Redox Nanodomains Are Induced by and Control Calcium Signaling at the ER-Mitochondrial Interface.

dc.contributor.author	Booth DM
dc.contributor.author	Enyedi Balázs
dc.contributor.author	Geiszt Miklós
dc.contributor.author	Várnai Péter
dc.contributor.author	Hajnoczky G
dc.date.accessioned	2018-07-05T06:54:44Z
dc.date.available	2018-07-05T06:54:44Z
dc.date.issued	2016
dc.identifier	84991109539
dc.identifier.citation	pagination=240-248; journalVolume=63; journalIssueNumber=2; journalTitle=MOLECULAR CELL;
dc.identifier.uri	http://repo.lib.semmelweis.hu//handle/123456789/4839
dc.identifier.uri	doi:10.1016/j.molcel.2016.05.040
dc.description.abstract	The ER-mitochondrial interface is central to calcium signaling, organellar dynamics, and lipid biosynthesis. The ER and mitochondrial membranes also host sources and targets of reactive oxygen species (ROS), but their local dynamics and relevance remained elusive since measurement and perturbation of ROS at the organellar interface has proven difficult. Employing drug-inducible synthetic ER-mitochondrial linkers, we overcame this problem and demonstrate that the ER-mitochondrial interface hosts a nanodomain of H2O2, which is induced by cytoplasmic [Ca(2+)] spikes and exerts a positive feedback on calcium oscillations. H2O2 nanodomains originate from the mitochondrial cristae, which are compressed upon calcium signal propagation to the mitochondria, likely due to Ca(2+)-induced K(+) and concomitant water influx to the matrix. Thus, ER-mitochondrial H2O2 nanodomains represent a component of inter-organelle communication, regulating calcium signaling and mitochondrial activities.
dc.relation.ispartof	urn:issn:1097-2765
dc.title	Redox Nanodomains Are Induced by and Control Calcium Signaling at the ER-Mitochondrial Interface.
dc.type	Journal Article
dc.date.updated	2018-02-19T12:03:35Z
dc.language.rfc3066	en
dc.identifier.mtmt	3112474
dc.identifier.wos	000381619300008
dc.identifier.pubmed	27397688