Citrin mediated metabolic rewiring in response to altered basal subcellular Ca2+ homeostasis

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作者
Zhanat Koshenov
Furkan E. Oflaz
Martin Hirtl
Benjamin Gottschalk
Rene Rost
Roland Malli
Wolfgang F. Graier
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[1] Medical University of Graz,Molecular Biology and Biochemistry, Gottfried Schatz Research Center
[2] BioTechMed Graz,undefined
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In contrast to long-term metabolic reprogramming, metabolic rewiring represents an instant and reversible cellular adaptation to physiological or pathological stress. Ca2+ signals of distinct spatio-temporal patterns control a plethora of signaling processes and can determine basal cellular metabolic setting, however, Ca2+ signals that define metabolic rewiring have not been conclusively identified and characterized. Here, we reveal the existence of a basal Ca2+ flux originating from extracellular space and delivered to mitochondria by Ca2+ leakage from inositol triphosphate receptors in mitochondria-associated membranes. This Ca2+ flux primes mitochondrial metabolism by maintaining glycolysis and keeping mitochondria energized for ATP production. We identified citrin, a well-defined Ca2+-binding component of malate-aspartate shuttle in the mitochondrial intermembrane space, as predominant target of this basal Ca2+ regulation. Our data emphasize that any manipulation of this ubiquitous Ca2+ system has the potency to initiate metabolic rewiring as an instant and reversible cellular adaptation to physiological or pathological stress.
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