RBPMS2 Is a Myocardial-Enriched Splicing Regulator Required for Cardiac Function.

Akerberg, Alexander A; Trembley, Michael; Butty, Vincent; Schwertner, Asya; Zhao, Long; Beerens, Manu; Liu, Xujie; Mahamdeh, Mohammed; Yuan, Shiaulou; Boyer, Laurie; MacRae, Calum; Nguyen, Christopher; Pu, William T; Burns, Caroline E; Burns, C Geoffrey

Akerberg, Alexander A; Trembley, Michael; Butty, Vincent; Schwertner, Asya; Zhao, Long; Beerens, Manu; Liu, Xujie; Mahamdeh, Mohammed; Yuan, Shiaulou; Boyer, Laurie; MacRae, Calum; Nguyen, Christopher; Pu, William T; Burns, Caroline E; Burns, C Geoffrey.

Akerberg AA; Division of Basic and Translational Cardiovascular Research, Department of Cardiology, Boston Children's Hospital, Boston' MA (A.A.A., M.T., X.L., W.T.P., C.E.B., C.G.B.).
Trembley M; Cardiovascular Research Center, Massachusetts General Hospital, Charlestown' MA (A.A.A., A.S., L.Z., M.M., S.Y., C.N., C.E.B., C.G.B.).
Butty V; Harvard Medical School, Boston, MA (A.A.A., M.T., A.S., L.Z., M.B., X.L., M.M., S.Y., C.M., C.N., W.T.P., C.E.B., C.G.B.).
Schwertner A; Division of Basic and Translational Cardiovascular Research, Department of Cardiology, Boston Children's Hospital, Boston' MA (A.A.A., M.T., X.L., W.T.P., C.E.B., C.G.B.).
Zhao L; Harvard Medical School, Boston, MA (A.A.A., M.T., A.S., L.Z., M.B., X.L., M.M., S.Y., C.M., C.N., W.T.P., C.E.B., C.G.B.).
Beerens M; BioMicroCenter, Department of Biology (V.B.), Massachusetts Institute of Technology, Cambridge' MA.
Liu X; Department of Biology (V.B., L.B.), Massachusetts Institute of Technology, Cambridge' MA.
Mahamdeh M; Cardiovascular Research Center, Massachusetts General Hospital, Charlestown' MA (A.A.A., A.S., L.Z., M.M., S.Y., C.N., C.E.B., C.G.B.).
Yuan S; Harvard Medical School, Boston, MA (A.A.A., M.T., A.S., L.Z., M.B., X.L., M.M., S.Y., C.M., C.N., W.T.P., C.E.B., C.G.B.).
Boyer L; Harvard Medical School, Boston, MA (A.A.A., M.T., A.S., L.Z., M.B., X.L., M.M., S.Y., C.M., C.N., W.T.P., C.E.B., C.G.B.).
MacRae C; Harvard Medical School, Boston, MA (A.A.A., M.T., A.S., L.Z., M.B., X.L., M.M., S.Y., C.M., C.N., W.T.P., C.E.B., C.G.B.).
Nguyen C; Division of Cardiovascular Medicine, Brigham and Women's Hospital, Boston, MA (M.B., C.M.).
Pu WT; Division of Basic and Translational Cardiovascular Research, Department of Cardiology, Boston Children's Hospital, Boston' MA (A.A.A., M.T., X.L., W.T.P., C.E.B., C.G.B.).
Burns CE; Harvard Medical School, Boston, MA (A.A.A., M.T., A.S., L.Z., M.B., X.L., M.M., S.Y., C.M., C.N., W.T.P., C.E.B., C.G.B.).
Burns CG; Cardiovascular Research Center, Massachusetts General Hospital, Charlestown' MA (A.A.A., A.S., L.Z., M.M., S.Y., C.N., C.E.B., C.G.B.).

Circ Res ; 131(12): 980-1000, 2022 12 02.

Article en En | MEDLINE | ID: mdl-36367103

ABSTRACT

ABSTRACT

BACKGROUND:

RBPs (RNA-binding proteins) perform indispensable functions in the post-transcriptional regulation of gene expression. Numerous RBPs have been implicated in cardiac development or physiology based on gene knockout studies and the identification of pathogenic RBP gene mutations in monogenic heart disorders. The discovery and characterization of additional RBPs performing indispensable functions in the heart will advance basic and translational cardiovascular research.

METHODS:

We performed a differential expression screen in zebrafish embryos to identify genes enriched in nkx2.5-positive cardiomyocytes or cardiopharyngeal progenitors compared to nkx2.5-negative cells from the same embryos. We investigated the myocardial-enriched gene RNA-binding protein with multiple splicing (variants) 2 [RBPMS2)] by generating and characterizing rbpms2 knockout zebrafish and human cardiomyocytes derived from RBPMS2-deficient induced pluripotent stem cells.

RESULTS:

We identified 1848 genes enriched in the nkx2.5-positive population. Among the most highly enriched genes, most with well-established functions in the heart, we discovered the ohnologs rbpms2a and rbpms2b, which encode an evolutionarily conserved RBP. Rbpms2 localizes selectively to cardiomyocytes during zebrafish heart development and strong cardiomyocyte expression persists into adulthood. Rbpms2-deficient embryos suffer from early cardiac dysfunction characterized by reduced ejection fraction. The functional deficit is accompanied by myofibril disarray, altered calcium handling, and differential alternative splicing events in mutant cardiomyocytes. These phenotypes are also observed in RBPMS2-deficient human cardiomyocytes, indicative of conserved molecular and cellular function. RNA-sequencing and comparative analysis of genes mis-spliced in RBPMS2-deficient zebrafish and human cardiomyocytes uncovered a conserved network of 29 ortholog pairs that require RBPMS2 for alternative splicing regulation, including RBFOX2, SLC8A1, and MYBPC3.

CONCLUSIONS:

Our study identifies RBPMS2 as a conserved regulator of alternative splicing, myofibrillar organization, and calcium handling in zebrafish and human cardiomyocytes.

Asunto(s)

Calcio; Miocardio; Proteínas de Unión al ARN; Proteínas de Pez Cebra; Animales; Humanos; Calcio/metabolismo; Miocardio/metabolismo; Miocitos Cardíacos/metabolismo; Proteínas Represoras/metabolismo; Factores de Empalme de ARN/metabolismo; Proteínas de Unión al ARN/genética; Proteínas de Unión al ARN/metabolismo; Pez Cebra/genética; Pez Cebra/metabolismo; Proteínas de Pez Cebra/genética; Proteínas de Pez Cebra/metabolismo

Palabras clave

RNA-binding proteins; alternative splicing; human induced pluripotent stem cells; myocytes, cardiac; zebrafish

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Texto completo: 1 Banco de datos: MEDLINE Asunto principal: Calcio / Proteínas de Unión al ARN / Proteínas de Pez Cebra / Miocardio Tipo de estudio: Prognostic_studies Límite: Animals / Humans Idioma: En Año: 2022 Tipo del documento: Article

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