Endolysosomal two-pore channels regulate autophagy in cardiomyocytes

Data de publicació: 01/06/2016

Autors de IIS La Fe

Manuel Portoles Sanz

Autor
Esther Roselló Lletí

Autor
Jose Miguel Rivera Otero

Autor

Autors aliens a IIS La Fe

Garcia-Rua, V
Feijoo-Bandin, S
Rodriguez-Penas, D
Mosquera-Leal, A
Abu-Assi, E
Beiras, A
Seoane, LM
Lear, P
Parrington, J
Gualillo, O
Parra, V
Hill, JA
Rothermel, B
Gonzalez-Juanatey, JR
Lago, F

Grups d'Investigació

Grupo de Investigación Clínica y Traslacional en Cardiología

Investigador Principal

Esther Roselló Lletí

Abstract

Autophagy participates in physiological and pathological remodelling of the heart. The endolysosomal two-pore channels (TPCs), TPC1 and TPC2, have been implicated in the regulation of autophagy. The present study aimed to investigate the role of TPC1 and TPC2 in basal and induced cardiac autophagic activity. In cultured cardiomyocytes, starvation induced a significant increase in TPC1 and TPC2 transcripts and protein levels that paralleled the increase in autophagy identified by increased LC3-II and decreased p62 levels. Small interfering RNA depletion of TPC2 alone or together with TPC1 increased both LC3II and p62 levels under basal conditions and in response to serumstarvation, suggesting that, under conditions of severe energy depletion (serum plus glucose starvation), changes in the autophagic flux (as assessed by use of bafilomycin A1) occurred either when TPC1 or TPC2 were downregulated. The knockdown of TPCs diminished cardiomyocyte viability under starvation and simulated ischaemia. Electron micrographs of hearts from TPC1/2 double knockout mice showed that cardiomyocytes contained large numbers of immature lysosomes with diameters significantly smaller than those of wild-type mice. In cardiac tissues from humans and rats, TPC1 and TPC2 transcripts and protein levels were higher in females than in males. Furthermore, transcript levels of TPCs correlated negatively with p62 levels in heart tissues. TPC1 and TPC2 are essential for appropriate basal and induced autophagic flux in cardiomyocytes (i.e. there is a negative effect on cell viability under stress conditions in their absence) and they are differentially expressed in male and female human and murine hearts, where they correlate with markers of autophagy.

Dades de la publicació

ISSN/ISSNe:: 0022-3751, 1469-7793
Tipus:: Article
Pàgines:: 3061-3077
DOI:: 10.1113/JP271332
PubMed:: 26757341
Factor d'Impacte:: 2,192 SCImago ℠
Quartil:: Q1 SCImago ℠

Documents

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Mètriques

Filiacions

Garcia-Rua, V:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain
Feijoo-Bandin, S:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain
Rodriguez-Penas, D:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain
Mosquera-Leal, A:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain
Abu-Assi, E:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain
Beiras, A:: Inst Biomed Res IDIS SERGAS, Dept Pathol, Santiago De Compostela, Spain
Seoane, LM:: Inst Biomed Res IDIS SERGAS, Dept Endocrine Pathophysiol, Santiago De Compostela, Spain
Lear, P:: Univ Oxford, Dept Pharmacol, Oxford OX1 2JD, England
Parrington, J:: Univ Oxford, Dept Pharmacol, Oxford OX1 2JD, England
Portoles, M:: La Fe Univ Hosp, Valencia, Spain
Rosello-Lleti, E:: La Fe Univ Hosp, Valencia, Spain
Rivera, M:: La Fe Univ Hosp, Valencia, Spain
Gualillo, O:: Inst Biomed Res IDIS SERGAS, Dept Neuroendocrine Interact Rheumat & Inflammato, Santiago De Compostela, Spain
Parra, V:: Univ Texas Southwestern Med Ctr, Dept Internal Med Cardiol & Mol Biol, Dallas, TX USA
Hill, JA:: Univ Texas Southwestern Med Ctr, Dept Internal Med Cardiol & Mol Biol, Dallas, TX USA
Rothermel, B:: Univ Texas Southwestern Med Ctr, Dept Internal Med Cardiol & Mol Biol, Dallas, TX USA
Gonzalez-Juanatey, JR:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain
Lago, F:: Inst Biomed Res IDIS SERGAS, Dept Cellular & Mol Cardiol, Santiago De Compostela, Spain

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