Increased ER-mitochondrial coupling promotes mitochondrial respiration and bioenergetics during early phases of ER stress

Roberto Bravo; Jose Miguel Vicencio; Valentina Parra; Rodrigo Troncoso; Juan Pablo Munoz; Michael Bui; Clara Quiroga; Andrea E. Rodriguez; Hugo E. Verdejo; Jorge Ferreira; Myriam Iglewski; Mario Chiong; Thomas Simmen; Antonio Zorzano; Joseph A. Hill; Beverly A. Rothermel; Gyorgy Szabadkai; Sergio Lavandero

doi:10.1242/jcs.080762

Increased ER-mitochondrial coupling promotes mitochondrial respiration and bioenergetics during early phases of ER stress

Roberto Bravo, Jose Miguel Vicencio, Valentina Parra, Rodrigo Troncoso, Juan Pablo Munoz, Michael Bui, Clara Quiroga, Andrea E. Rodriguez, Hugo E. Verdejo, Jorge Ferreira, Myriam Iglewski, Mario Chiong, Thomas Simmen, Antonio Zorzano, Joseph A. Hill, Beverly A. Rothermel, Gyorgy Szabadkai, Sergio Lavandero

Universidad de Chile

Résultat de recherche › examen par les pairs

423 Citations (Scopus)

Résumé

Increasing evidence indicates that endoplasmic reticulum (ER) stress activates the adaptive unfolded protein response (UPR), but that beyond a certain degree of ER damage, this response triggers apoptotic pathways. The general mechanisms of the UPR and its apoptotic pathways are well characterized. However, the metabolic events that occur during the adaptive phase of ER stress, before the cell death response, remain unknown. Here, we show that, during the onset of ER stress, the reticular and mitochondrial networks are redistributed towards the perinuclear area and their points of connection are increased in a microtubule-dependent fashion. A localized increase in mitochondrial transmembrane potential is observed only in redistributed mitochondria, whereas mitochondria that remain in other subcellular zones display no significant changes. Spatial re-organization of these organelles correlates with an increase in ATP levels, oxygen consumption, reductive power and increased mitochondrial Ca ²⁺ uptake. Accordingly, uncoupling of the organelles or blocking Ca ²⁺ transfer impaired the metabolic response, rendering cells more vulnerable to ER stress. Overall, these data indicate that ER stress induces an early increase in mitochondrial metabolism that depends crucially upon organelle coupling and Ca ²⁺ transfer, which, by enhancing cellular bioenergetics, establishes the metabolic basis for the adaptation to this response.

Langue d'origine	English
Pages (de-à)	2143-2152
Nombre de pages	10
Journal	Journal of Cell Science
Volume	124
Numéro de publication	13
DOI	https://doi.org/10.1242/jcs.080762
Statut de publication	Published - juill. 1 2011

Financement

Bailleurs de fonds	Numéro du bailleur de fonds
National Heart, Lung, and Blood Institute	R01HL072016

ASJC Scopus Subject Areas

Cell Biology

Accès au document

10.1242/jcs.080762

Autres fichiers et liens

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Bravo, R., Vicencio, J. M., Parra, V., Troncoso, R., Munoz, J. P., Bui, M., Quiroga, C., Rodriguez, A. E., Verdejo, H. E., Ferreira, J., Iglewski, M., Chiong, M., Simmen, T., Zorzano, A., Hill, J. A., Rothermel, B. A., Szabadkai, G., & Lavandero, S. (2011). Increased ER-mitochondrial coupling promotes mitochondrial respiration and bioenergetics during early phases of ER stress. Journal of Cell Science, 124(13), 2143-2152. https://doi.org/10.1242/jcs.080762

Bravo, R, Vicencio, JM, Parra, V, Troncoso, R, Munoz, JP, Bui, M, Quiroga, C, Rodriguez, AE, Verdejo, HE, Ferreira, J, Iglewski, M, Chiong, M, Simmen, T, Zorzano, A, Hill, JA, Rothermel, BA, Szabadkai, G & Lavandero, S 2011, 'Increased ER-mitochondrial coupling promotes mitochondrial respiration and bioenergetics during early phases of ER stress', Journal of Cell Science, vol. 124, n° 13, pp. 2143-2152. https://doi.org/10.1242/jcs.080762

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abstract = "Increasing evidence indicates that endoplasmic reticulum (ER) stress activates the adaptive unfolded protein response (UPR), but that beyond a certain degree of ER damage, this response triggers apoptotic pathways. The general mechanisms of the UPR and its apoptotic pathways are well characterized. However, the metabolic events that occur during the adaptive phase of ER stress, before the cell death response, remain unknown. Here, we show that, during the onset of ER stress, the reticular and mitochondrial networks are redistributed towards the perinuclear area and their points of connection are increased in a microtubule-dependent fashion. A localized increase in mitochondrial transmembrane potential is observed only in redistributed mitochondria, whereas mitochondria that remain in other subcellular zones display no significant changes. Spatial re-organization of these organelles correlates with an increase in ATP levels, oxygen consumption, reductive power and increased mitochondrial Ca 2+ uptake. Accordingly, uncoupling of the organelles or blocking Ca 2+ transfer impaired the metabolic response, rendering cells more vulnerable to ER stress. Overall, these data indicate that ER stress induces an early increase in mitochondrial metabolism that depends crucially upon organelle coupling and Ca 2+ transfer, which, by enhancing cellular bioenergetics, establishes the metabolic basis for the adaptation to this response.",

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AU - Bravo, Roberto

AU - Vicencio, Jose Miguel

AU - Parra, Valentina

AU - Troncoso, Rodrigo

AU - Munoz, Juan Pablo

AU - Bui, Michael

AU - Quiroga, Clara

AU - Rodriguez, Andrea E.

AU - Verdejo, Hugo E.

AU - Ferreira, Jorge

AU - Iglewski, Myriam

AU - Chiong, Mario

AU - Simmen, Thomas

AU - Zorzano, Antonio

AU - Hill, Joseph A.

AU - Rothermel, Beverly A.

AU - Szabadkai, Gyorgy

AU - Lavandero, Sergio

PY - 2011/7/1

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N2 - Increasing evidence indicates that endoplasmic reticulum (ER) stress activates the adaptive unfolded protein response (UPR), but that beyond a certain degree of ER damage, this response triggers apoptotic pathways. The general mechanisms of the UPR and its apoptotic pathways are well characterized. However, the metabolic events that occur during the adaptive phase of ER stress, before the cell death response, remain unknown. Here, we show that, during the onset of ER stress, the reticular and mitochondrial networks are redistributed towards the perinuclear area and their points of connection are increased in a microtubule-dependent fashion. A localized increase in mitochondrial transmembrane potential is observed only in redistributed mitochondria, whereas mitochondria that remain in other subcellular zones display no significant changes. Spatial re-organization of these organelles correlates with an increase in ATP levels, oxygen consumption, reductive power and increased mitochondrial Ca 2+ uptake. Accordingly, uncoupling of the organelles or blocking Ca 2+ transfer impaired the metabolic response, rendering cells more vulnerable to ER stress. Overall, these data indicate that ER stress induces an early increase in mitochondrial metabolism that depends crucially upon organelle coupling and Ca 2+ transfer, which, by enhancing cellular bioenergetics, establishes the metabolic basis for the adaptation to this response.

AB - Increasing evidence indicates that endoplasmic reticulum (ER) stress activates the adaptive unfolded protein response (UPR), but that beyond a certain degree of ER damage, this response triggers apoptotic pathways. The general mechanisms of the UPR and its apoptotic pathways are well characterized. However, the metabolic events that occur during the adaptive phase of ER stress, before the cell death response, remain unknown. Here, we show that, during the onset of ER stress, the reticular and mitochondrial networks are redistributed towards the perinuclear area and their points of connection are increased in a microtubule-dependent fashion. A localized increase in mitochondrial transmembrane potential is observed only in redistributed mitochondria, whereas mitochondria that remain in other subcellular zones display no significant changes. Spatial re-organization of these organelles correlates with an increase in ATP levels, oxygen consumption, reductive power and increased mitochondrial Ca 2+ uptake. Accordingly, uncoupling of the organelles or blocking Ca 2+ transfer impaired the metabolic response, rendering cells more vulnerable to ER stress. Overall, these data indicate that ER stress induces an early increase in mitochondrial metabolism that depends crucially upon organelle coupling and Ca 2+ transfer, which, by enhancing cellular bioenergetics, establishes the metabolic basis for the adaptation to this response.

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Increased ER-mitochondrial coupling promotes mitochondrial respiration and bioenergetics during early phases of ER stress

Résumé

Financement

ASJC Scopus Subject Areas

Accès au document

Autres fichiers et liens

Empreinte numérique

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