Astragalosides increase the cardiac diastolic function and regulate the “Calcium sensing receptor-protein kinase C-protein phosphatase 1” pathway in rats with heart failure - 29/05/18
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Graphical abstract |
Highlights |
• | The PKC-α expression and PP-1 activity was decreased when CaSR was inhibited. |
• | There is a “CaSR - PKC - PP1–PLB–Ca2+-ATPase –cardiac diastolic function” pathway in myocardium. |
• | Astragalosides regulated cardiac diastolic function. |
• | Astragalosides regulated the “CaSR - PKC - PP1–PLB–Ca2+-ATPase” pathway in myocardium. |
Abstract |
This study was designed to investigate the effects of astragalosides on cardiac diastolic function, and an emphasis was placed on the variation of the upstream molecular regulators of phospholamban. Chronic heart failure (CHF) rats were induced by ligaturing the left anterior coronary artery, and rats in the therapeutic groups were treated with either a 50 mg/kg dose of captopril, 10 mg/kg dose of astragalosides or 20 mg/kg dose of astragalosides. Four weeks after treatment, the ratio of the early and atrial peak filling velocities (E/A) and maximal slope diastolic pressure decrement (-dp/dt) both decreased in CHF rats (by 30.3% and 25.5%, respectively) and significantly increased in 20 mg/kg astragalosides and captopril-treated rats. The protein phosphatase-1 activity was lower in the 20 mg/kg astragalosides group than in the CHF group (0.22 vs 0.44, P < 0.01), and the inhibitor-1 levels in the astragalosides and captopril-treated groups were increased. Chronic heart failure increased expression of protein kinase C-α and calcium-sensing receptor, and these changes were attenuated by astragalosides therapy. Astragalosides restored the diastolic dysfunction of chronic heart failure rats, possibly by downregulation of calcium-sensing receptor and protein kinase C-α, which in turn augmented inhibitor-1 expression, reduced protein phosphatase-1 activity and increased phospholamban phosphorylation.
El texto completo de este artículo está disponible en PDF.Abbreviations : ASTA, SERCA, Cap, PLB, PP-1, PKA, CaSR, PLC, PKC, I-1, LVEDP, EF
Keywords : Chronic heart failure, Diastolic function, Calcium sensing receptor, Phospholipase C, Protein kinase C, Protein phosphatase inhibitor-1, Protein phosphatase-1 (PP-1)
Esquema
Vol 103
P. 838-843 - juillet 2018 Regresar al número
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