A brain-specific isoform of mitochondrial apoptosis-inducing factor: AIF2

E. Hangen; D. De Zio; M. Bordi; C. Zhu; P. Dessen; F. Caffin; S. Lachkar; J. L. Perfettini; V. Lazar; J. Benard; G. M. Fimia; M. Piacentini; F. Harper; G. Pierron; J. M. Vicencio; P. Bénit; A. De Andrade; G. Höglinger; C. Culmsee; P. Rustin; K. Blomgren; F. Cecconi; G. Kroemer; N. Modjtahedi

doi:10.1038/cdd.2009.211

A brain-specific isoform of mitochondrial apoptosis-inducing factor: AIF2

E. Hangen, D. De Zio, M. Bordi, C. Zhu, P. Dessen, F. Caffin, S. Lachkar, J. L. Perfettini, V. Lazar, J. Benard, G. M. Fimia, M. Piacentini, F. Harper, G. Pierron, J. M. Vicencio, P. Bénit, A. De Andrade, G. Höglinger, C. Culmsee, P. RustinK. Blomgren, F. Cecconi, G. Kroemer, N. Modjtahedi

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

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Abstract

Apoptosis-inducing factor (AIF) has important supportive as well as potentially lethal roles in neurons. Under normal physiological conditions, AIF is a vital redox-active mitochondrial enzyme, whereas in pathological situations, it translocates from mitochondria to the nuclei of injured neurons and mediates apoptotic chromatin condensation and cell death. In this study, we reveal the existence of a brain-specific isoform of AIF, AIF2, whose expression increases as neuronal precursor cells differentiate. AIF2 arises from the utilization of the alternative exon 2b, yet uses the same remaining 15 exons as the ubiquitous AIF1 isoform. AIF1 and AIF2 are similarly imported to mitochondria in which they anchor to the inner membrane facing the intermembrane space. However, the mitochondrial inner membrane sorting signal encoded in the exon 2b of AIF2 is more hydrophobic than that of AIF1, indicating a stronger membrane anchorage of AIF2 than AIF1. AIF2 is more difficult to be desorbed from mitochondria than AIF1 on exposure to non-ionic detergents or basic pH. Furthermore, AIF2 dimerizes with AIF1, thereby preventing its release from mitochondria. Conversely, it is conceivable that a neuron-specific AIF isoform, AIF2, may have been designed to be retained in mitochondria and to minimize its potential neurotoxic activity.

Originalsprache	Englisch
Seiten (von - bis)	1155-1166
Seitenumfang	12
Fachzeitschrift	Cell Death and Differentiation
Jahrgang	17
Ausgabenummer	7
DOIs	https://doi.org/10.1038/cdd.2009.211
Publikationsstatus	Veröffentlicht - Juli 2010
Extern publiziert	Ja

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Hangen, E., De Zio, D., Bordi, M., Zhu, C., Dessen, P., Caffin, F., Lachkar, S., Perfettini, J. L., Lazar, V., Benard, J., Fimia, G. M., Piacentini, M., Harper, F., Pierron, G., Vicencio, J. M., Bénit, P., De Andrade, A., Höglinger, G., Culmsee, C., ... Modjtahedi, N. (2010). A brain-specific isoform of mitochondrial apoptosis-inducing factor: AIF2. Cell Death and Differentiation, 17(7), 1155-1166. https://doi.org/10.1038/cdd.2009.211

@article{5ee5673bffba40ae8c9c9aacfc948eb2,

title = "A brain-specific isoform of mitochondrial apoptosis-inducing factor: AIF2",

abstract = "Apoptosis-inducing factor (AIF) has important supportive as well as potentially lethal roles in neurons. Under normal physiological conditions, AIF is a vital redox-active mitochondrial enzyme, whereas in pathological situations, it translocates from mitochondria to the nuclei of injured neurons and mediates apoptotic chromatin condensation and cell death. In this study, we reveal the existence of a brain-specific isoform of AIF, AIF2, whose expression increases as neuronal precursor cells differentiate. AIF2 arises from the utilization of the alternative exon 2b, yet uses the same remaining 15 exons as the ubiquitous AIF1 isoform. AIF1 and AIF2 are similarly imported to mitochondria in which they anchor to the inner membrane facing the intermembrane space. However, the mitochondrial inner membrane sorting signal encoded in the exon 2b of AIF2 is more hydrophobic than that of AIF1, indicating a stronger membrane anchorage of AIF2 than AIF1. AIF2 is more difficult to be desorbed from mitochondria than AIF1 on exposure to non-ionic detergents or basic pH. Furthermore, AIF2 dimerizes with AIF1, thereby preventing its release from mitochondria. Conversely, it is conceivable that a neuron-specific AIF isoform, AIF2, may have been designed to be retained in mitochondria and to minimize its potential neurotoxic activity.",

keywords = "Brain development, Neural differentiation, Neural progenitor, Neuroblastoma, Oxidative phosphorylation",

author = "E. Hangen and {De Zio}, D. and M. Bordi and C. Zhu and P. Dessen and F. Caffin and S. Lachkar and Perfettini, {J. L.} and V. Lazar and J. Benard and Fimia, {G. M.} and M. Piacentini and F. Harper and G. Pierron and Vicencio, {J. M.} and P. B{\'e}nit and {De Andrade}, A. and G. H{\"o}glinger and C. Culmsee and P. Rustin and K. Blomgren and F. Cecconi and G. Kroemer and N. Modjtahedi",

note = "Funding Information: Acknowledgements. EH is supported by a fellowship from the Ligue Nationale contre le Cancer. GK is supported by grants from European Union (projects Apo-Sys, ChemoRes, Death-Train), La Ligue Nationale Contre le Cancer ({\'e}quipe lab{\'e}lis{\'e}e), Institut National du Cancer (INCa), Agence Nationale de Recherche (ANR). FC is supported by grants from the Telethon Foundation, AIRC and the Italian Ministry of University and Research. PB and PR are supported by grants from European Union (project EumitoCombat), Leducq foundation. GH is supported by the German National Genome Research Network (01GS08136-4). We acknowledge the DTP at NCI for providing RNA samples for NCI60 panel of cancer cell lines; Marcel Leist, University of Konstanz, Germany for providing the LUHMES cells; Abdelali Jalil, Didier M{\'e}tivier and Fulvio Florenzano for help with flow cytometry and confocal microscopy; Eric Jacquet and Imagif (CNRS) Platform for quantitative RT-PCR analyses.",

year = "2010",

month = jul,

doi = "10.1038/cdd.2009.211",

language = "English",

volume = "17",

pages = "1155--1166",

journal = "Cell Death and Differentiation",

issn = "1350-9047",

publisher = "Springer Nature",

number = "7",

}

Hangen, E, De Zio, D, Bordi, M, Zhu, C, Dessen, P, Caffin, F, Lachkar, S, Perfettini, JL, Lazar, V, Benard, J, Fimia, GM, Piacentini, M, Harper, F, Pierron, G, Vicencio, JM, Bénit, P, De Andrade, A, Höglinger, G, Culmsee, C, Rustin, P, Blomgren, K, Cecconi, F, Kroemer, G & Modjtahedi, N 2010, 'A brain-specific isoform of mitochondrial apoptosis-inducing factor: AIF2', Cell Death and Differentiation, Jg. 17, Nr. 7, S. 1155-1166. https://doi.org/10.1038/cdd.2009.211

TY - JOUR

T1 - A brain-specific isoform of mitochondrial apoptosis-inducing factor

T2 - AIF2

AU - Hangen, E.

AU - De Zio, D.

AU - Bordi, M.

AU - Zhu, C.

AU - Dessen, P.

AU - Caffin, F.

AU - Lachkar, S.

AU - Perfettini, J. L.

AU - Lazar, V.

AU - Benard, J.

AU - Fimia, G. M.

AU - Piacentini, M.

AU - Harper, F.

AU - Pierron, G.

AU - Vicencio, J. M.

AU - Bénit, P.

AU - De Andrade, A.

AU - Höglinger, G.

AU - Culmsee, C.

AU - Rustin, P.

AU - Blomgren, K.

AU - Cecconi, F.

AU - Kroemer, G.

AU - Modjtahedi, N.

N1 - Funding Information: Acknowledgements. EH is supported by a fellowship from the Ligue Nationale contre le Cancer. GK is supported by grants from European Union (projects Apo-Sys, ChemoRes, Death-Train), La Ligue Nationale Contre le Cancer (équipe labélisée), Institut National du Cancer (INCa), Agence Nationale de Recherche (ANR). FC is supported by grants from the Telethon Foundation, AIRC and the Italian Ministry of University and Research. PB and PR are supported by grants from European Union (project EumitoCombat), Leducq foundation. GH is supported by the German National Genome Research Network (01GS08136-4). We acknowledge the DTP at NCI for providing RNA samples for NCI60 panel of cancer cell lines; Marcel Leist, University of Konstanz, Germany for providing the LUHMES cells; Abdelali Jalil, Didier Métivier and Fulvio Florenzano for help with flow cytometry and confocal microscopy; Eric Jacquet and Imagif (CNRS) Platform for quantitative RT-PCR analyses.

PY - 2010/7

Y1 - 2010/7

N2 - Apoptosis-inducing factor (AIF) has important supportive as well as potentially lethal roles in neurons. Under normal physiological conditions, AIF is a vital redox-active mitochondrial enzyme, whereas in pathological situations, it translocates from mitochondria to the nuclei of injured neurons and mediates apoptotic chromatin condensation and cell death. In this study, we reveal the existence of a brain-specific isoform of AIF, AIF2, whose expression increases as neuronal precursor cells differentiate. AIF2 arises from the utilization of the alternative exon 2b, yet uses the same remaining 15 exons as the ubiquitous AIF1 isoform. AIF1 and AIF2 are similarly imported to mitochondria in which they anchor to the inner membrane facing the intermembrane space. However, the mitochondrial inner membrane sorting signal encoded in the exon 2b of AIF2 is more hydrophobic than that of AIF1, indicating a stronger membrane anchorage of AIF2 than AIF1. AIF2 is more difficult to be desorbed from mitochondria than AIF1 on exposure to non-ionic detergents or basic pH. Furthermore, AIF2 dimerizes with AIF1, thereby preventing its release from mitochondria. Conversely, it is conceivable that a neuron-specific AIF isoform, AIF2, may have been designed to be retained in mitochondria and to minimize its potential neurotoxic activity.

AB - Apoptosis-inducing factor (AIF) has important supportive as well as potentially lethal roles in neurons. Under normal physiological conditions, AIF is a vital redox-active mitochondrial enzyme, whereas in pathological situations, it translocates from mitochondria to the nuclei of injured neurons and mediates apoptotic chromatin condensation and cell death. In this study, we reveal the existence of a brain-specific isoform of AIF, AIF2, whose expression increases as neuronal precursor cells differentiate. AIF2 arises from the utilization of the alternative exon 2b, yet uses the same remaining 15 exons as the ubiquitous AIF1 isoform. AIF1 and AIF2 are similarly imported to mitochondria in which they anchor to the inner membrane facing the intermembrane space. However, the mitochondrial inner membrane sorting signal encoded in the exon 2b of AIF2 is more hydrophobic than that of AIF1, indicating a stronger membrane anchorage of AIF2 than AIF1. AIF2 is more difficult to be desorbed from mitochondria than AIF1 on exposure to non-ionic detergents or basic pH. Furthermore, AIF2 dimerizes with AIF1, thereby preventing its release from mitochondria. Conversely, it is conceivable that a neuron-specific AIF isoform, AIF2, may have been designed to be retained in mitochondria and to minimize its potential neurotoxic activity.

KW - Brain development

KW - Neural differentiation

KW - Neural progenitor

KW - Neuroblastoma

KW - Oxidative phosphorylation

UR - http://www.scopus.com/inward/record.url?scp=77953616608&partnerID=8YFLogxK

U2 - 10.1038/cdd.2009.211

DO - 10.1038/cdd.2009.211

M3 - Article

C2 - 20111043

AN - SCOPUS:77953616608

SN - 1350-9047

VL - 17

SP - 1155

EP - 1166

JO - Cell Death and Differentiation

JF - Cell Death and Differentiation

IS - 7

ER -

A brain-specific isoform of mitochondrial apoptosis-inducing factor: AIF2

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