Mutant Phosphodiesterase 3A Protects From Hypertension-Induced Cardiac Damage-Reference-Cited by-同舟云学术

Mutant Phosphodiesterase 3A Protects From Hypertension-Induced Cardiac Damage

Published:2022-12-06 Issue:23 Volume:146 Page:1758-1778
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Ercu Maria¹²,Mücke Michael B.¹²³^ORCID,Pallien Tamara¹²,Markó Lajos²³⁴^ORCID,Sholokh Anastasiia¹²³^ORCID,Schächterle Carolin¹,Aydin Atakan¹,Kidd Alexa⁵,Walter Stephan⁶^ORCID,Esmati Yasmin²³⁴,McMurray Brandon J.⁷^ORCID,Lato Daniella F.⁷^ORCID,Yumi Sunaga-Franze Daniele¹^ORCID,Dierks Philip H.¹^ORCID,Flores Barbara Isabel Montesinos¹,Walker-Gray Ryan¹,Gong Maolian¹⁴^ORCID,Merticariu Claudia¹,Zühlke Kerstin¹,Russwurm Michael⁸,Liu Tiannan¹,Batolomaeus Theda U.P.²³⁴^ORCID,Pautz Sabine⁹,Schelenz Stefanie¹,Taube Martin¹,Napieczynska Hanna¹,Heuser Arnd¹,Eichhorst Jenny¹⁰,Lehmann Martin¹⁰,Miller Duncan C.¹²^ORCID,Diecke Sebastian¹²¹¹,Qadri Fatimunnisa¹,Popova Elena¹,Langanki Reika¹,Movsesian Matthew A.,Herberg Friedrich W.⁹^ORCID,Forslund Sofia K.¹²³⁴¹¹,Müller Dominik N.¹²⁴^ORCID,Borodina Tatiana¹,Maass Philipp G.⁷¹²,Bähring Sylvia¹³⁴^ORCID,Hübner Norbert¹²³,Bader Michael¹²³¹³,Klussmann Enno¹²^ORCID

Affiliation:

1. Max-Delbrück-Center for Molecular Medicine in the Helmholtz Association (MDC), Berlin, Germany (M.E., M.B.M., T.P., A.S., C.S., A.A., D.Y.S.-F., P.H.D., B.I.M.F., R.W.-G., M.G., C.M., K.Z., T.L., S.S., M.T., H.N., A.H., D.C.M., S.D., F.Q., E.P., R.L., S.K.F., D.N.M., T.B., S.B., N.H., M.B., E.K.).

2. DZHK (German Centre for Cardiovascular Research), partner site Berlin, Germany (M.E., M.B.M., T.P., L.M., A.S., Y.E., T.U.P.B., D.C.M., S.D., S.K.F., D.N.M., N.H., M.B., E.K.).

3. Charité-Universitätsmedizin Berlin, corporate member of Freie Universität Berlin and Humboldt-Universität zu Berlin, Germany (M.B.M., L.M., A.S., Y.E., T.U.P.B., S.K.F., S.B., N.H., M.B.).

4. Experimental and Clinical Research Center, a cooperation between the Max-Delbrück Center for Molecular Medicine in the Helmholtz Association and the Charité Universitätsmedizin Berlin, Germany (L.M., Y.E., M.G., T.U.P.B., S.K.F., D.N.M., S.B.).

5. Clinical Genetics Ltd, Christchurch, New Zealand (A.K.).

6. MVZ Nierenzentrum Limburg, Germany (S.W.).

7. Genetics and Genome Biology Program, SickKids Research Institute, Toronto, ON, Canada (B.J.M., D.F.L., P.G.M.).

8. Institut für Pharmakologie und Toxikologie, Medizinische Fakultät MA N1, Ruhr-Universität Bochum, Germany (M.R.).

9. Department of Biochemistry, University of Kassel, Germany (S.P., F.W.H.).

10. Leibniz-Forschungsinstitut für Molekulare Pharmakologie (FMP), Berlin, Germany (J.E., M.L.).

11. Berlin Institute of Health (BIH), Germany (S.D., S.K.F.).

12. Department of Molecular Genetics, University of Toronto, ON, Canada (P.G.M.).

13. Institute for Biology, University of Lübeck, Germany (M.B.).

Abstract

Background: Phosphodiesterase 3A ( PDE3A ) gain-of-function mutations cause hypertension with brachydactyly (HTNB) and lead to stroke. Increased peripheral vascular resistance, rather than salt retention, is responsible. It is surprising that the few patients with HTNB examined so far did not develop cardiac hypertrophy or heart failure. We hypothesized that, in the heart, PDE3A mutations could be protective. Methods: We studied new patients. CRISPR-Cas9–engineered rat HTNB models were phenotyped by telemetric blood pressure measurements, echocardiography, microcomputed tomography, RNA-sequencing, and single nuclei RNA-sequencing. Human induced pluripotent stem cells carrying PDE3A mutations were established, differentiated to cardiomyocytes, and analyzed by Ca 2+ imaging. We used Förster resonance energy transfer and biochemical assays. Results: We identified a new PDE3A mutation in a family with HTNB. It maps to exon 13 encoding the enzyme’s catalytic domain. All hitherto identified HTNB PDE3A mutations cluster in exon 4 encoding a region N-terminally from the catalytic domain of the enzyme. The mutations were recapitulated in rat models. Both exon 4 and 13 mutations led to aberrant phosphorylation, hyperactivity, and increased PDE3A enzyme self-assembly. The left ventricles of our patients with HTNB and the rat models were normal despite preexisting hypertension. A catecholamine challenge elicited cardiac hypertrophy in HTNB rats only to the level of wild-type rats and improved the contractility of the mutant hearts, compared with wild-type rats. The β-adrenergic system, phosphodiesterase activity, and cAMP levels in the mutant hearts resembled wild-type hearts, whereas phospholamban phosphorylation was decreased in the mutants. In our induced pluripotent stem cell cardiomyocyte models, the PDE3A mutations caused adaptive changes of Ca 2+ cycling. RNA-sequencing and single nuclei RNA-sequencing identified differences in mRNA expression between wild-type and mutants, affecting, among others, metabolism and protein folding. Conclusions: Although in vascular smooth muscle, PDE3A mutations cause hypertension, they confer protection against hypertension-induced cardiac damage in hearts. Nonselective PDE3A inhibition is a final, short-term option in heart failure treatment to increase cardiac cAMP and improve contractility. Our data argue that mimicking the effect of PDE3A mutations in the heart rather than nonselective PDE3 inhibition is cardioprotective in the long term. Our findings could facilitate the search for new treatments to prevent hypertension-induced cardiac damage.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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