OPA1 and MICOS Regulate mitochondrial crista dynamics and formation

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作者
Chao Hu
Li Shu
Xiaoshuai Huang
Jianglong Yu
liuju Li
Longlong Gong
Meigui Yang
Zhida Wu
Zhi Gao
Yungang Zhao
Liangyi Chen
Zhiyin Song
机构
[1] Hubei Key Laboratory of Cell Homeostasis,
[2] Frontier Science Center for Immunology and Metabolism,undefined
[3] College of Life Sciences,undefined
[4] Wuhan University,undefined
[5] State Key Laboratory of Membrane Biology,undefined
[6] Beijing Key Laboratory of Cardiometabolic Molecular Medicine,undefined
[7] Institute of Molecular Medicine,undefined
[8] Peking University,undefined
[9] Tianjin Key Laboratory of Exercise Physiology and Sports Medicine,undefined
[10] Institute of Sports and Health,undefined
[11] Tianjin Sport University,undefined
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摘要
Mitochondrial cristae are the main site for oxidative phosphorylation, which is critical for cellular energy production. Upon different physiological or pathological stresses, mitochondrial cristae undergo remodeling to reprogram mitochondrial function. However, how mitochondrial cristae are formed, maintained, and remolded is still largely unknown due to the technical challenges of tracking mitochondrial crista dynamics in living cells. Here, using live-cell Hessian structured illumination microscopy combined with transmission electron microscopy, focused ion beam/scanning electron microscopy, and three-dimensional tomographic reconstruction, we show, in living cells, that mitochondrial cristae are highly dynamic and undergo morphological changes, including elongation, shortening, fusion, division, and detachment from the mitochondrial inner boundary membrane (IBM). In addition, we find that OPA1, Yme1L, MICOS, and Sam50, along with the newly identified crista regulator ATAD3A, control mitochondrial crista dynamics. Furthermore, we discover two new types of mitochondrial crista in dysfunctional mitochondria, “cut-through crista” and “spherical crista”, which are formed due to incomplete mitochondrial fusion and dysfunction of the MICOS complex. Interestingly, cut-through crista can convert to “lamellar crista”. Overall, we provide a direct link between mitochondrial crista formation and mitochondrial crista dynamics.
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