CLIC4 localizes to mitochondrial-associated membranes and mediates cardioprotection
Genre
Journal articleDate
2022-10-21Author
Ponnalagu, DevasenaHamilton, Shanna
Sanghvi, Shridhar
Antelo, Diego
Schwieterman, Neill
Hansra, Inderjot
Xu, Xianyao
Gao, Erhe
Edwards, John C.
Bansal, Shyam S.
Wold, Loren E.
Terentyev, Dmitry
Janssen, Paul M. L.
Hund, Thomas J.
Khan, Mahmood
Kohut, Andrew R.
Koch, Walter J.
Singh, Harpreet
Group
Center for Translational Medicine (Temple University)Permanent link to this record
http://hdl.handle.net/20.500.12613/9977
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http://dx.doi.org/10.1126/sciadv.abo1244Abstract
Mitochondrial-associated membranes (MAMs) are known to modulate organellar and cellular functions and can subsequently affect pathophysiology including myocardial ischemia-reperfusion (IR) injury. Thus, identifying molecular targets in MAMs that regulate the outcome of IR injury will hold a key to efficient therapeutics. Here, we found chloride intracellular channel protein (CLIC4) presence in MAMs of cardiomyocytes and demonstrate its role in modulating ER and mitochondrial calcium homeostasis under physiological and pathological conditions. In a murine model, loss of CLIC4 increased myocardial infarction and substantially reduced cardiac function after IR injury. CLIC4 null cardiomyocytes showed increased apoptosis and mitochondrial dysfunction upon hypoxia-reoxygenation injury in comparison to wild-type cardiomyocytes. Overall, our results indicate that MAM-CLIC4 is a key mediator of cellular response to IR injury and therefore may have a potential implication on other pathophysiological processes.Citation
Devasena Ponnalagu et al. ,CLIC4 localizes to mitochondrial-associated membranes and mediates cardioprotection.Sci. Adv.8,eabo1244(2022).DOI:10.1126/sciadv.abo1244Citation to related work
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Science Advances, Vol. 8, Iss. 42ADA compliance
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