Reduced ER-mitochondria Connectivity Promotes Neuroblastoma Multidrug Resistance

Overview

Journal EMBO J

Specialties Biotechnology
Molecular Biology

Date 2022 Feb 25

PMID 35211994

Authors

Jorida Coku

David M Booth

Jan Skoda

Madison C Pedrotty

Jennifer Vogel

Kangning Liu

Annette Vu

Erica L Carpenter

Jamie C Ye

Michelle A Chen

Peter Dunbar

Elizabeth Scadden

Taekyung D Yun

Eiko Nakamaru-Ogiso

Estela Area-Gomez

Yimei Li

Kelly C Goldsmith

C Patrick Reynolds

Gyorgy Hajnoczky

Michael D Hogarty

Affiliations

Soon will be listed here.

Abstract

Most cancer deaths result from progression of therapy resistant disease, yet our understanding of this phenotype is limited. Cancer therapies generate stress signals that act upon mitochondria to initiate apoptosis. Mitochondria isolated from neuroblastoma cells were exposed to tBid or Bim, death effectors activated by therapeutic stress. Multidrug-resistant tumor cells obtained from children at relapse had markedly attenuated Bak and Bax oligomerization and cytochrome c release (surrogates for apoptotic commitment) in comparison with patient-matched tumor cells obtained at diagnosis. Electron microscopy identified reduced ER-mitochondria-associated membranes (MAMs; ER-mitochondria contacts, ERMCs) in therapy-resistant cells, and genetically or biochemically reducing MAMs in therapy-sensitive tumors phenocopied resistance. MAMs serve as platforms to transfer Ca and bioactive lipids to mitochondria. Reduced Ca transfer was found in some but not all resistant cells, and inhibiting transfer did not attenuate apoptotic signaling. In contrast, reduced ceramide synthesis and transfer was common to resistant cells and its inhibition induced stress resistance. We identify ER-mitochondria-associated membranes as physiologic regulators of apoptosis via ceramide transfer and uncover a previously unrecognized mechanism for cancer multidrug resistance.

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