Author
Listed:
- Yuan Lin
(Peking University
New York University School of Medicine)
- Lin-Lin Li
(Chinese Academy of Sciences)
- Wei Nie
(Peking University)
- Xiaolei Liu
(Chinese Academy of Sciences)
- Avital Adler
(New York University School of Medicine)
- Chi Xiao
(Chinese Academy of Sciences)
- Fujian Lu
(Peking University)
- Liping Wang
(Chinese Academy of Sciences)
- Hua Han
(Chinese Academy of Sciences)
- Xianhua Wang
(Peking University)
- Wen-Biao Gan
(New York University School of Medicine)
- Heping Cheng
(Peking University)
Abstract
Mitochondrial calcium ([Ca2+]mito) dynamics plays vital roles in regulating fundamental cellular and organellar functions including bioenergetics. However, neuronal [Ca2+]mito dynamics in vivo and its regulation by brain activity are largely unknown. By performing two-photon Ca2+ imaging in the primary motor (M1) and visual cortexes (V1) of awake behaving mice, we find that discrete [Ca2+]mito transients occur synchronously over somatic and dendritic mitochondrial network, and couple with cytosolic calcium ([Ca2+]cyto) transients in a probabilistic, rather than deterministic manner. The amplitude, duration, and frequency of [Ca2+]cyto transients constitute important determinants of the coupling, and the coupling fidelity is greatly increased during treadmill running (in M1 neurons) and visual stimulation (in V1 neurons). Moreover, Ca2+/calmodulin kinase II is mechanistically involved in modulating the dynamic coupling process. Thus, activity-dependent dynamic [Ca2+]mito-to-[Ca2+]cyto coupling affords an important mechanism whereby [Ca2+]mito decodes brain activity for the regulation of mitochondrial bioenergetics to meet fluctuating neuronal energy demands as well as for neuronal information processing.
Suggested Citation
Yuan Lin & Lin-Lin Li & Wei Nie & Xiaolei Liu & Avital Adler & Chi Xiao & Fujian Lu & Liping Wang & Hua Han & Xianhua Wang & Wen-Biao Gan & Heping Cheng, 2019.
"Brain activity regulates loose coupling between mitochondrial and cytosolic Ca2+ transients,"
Nature Communications, Nature, vol. 10(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:10:y:2019:i:1:d:10.1038_s41467-019-13142-0
DOI: 10.1038/s41467-019-13142-0
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