Bcl2L13 is a ceramide synthase inhibitor in glioblastoma

Samuel A. Jensen; Andrea E. Calvert; Giora Volpert; Fotini M. Kouri; Lisa A. Hurley; Janina P. Luciano; Yongfei Wu; Alexandra Chalastanis; Anthony H. Futerman; Alexander H. Stegh

doi:10.1073/pnas.1316700111

Bcl2L13 is a ceramide synthase inhibitor in glioblastoma

Samuel A. Jensen, Andrea E. Calvert, Giora Volpert, Fotini M. Kouri, Lisa A. Hurley, Janina P. Luciano, Yongfei Wu, Alexandra Chalastanis, Anthony H. Futerman, Alexander H. Stegh

Department of Biomolecular Sciences

Weizmann Institute of Science

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

Abstract

Therapy resistance is a major limitation to the successful treatment of cancer. Here, we identify Bcl2-like 13 (Bcl2L13), an atypical member of the Bcl-2 family, as a therapy susceptibility gene with elevated expression in solid and blood cancers, including glioblastoma (GBM). We demonstrate that mitochondria-Associated Bcl2L13 inhibits apoptosis induced by a wide spectrum of chemo- and targeted therapies upstream of Bcl2-Associated X protein activation and mitochondrial outer membrane permeabilization in vitro and promotes GBM tumor growth in vivo. Mechanistically, Bcl2L13 binds to proapoptotic ceramide synthases 2 (CerS2) and 6 (CerS6) via a unique C-terminal 250-Aa sequence located between its Bcl-2 homology and membrane anchor domains and blocks homo- and heteromeric CerS2/6 complex formation and activity. Correspondingly, CerS2/6 activity and Bcl2L13 abundance are inversely correlated in GBM tumors. Thus, our genetic and functional studies identify Bcl2L13 as a regulator of therapy susceptibility and point to the Bcl2L13-CerS axis as a promising target to enhance responses of therapy-refractory cancers toward conventional and targeted regimens currently in clinical use.

Original language	English
Pages (from-to)	5682-5687
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	111
Issue number	15
DOIs	https://doi.org/10.1073/pnas.1316700111
State	Published - 15 Apr 2014

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@article{2f9a197af240420cb84e745382feca00,

title = "Bcl2L13 is a ceramide synthase inhibitor in glioblastoma",

abstract = "Therapy resistance is a major limitation to the successful treatment of cancer. Here, we identify Bcl2-like 13 (Bcl2L13), an atypical member of the Bcl-2 family, as a therapy susceptibility gene with elevated expression in solid and blood cancers, including glioblastoma (GBM). We demonstrate that mitochondria-Associated Bcl2L13 inhibits apoptosis induced by a wide spectrum of chemo- and targeted therapies upstream of Bcl2-Associated X protein activation and mitochondrial outer membrane permeabilization in vitro and promotes GBM tumor growth in vivo. Mechanistically, Bcl2L13 binds to proapoptotic ceramide synthases 2 (CerS2) and 6 (CerS6) via a unique C-terminal 250-Aa sequence located between its Bcl-2 homology and membrane anchor domains and blocks homo- and heteromeric CerS2/6 complex formation and activity. Correspondingly, CerS2/6 activity and Bcl2L13 abundance are inversely correlated in GBM tumors. Thus, our genetic and functional studies identify Bcl2L13 as a regulator of therapy susceptibility and point to the Bcl2L13-CerS axis as a promising target to enhance responses of therapy-refractory cancers toward conventional and targeted regimens currently in clinical use.",

author = "Jensen, {Samuel A.} and Calvert, {Andrea E.} and Giora Volpert and Kouri, {Fotini M.} and Hurley, {Lisa A.} and Luciano, {Janina P.} and Yongfei Wu and Alexandra Chalastanis and Futerman, {Anthony H.} and Stegh, {Alexander H.}",

note = "National Cancer Center (NCI) [P30 CA060553]; American Cancer Society, Illinois division; Israel Science Foundation [0888/11]; NCI/National Institutes of Health Training Grant [T32CA09560]; Dixon Translational Research Grants Initiative of the Northwestern Memorial Foundation; James S. MacDonnell 21st Century Initiative; Coffman Charitable Trust; Minerva Foundation; Malkin Scholars Programs of the Robert H. Lurie Comprehensive Cancer Center of Northwestern UniversityWe thank the Cell Imaging Facility, the Flow Cytometry Core Facility, and the Mouse Histology and Phenotyping Laboratory at Northwestern University, all of which are supported by National Cancer Center (NCI) Support Grant P30 CA060553 awarded to the Robert H. Lurie Comprehensive Cancer Center. This research was supported by a grant from the American Cancer Society, Illinois division (to A. H. S.); Israel Science Foundation Grant 0888/11 (to A. H. F.); NCI/National Institutes of Health Training Grant T32CA09560 (to S.A.J. and A. E. C.); the Dixon Translational Research Grants Initiative of the Northwestern Memorial Foundation, the James S. MacDonnell 21st Century Initiative, and the Coffman Charitable Trust (all A. H. S.); The Minerva Foundation (A. H. F.); and the Malkin Scholars Programs of the Robert H. Lurie Comprehensive Cancer Center of Northwestern University (S.A.J.).",

year = "2014",

month = apr,

day = "15",

doi = "10.1073/pnas.1316700111",

language = "الإنجليزيّة",

volume = "111",

pages = "5682--5687",

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TY - JOUR

T1 - Bcl2L13 is a ceramide synthase inhibitor in glioblastoma

AU - Jensen, Samuel A.

AU - Calvert, Andrea E.

AU - Volpert, Giora

AU - Kouri, Fotini M.

AU - Hurley, Lisa A.

AU - Luciano, Janina P.

AU - Wu, Yongfei

AU - Chalastanis, Alexandra

AU - Futerman, Anthony H.

AU - Stegh, Alexander H.

N1 - National Cancer Center (NCI) [P30 CA060553]; American Cancer Society, Illinois division; Israel Science Foundation [0888/11]; NCI/National Institutes of Health Training Grant [T32CA09560]; Dixon Translational Research Grants Initiative of the Northwestern Memorial Foundation; James S. MacDonnell 21st Century Initiative; Coffman Charitable Trust; Minerva Foundation; Malkin Scholars Programs of the Robert H. Lurie Comprehensive Cancer Center of Northwestern UniversityWe thank the Cell Imaging Facility, the Flow Cytometry Core Facility, and the Mouse Histology and Phenotyping Laboratory at Northwestern University, all of which are supported by National Cancer Center (NCI) Support Grant P30 CA060553 awarded to the Robert H. Lurie Comprehensive Cancer Center. This research was supported by a grant from the American Cancer Society, Illinois division (to A. H. S.); Israel Science Foundation Grant 0888/11 (to A. H. F.); NCI/National Institutes of Health Training Grant T32CA09560 (to S.A.J. and A. E. C.); the Dixon Translational Research Grants Initiative of the Northwestern Memorial Foundation, the James S. MacDonnell 21st Century Initiative, and the Coffman Charitable Trust (all A. H. S.); The Minerva Foundation (A. H. F.); and the Malkin Scholars Programs of the Robert H. Lurie Comprehensive Cancer Center of Northwestern University (S.A.J.).

PY - 2014/4/15

Y1 - 2014/4/15

N2 - Therapy resistance is a major limitation to the successful treatment of cancer. Here, we identify Bcl2-like 13 (Bcl2L13), an atypical member of the Bcl-2 family, as a therapy susceptibility gene with elevated expression in solid and blood cancers, including glioblastoma (GBM). We demonstrate that mitochondria-Associated Bcl2L13 inhibits apoptosis induced by a wide spectrum of chemo- and targeted therapies upstream of Bcl2-Associated X protein activation and mitochondrial outer membrane permeabilization in vitro and promotes GBM tumor growth in vivo. Mechanistically, Bcl2L13 binds to proapoptotic ceramide synthases 2 (CerS2) and 6 (CerS6) via a unique C-terminal 250-Aa sequence located between its Bcl-2 homology and membrane anchor domains and blocks homo- and heteromeric CerS2/6 complex formation and activity. Correspondingly, CerS2/6 activity and Bcl2L13 abundance are inversely correlated in GBM tumors. Thus, our genetic and functional studies identify Bcl2L13 as a regulator of therapy susceptibility and point to the Bcl2L13-CerS axis as a promising target to enhance responses of therapy-refractory cancers toward conventional and targeted regimens currently in clinical use.

AB - Therapy resistance is a major limitation to the successful treatment of cancer. Here, we identify Bcl2-like 13 (Bcl2L13), an atypical member of the Bcl-2 family, as a therapy susceptibility gene with elevated expression in solid and blood cancers, including glioblastoma (GBM). We demonstrate that mitochondria-Associated Bcl2L13 inhibits apoptosis induced by a wide spectrum of chemo- and targeted therapies upstream of Bcl2-Associated X protein activation and mitochondrial outer membrane permeabilization in vitro and promotes GBM tumor growth in vivo. Mechanistically, Bcl2L13 binds to proapoptotic ceramide synthases 2 (CerS2) and 6 (CerS6) via a unique C-terminal 250-Aa sequence located between its Bcl-2 homology and membrane anchor domains and blocks homo- and heteromeric CerS2/6 complex formation and activity. Correspondingly, CerS2/6 activity and Bcl2L13 abundance are inversely correlated in GBM tumors. Thus, our genetic and functional studies identify Bcl2L13 as a regulator of therapy susceptibility and point to the Bcl2L13-CerS axis as a promising target to enhance responses of therapy-refractory cancers toward conventional and targeted regimens currently in clinical use.

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U2 - 10.1073/pnas.1316700111

DO - 10.1073/pnas.1316700111

M3 - مقالة

SN - 0027-8424

VL - 111

SP - 5682

EP - 5687

JO - Proceedings of the National Academy of Sciences of the United States of America

JF - Proceedings of the National Academy of Sciences of the United States of America

IS - 15

ER -

Bcl2L13 is a ceramide synthase inhibitor in glioblastoma

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