Cardioprotection by Klotho through downregulation of TRPC6 channels in the mouse heart

Jian Xie; Seung Kuy Cha; Sung Wan An; Makoto Kuro-O; Lutz Birnbaumer; Chou Long Huang

doi:10.1038/ncomms2240

Cardioprotection by Klotho through downregulation of TRPC6 channels in the mouse heart

Jian Xie, Seung Kuy Cha, Sung Wan An, Makoto Kuro-O, Lutz Birnbaumer, Chou Long Huang

Research output: Contribution to journal › Article › peer-review

268 Scopus citations

Abstract

Klotho is a membrane protein predominantly produced in the kidney that exerts some antiageing effects. Ageing is associated with an increased risk of heart failure; whether Klotho is cardioprotective is unknown. Here we show that Klotho-deficient mice have no baseline cardiac abnormalities but develop exaggerated pathological cardiac hypertrophy and remodelling in response to stress. Cardioprotection by Klotho in normal mice is mediated by downregulation of TRPC6 channels in the heart. We demonstrate that deletion of Trpc6 prevents stress-induced exaggerated cardiac remodelling in Klotho-deficient mice. Furthermore, mice with heart-specific overexpression of TRPC6 develop spontaneous cardiac hypertrophy and remodelling. Klotho overexpression ameliorates cardiac pathologies in these mice and improves their long-term survival. Soluble Klotho present in the systemic circulation inhibits TRPC6 currents in cardiomyocytes by blocking phosphoinositide-3-kinase-dependent exocytosis of TRPC6 channels. These results provide a new perspective on the pathogenesis of cardiomyopathies and open new avenues for treatment of the disease.

Original language	English (US)
Article number	1238
Journal	Nature communications
Volume	3
DOIs	https://doi.org/10.1038/ncomms2240
State	Published - 2012

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General Physics and Astronomy

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10.1038/ncomms2240

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@article{196644bfa3c34ade98e8aa151f645902,

title = "Cardioprotection by Klotho through downregulation of TRPC6 channels in the mouse heart",

abstract = "Klotho is a membrane protein predominantly produced in the kidney that exerts some antiageing effects. Ageing is associated with an increased risk of heart failure; whether Klotho is cardioprotective is unknown. Here we show that Klotho-deficient mice have no baseline cardiac abnormalities but develop exaggerated pathological cardiac hypertrophy and remodelling in response to stress. Cardioprotection by Klotho in normal mice is mediated by downregulation of TRPC6 channels in the heart. We demonstrate that deletion of Trpc6 prevents stress-induced exaggerated cardiac remodelling in Klotho-deficient mice. Furthermore, mice with heart-specific overexpression of TRPC6 develop spontaneous cardiac hypertrophy and remodelling. Klotho overexpression ameliorates cardiac pathologies in these mice and improves their long-term survival. Soluble Klotho present in the systemic circulation inhibits TRPC6 currents in cardiomyocytes by blocking phosphoinositide-3-kinase-dependent exocytosis of TRPC6 channels. These results provide a new perspective on the pathogenesis of cardiomyopathies and open new avenues for treatment of the disease.",

author = "Jian Xie and Cha, {Seung Kuy} and An, {Sung Wan} and Makoto Kuro-O and Lutz Birnbaumer and Huang, {Chou Long}",

note = "Funding Information: We thank Eric Olson for TRPC6-Tg mice, Jyothsna Gattineni for assistance with measurements of serum FGF23 and phosphate, Masaya Takahashi and Kim Kangasniemi for cardiac MRI, and Peter Igarashi, Orson Moe and Aylin Rodan for discussions and comments. This work was supported by NIH (DK59530, DK85726, DK79328, DK91392), the Intramural Research Program of the NIH (ZO1-ES-101684) and by a GRIP grant from Genzyme, Inc. C.-L.H. holds the Jacob Lemann Professorship in Calcium Transport of University of Texas Southwestern Medical Center.",

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AU - An, Sung Wan

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AU - Birnbaumer, Lutz

AU - Huang, Chou Long

N1 - Funding Information: We thank Eric Olson for TRPC6-Tg mice, Jyothsna Gattineni for assistance with measurements of serum FGF23 and phosphate, Masaya Takahashi and Kim Kangasniemi for cardiac MRI, and Peter Igarashi, Orson Moe and Aylin Rodan for discussions and comments. This work was supported by NIH (DK59530, DK85726, DK79328, DK91392), the Intramural Research Program of the NIH (ZO1-ES-101684) and by a GRIP grant from Genzyme, Inc. C.-L.H. holds the Jacob Lemann Professorship in Calcium Transport of University of Texas Southwestern Medical Center.

PY - 2012

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N2 - Klotho is a membrane protein predominantly produced in the kidney that exerts some antiageing effects. Ageing is associated with an increased risk of heart failure; whether Klotho is cardioprotective is unknown. Here we show that Klotho-deficient mice have no baseline cardiac abnormalities but develop exaggerated pathological cardiac hypertrophy and remodelling in response to stress. Cardioprotection by Klotho in normal mice is mediated by downregulation of TRPC6 channels in the heart. We demonstrate that deletion of Trpc6 prevents stress-induced exaggerated cardiac remodelling in Klotho-deficient mice. Furthermore, mice with heart-specific overexpression of TRPC6 develop spontaneous cardiac hypertrophy and remodelling. Klotho overexpression ameliorates cardiac pathologies in these mice and improves their long-term survival. Soluble Klotho present in the systemic circulation inhibits TRPC6 currents in cardiomyocytes by blocking phosphoinositide-3-kinase-dependent exocytosis of TRPC6 channels. These results provide a new perspective on the pathogenesis of cardiomyopathies and open new avenues for treatment of the disease.

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Cardioprotection by Klotho through downregulation of TRPC6 channels in the mouse heart

Abstract

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