Troponin I Tyrosine Phosphorylation Beneficially Accelerates Diastolic Function.

Salyer, Lorien G; Salhi, Hussam E; Brundage, Elizabeth A; Shettigar, Vikram; Sturgill, Sarah L; Zanella, Helena; Templeton, Benjamin; Abay, Eaman; Emmer, Kathryn M; Lowe, Jeovanna; Rafael-Fortney, Jill A; Parinandi, Narasimham; Foster, D Brian; McKinsey, Timothy A; Woulfe, Kathleen C; Ziolo, Mark T; Biesiadecki, Brandon J

Salyer, Lorien G; Salhi, Hussam E; Brundage, Elizabeth A; Shettigar, Vikram; Sturgill, Sarah L; Zanella, Helena; Templeton, Benjamin; Abay, Eaman; Emmer, Kathryn M; Lowe, Jeovanna; Rafael-Fortney, Jill A; Parinandi, Narasimham; Foster, D Brian; McKinsey, Timothy A; Woulfe, Kathleen C; Ziolo, Mark T; Biesiadecki, Brandon J.

Afiliación

Salyer LG; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Salhi HE; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Brundage EA; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Shettigar V; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Sturgill SL; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Zanella H; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Templeton B; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Abay E; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Emmer KM; University Laboratory Animal Resources (K.M.E.), Ohio State University, Columbus.
Lowe J; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Rafael-Fortney JA; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.
Parinandi N; Division of Pulmonary, Critical Care and Sleep Medicine (N.P.), Ohio State University, Columbus.
Foster DB; Division of Cardiology, Department of Medicine, The Johns Hopkins University School of Medicine, Baltimore, MD (D.B.F.).
McKinsey TA; Department of Medicine, Division of Cardiology (T.A.M., K.C.W.), University of Colorado Anschutz Medical Campus, Aurora.
Woulfe KC; Consortium for Fibrosis Research and Translation (T.A.M.), University of Colorado Anschutz Medical Campus, Aurora.
Ziolo MT; Department of Medicine, Division of Cardiology (T.A.M., K.C.W.), University of Colorado Anschutz Medical Campus, Aurora.
Biesiadecki BJ; Department of Physiology and Cell Biology, Davis Heart and Lung Research Institute (L.G.S., H.E.S., E.A.B., V.S., S.L.S., H.Z., B.T., E.A., J.L., J.A.R.-F., M.T.Z., B.J.B.), Ohio State University, Columbus.

Circ Res ; 134(1): 33-45, 2024 01 05.

Article en En | MEDLINE | ID: mdl-38095088

ABSTRACT

ABSTRACT

BACKGROUND:

A healthy heart is able to modify its function and increase relaxation through post-translational modifications of myofilament proteins. While there are known examples of serine/threonine kinases directly phosphorylating myofilament proteins to modify heart function, the roles of tyrosine (Y) phosphorylation to directly modify heart function have not been demonstrated. The myofilament protein TnI (troponin I) is the inhibitory subunit of the troponin complex and is a key regulator of cardiac contraction and relaxation. We previously demonstrated that TnI-Y26 phosphorylation decreases calcium-sensitive force development and accelerates calcium dissociation, suggesting a novel role for tyrosine kinase-mediated TnI-Y26 phosphorylation to regulate cardiac relaxation. Therefore, we hypothesize that increasing TnI-Y26 phosphorylation will increase cardiac relaxation in vivo and be beneficial during pathological diastolic dysfunction.

METHODS:

The signaling pathway involved in TnI-Y26 phosphorylation was predicted in silico and validated by tyrosine kinase activation and inhibition in primary adult murine cardiomyocytes. To investigate how TnI-Y26 phosphorylation affects cardiac muscle, structure, and function in vivo, we developed a novel TnI-Y26 phosphorylation-mimetic mouse that was subjected to echocardiography, pressure-volume loop hemodynamics, and myofibril mechanical studies. TnI-Y26 phosphorylation-mimetic mice were further subjected to the nephrectomy/DOCA (deoxycorticosterone acetate) model of diastolic dysfunction to investigate the effects of increased TnI-Y26 phosphorylation in disease.

RESULTS:

Src tyrosine kinase is sufficient to phosphorylate TnI-Y26 in cardiomyocytes. TnI-Y26 phosphorylation accelerates in vivo relaxation without detrimental structural or systolic impairment. In a mouse model of diastolic dysfunction, TnI-Y26 phosphorylation is beneficial and protects against the development of disease.

CONCLUSIONS:

We have demonstrated that tyrosine kinase phosphorylation of TnI is a novel mechanism to directly and beneficially accelerate myocardial relaxation in vivo.

Asunto(s)

Calcio; Troponina I; Ratones; Animales; Fosforilación; Troponina I/genética; Calcio/metabolismo; Procesamiento Proteico-Postraduccional; Contracción Miocárdica/fisiología; Miofibrillas/metabolismo; Proteínas Tirosina Quinasas; Tirosina/metabolismo; Tirosina/farmacología

Palabras clave

hemodynamics; myofibrils; phosphorylation; troponin I; tyrosine

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Texto completo: 1 Colección: 01-internacional Banco de datos: MEDLINE Asunto principal: Calcio / Troponina I Límite: Animals Idioma: En Revista: Circ Res Año: 2024 Tipo del documento: Article

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