblasts were analyzed by RNA deep sequencing. Results: 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. Conclusions: We identified the molecules bufalin and lycorine as drug candidates for therapeutic applications in cardiac fibrosis and diastolic dysfunction.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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5. Lycorine hydrochloride selectively inhibits human ovarian cancer cell proliferation and tumor neovascularization with very low toxicity

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