Allele-Specific Silencing Ameliorates Restrictive Cardiomyopathy Attributable to a Human Myosin Regulatory Light Chain Mutation.

Zaleta-Rivera, Kathia; Dainis, Alexandra; Ribeiro, Alexandre J S; Cordero, Pablo; Rubio, Gabriel; Shang, Ching; Liu, Jing; Finsterbach, Thomas; Parikh, Victoria N; Sutton, Shirley; Seo, Kinya; Sinha, Nikita; Jain, Nikhil; Huang, Yong; Hajjar, Roger J; Kay, Mark A; Szczesna-Cordary, Danuta; Pruitt, Beth L; Wheeler, Matthew T; Ashley, Euan A

Zaleta-Rivera, Kathia; Dainis, Alexandra; Ribeiro, Alexandre J S; Cordero, Pablo; Rubio, Gabriel; Shang, Ching; Liu, Jing; Finsterbach, Thomas; Parikh, Victoria N; Sutton, Shirley; Seo, Kinya; Sinha, Nikita; Jain, Nikhil; Huang, Yong; Hajjar, Roger J; Kay, Mark A; Szczesna-Cordary, Danuta; Pruitt, Beth L; Wheeler, Matthew T; Ashley, Euan A.

Afiliación

Zaleta-Rivera K; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Dainis A; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Ribeiro AJS; Department of Mechanical Engineering, Stanford University, CA (A.J.S.R., B.L.P.).
Cordero P; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Rubio G; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Shang C; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Liu J; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Finsterbach T; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Parikh VN; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Sutton S; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Seo K; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Sinha N; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Jain N; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Huang Y; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.
Hajjar RJ; Cardiovascular Institute, Cardiovascular Research Center at Icahn School of Medicine at Mount Sinai, New York, NY (R.J.H.).
Kay MA; Department of Genetics (M.A.K., E.A.A.), Stanford University School of Medicine, CA.
Szczesna-Cordary D; Department of Pediatrics (M.A.K.), Stanford University School of Medicine, CA.
Pruitt BL; Department of Molecular and Cellular Pharmacology, University of Miami Leonard M. Miller School of Medicine, FL (D.S.-C.).
Wheeler MT; Department of Mechanical Engineering, Stanford University, CA (A.J.S.R., B.L.P.).
Ashley EA; Division of Cardiovascular Medicine (K.Z.-R., A.D., P.C., G.R., C.S., J.L., T.F., W.N.P., S.S., K.S., N.S., N.J., Y.H., M.T.W., E.A.A.), Stanford University School of Medicine, CA.

Circulation ; 140(9): 765-778, 2019 08 27.

Article en En | MEDLINE | ID: mdl-31315475

ABSTRACT

ABSTRACT

BACKGROUND:

Restrictive cardiomyopathy is a rare heart disease associated with mutations in sarcomeric genes and with phenotypic overlap with hypertrophic cardiomyopathy. There is no approved therapy directed at the underlying cause. Here, we explore the potential of an interfering RNA (RNAi) therapeutic for a human sarcomeric mutation in MYL2 causative of restrictive cardiomyopathy in a mouse model.

METHODS:

A short hairpin RNA (M7.8L) was selected from a pool for specificity and efficacy. Two groups of myosin regulatory light chain N47K transgenic mice were injected with M7.8L packaged in adeno-associated virus 9 at 3 days of age and 60 days of age. Mice were subjected to treadmill exercise and echocardiography after treatment to determine maximal oxygen uptake and left ventricular mass. At the end of treatment, heart, lung, liver, and kidney tissue was harvested to determine viral tropism and for transcriptomic and proteomic analysis. Cardiomyocytes were isolated for single-cell studies.

RESULTS:

A one-time injection of AAV9-M7.8L RNAi in 3-day-old humanized regulatory light chain mutant transgenic mice silenced the mutated allele (RLC-47K) with minimal effects on the normal allele (RLC-47N) assayed at 16 weeks postinjection. AAV9-M7.8L RNAi suppressed the expression of hypertrophic biomarkers, reduced heart weight, and attenuated a pathological increase in left ventricular mass. Single adult cardiac myocytes from mice treated with AAV9-M7.8L showed partial restoration of contraction, relaxation, and calcium kinetics. In addition, cardiac stress protein biomarkers, such as calmodulin-dependent protein kinase II and the transcription activator Brg1 were reduced, suggesting recovery toward a healthy myocardium. Transcriptome analyses further revealed no significant changes of argonaute (AGO1, AGO2) and endoribonuclease dicer (DICER1) transcripts, and endogenous microRNAs were preserved, suggesting that the RNAi pathway was not saturated.

CONCLUSIONS:

Our results show the feasibility, efficacy, and safety of RNAi therapeutics directed towards human restrictive cardiomyopathy. This is a promising step toward targeted therapy for a prevalent human disease.

Asunto(s)

Cardiomiopatía Restrictiva/patología; Cadenas Ligeras de Miosina/metabolismo; Interferencia de ARN; Alelos; Animales; Calcio/metabolismo; Proteína Quinasa Tipo 2 Dependiente de Calcio Calmodulina/genética; Proteína Quinasa Tipo 2 Dependiente de Calcio Calmodulina/metabolismo; Cardiomiopatía Restrictiva/prevención & control; ADN Helicasas/genética; ADN Helicasas/metabolismo; Modelos Animales de Enfermedad; Redes Reguladoras de Genes; Vectores Genéticos/metabolismo; Humanos; Ratones; Ratones Transgénicos; Contracción Muscular; Mutagénesis Sitio-Dirigida; Miocardio/metabolismo; Miocitos Cardíacos/citología; Miocitos Cardíacos/metabolismo; Cadenas Ligeras de Miosina/antagonistas & inhibidores; Cadenas Ligeras de Miosina/genética; ARN Interferente Pequeño/metabolismo

Palabras clave

RNA interference; RNA, small interfering; adeno-associated virus; cardiomyopathy, restrictive; mice, transgenic; sequence analysis, RNA

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Texto completo: 1 Colección: 01-internacional Base de datos: MEDLINE Asunto principal: Cardiomiopatía Restrictiva / Cadenas Ligeras de Miosina / Interferencia de ARN Tipo de estudio: Prognostic_studies Límite: Animals / Humans Idioma: En Revista: Circulation Año: 2019 Tipo del documento: Article País de afiliación: Canadá

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