The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1

J. M. Vicencio; C. Ortiz; A. Criollo; A. W.E. Jones; O. Kepp; L. Galluzzi; N. Joza; I. Vitale; E. Morselli; M. Tailler; M. Castedo; M. C. Maiuri; J. Molgó; G. Szabadkai; S. Lavandero; G. Kroemer

doi:10.1038/cdd.2009.34

The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1

J. M. Vicencio, C. Ortiz, A. Criollo, A. W.E. Jones, O. Kepp, L. Galluzzi, N. Joza, I. Vitale, E. Morselli, M. Tailler, M. Castedo, M. C. Maiuri, J. Molgó, G. Szabadkai, S. Lavandero, G. Kroemer^*

^*Autor correspondiente de este trabajo

Producción científica: Contribución a una revista › Artículo › revisión exhaustiva

259 Citas (Scopus)

Resumen

The inositol 1,4,5-trisphosphate receptor (IP₃R) is a major regulator of apoptotic signaling. Through interactions with members of the Bcl-2 family of proteins, it drives calcium (Ca²⁺) transients from the endoplasmic reticulum (ER) to mitochondria, thereby establishing a functional and physical link between these organelles. Importantly, the IP₃R also regulates autophagy, and in particular, its inhibition/depletion strongly induces macroautophagy. Here, we show that the IP₃R antagonist xestospongin B induces autophagy by disrupting a molecular complex formed by the IP₃ R and Beclin 1, an interaction that is increased or inhibited by overexpression or knockdown of Bcl-2, respectively. An effect of Beclin 1 on Ca²⁺ homeostasis was discarded as siRNA-mediated knockdown of Beclin 1 did not affect cytosolic or luminal ER Ca²⁺ levels. Xestospongin B- or starvation-induced autophagy was inhibited by overexpression of the IP₃R ligand-binding domain, which coimmunoprecipitated with Beclin 1. These results identify IP₃R as a new regulator of the Beclin 1 complex that may bridge signals converging on the ER and initial phagophore formation.

Idioma original	Inglés
Páginas (desde-hasta)	1006-1017
Número de páginas	12
Publicación	Cell Death and Differentiation
Volumen	16
N.º	7
DOI	https://doi.org/10.1038/cdd.2009.34
Estado	Publicada - 2009
Publicado de forma externa	Sí

Áreas temáticas de ASJC Scopus

Biología molecular
Biología celular

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Vicencio, J. M., Ortiz, C., Criollo, A., Jones, A. W. E., Kepp, O., Galluzzi, L., Joza, N., Vitale, I., Morselli, E., Tailler, M., Castedo, M., Maiuri, M. C., Molgó, J., Szabadkai, G., Lavandero, S., & Kroemer, G. (2009). The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1. Cell Death and Differentiation, 16(7), 1006-1017. https://doi.org/10.1038/cdd.2009.34

@article{16944f570d91422ba30290c25fe267a2,

title = "The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1",

abstract = "The inositol 1,4,5-trisphosphate receptor (IP3R) is a major regulator of apoptotic signaling. Through interactions with members of the Bcl-2 family of proteins, it drives calcium (Ca2+) transients from the endoplasmic reticulum (ER) to mitochondria, thereby establishing a functional and physical link between these organelles. Importantly, the IP3R also regulates autophagy, and in particular, its inhibition/depletion strongly induces macroautophagy. Here, we show that the IP3R antagonist xestospongin B induces autophagy by disrupting a molecular complex formed by the IP3 R and Beclin 1, an interaction that is increased or inhibited by overexpression or knockdown of Bcl-2, respectively. An effect of Beclin 1 on Ca2+ homeostasis was discarded as siRNA-mediated knockdown of Beclin 1 did not affect cytosolic or luminal ER Ca2+ levels. Xestospongin B- or starvation-induced autophagy was inhibited by overexpression of the IP3R ligand-binding domain, which coimmunoprecipitated with Beclin 1. These results identify IP3R as a new regulator of the Beclin 1 complex that may bridge signals converging on the ER and initial phagophore formation.",

author = "Vicencio, {J. M.} and C. Ortiz and A. Criollo and Jones, {A. W.E.} and O. Kepp and L. Galluzzi and N. Joza and I. Vitale and E. Morselli and M. Tailler and M. Castedo and Maiuri, {M. C.} and J. Molg{\'o} and G. Szabadkai and S. Lavandero and G. Kroemer",

note = "Funding Information: Acknowledgements. GK is supported by the Ligue Nationale contre le Cancer ({\'e}quipe labellis{\'e}e), European Commission (RIGHT, ChemoRes, Apop-Train, Apo-SYs), Agence Nationale pour la Recherche, Canc{\'e}rop{\^o}le Ile-de-France and Institut National contre le Cancer (INCa). We thank the International Collaboration Program ECOS-CONICYT, project C08S01. JMV is supported by Fondation pour la Recherche M{\'e}dicale and CONICYT. CO holds a PhD scholarship from CONICYT, Chile. OK is supported by EMBO. AWEJ is a Medical Research Council student. We also thank Michael R Duchen (University College London) for the use of confocal facility (Zeiss LSM 510 Meta) and discussions, as well as to Dr. Roger Y Tsien (University of California at San Diego) for the donation of ERD1.",

year = "2009",

doi = "10.1038/cdd.2009.34",

language = "English",

volume = "16",

pages = "1006--1017",

journal = "Cell Death and Differentiation",

issn = "1350-9047",

publisher = "Springer Nature",

number = "7",

}

Vicencio, JM, Ortiz, C, Criollo, A, Jones, AWE, Kepp, O, Galluzzi, L, Joza, N, Vitale, I, Morselli, E, Tailler, M, Castedo, M, Maiuri, MC, Molgó, J, Szabadkai, G, Lavandero, S & Kroemer, G 2009, 'The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1', Cell Death and Differentiation, vol. 16, n.º 7, pp. 1006-1017. https://doi.org/10.1038/cdd.2009.34

TY - JOUR

T1 - The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1

AU - Vicencio, J. M.

AU - Ortiz, C.

AU - Criollo, A.

AU - Jones, A. W.E.

AU - Kepp, O.

AU - Galluzzi, L.

AU - Joza, N.

AU - Vitale, I.

AU - Morselli, E.

AU - Tailler, M.

AU - Castedo, M.

AU - Maiuri, M. C.

AU - Molgó, J.

AU - Szabadkai, G.

AU - Lavandero, S.

AU - Kroemer, G.

N1 - Funding Information: Acknowledgements. GK is supported by the Ligue Nationale contre le Cancer (équipe labellisée), European Commission (RIGHT, ChemoRes, Apop-Train, Apo-SYs), Agence Nationale pour la Recherche, Cancéropôle Ile-de-France and Institut National contre le Cancer (INCa). We thank the International Collaboration Program ECOS-CONICYT, project C08S01. JMV is supported by Fondation pour la Recherche Médicale and CONICYT. CO holds a PhD scholarship from CONICYT, Chile. OK is supported by EMBO. AWEJ is a Medical Research Council student. We also thank Michael R Duchen (University College London) for the use of confocal facility (Zeiss LSM 510 Meta) and discussions, as well as to Dr. Roger Y Tsien (University of California at San Diego) for the donation of ERD1.

PY - 2009

Y1 - 2009

N2 - The inositol 1,4,5-trisphosphate receptor (IP3R) is a major regulator of apoptotic signaling. Through interactions with members of the Bcl-2 family of proteins, it drives calcium (Ca2+) transients from the endoplasmic reticulum (ER) to mitochondria, thereby establishing a functional and physical link between these organelles. Importantly, the IP3R also regulates autophagy, and in particular, its inhibition/depletion strongly induces macroautophagy. Here, we show that the IP3R antagonist xestospongin B induces autophagy by disrupting a molecular complex formed by the IP3 R and Beclin 1, an interaction that is increased or inhibited by overexpression or knockdown of Bcl-2, respectively. An effect of Beclin 1 on Ca2+ homeostasis was discarded as siRNA-mediated knockdown of Beclin 1 did not affect cytosolic or luminal ER Ca2+ levels. Xestospongin B- or starvation-induced autophagy was inhibited by overexpression of the IP3R ligand-binding domain, which coimmunoprecipitated with Beclin 1. These results identify IP3R as a new regulator of the Beclin 1 complex that may bridge signals converging on the ER and initial phagophore formation.

AB - The inositol 1,4,5-trisphosphate receptor (IP3R) is a major regulator of apoptotic signaling. Through interactions with members of the Bcl-2 family of proteins, it drives calcium (Ca2+) transients from the endoplasmic reticulum (ER) to mitochondria, thereby establishing a functional and physical link between these organelles. Importantly, the IP3R also regulates autophagy, and in particular, its inhibition/depletion strongly induces macroautophagy. Here, we show that the IP3R antagonist xestospongin B induces autophagy by disrupting a molecular complex formed by the IP3 R and Beclin 1, an interaction that is increased or inhibited by overexpression or knockdown of Bcl-2, respectively. An effect of Beclin 1 on Ca2+ homeostasis was discarded as siRNA-mediated knockdown of Beclin 1 did not affect cytosolic or luminal ER Ca2+ levels. Xestospongin B- or starvation-induced autophagy was inhibited by overexpression of the IP3R ligand-binding domain, which coimmunoprecipitated with Beclin 1. These results identify IP3R as a new regulator of the Beclin 1 complex that may bridge signals converging on the ER and initial phagophore formation.

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U2 - 10.1038/cdd.2009.34

DO - 10.1038/cdd.2009.34

M3 - Article

C2 - 19325567

AN - SCOPUS:67549135655

SN - 1350-9047

VL - 16

SP - 1006

EP - 1017

JO - Cell Death and Differentiation

JF - Cell Death and Differentiation

IS - 7

ER -

The inositol 1,4,5-trisphosphate receptor regulates autophagy through its interaction with Beclin 1

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