In situ architecture of Opa1-dependent mitochondrial cristae remodeling
pmc: PMC9882235 , PMC10897290
handle: 1721.1/153403
In situ architecture of Opa1-dependent mitochondrial cristae remodeling
AbstractCristae membrane state plays a central role in regulating mitochondrial function and cellular metabolism. The protein Optic atrophy 1 (Opa1) is an important crista remodeler that exists as two forms in the mitochondrion, a membrane-anchored long form (l-Opa1) and a processed short form (s-Opa1). The mechanisms for how Opa1 influences cristae shape have remained unclear due to lack of native three-dimensional views of cristae. We perform in situ cryo-electron tomography of cryo-focused ion beam milled mouse embryonic fibroblasts with defined Opa1 states to understand how each form of Opa1 influences cristae architecture. In our tomograms, we observe a variety of cristae shapes with distinct trends dependent on s-Opa1:l-Opa1 balance. Increased l-Opa1 levels promote cristae stacking and elongated mitochondria, while increased s-Opa1 levels correlated with irregular cristae packing and round mitochondria shape. Functional assays indicate a role for l-Opa1 in wild-type apoptotic and calcium handling responses, and show a compromised respiratory function under Opa1 imbalance. In summary, we provide three-dimensional visualization of cristae architecture to reveal relationships between mitochondrial ultrastructure and cellular function dependent on Opa1-mediated membrane remodeling.
- MASSACHUSETTS GENERAL HOSPITAL
- ECOLE POLYTECHNIQUE FEDERALE DE LAUSANNE Switzerland
- Chinese Academy of Sciences China (People's Republic of)
- Harvard Medical School United States
- Massachusetts General Hospital United States
Mitochondrial Proteins, Mice, Mitochondrial Membranes, Animals, Fibroblasts, Article, Mitochondria
Mitochondrial Proteins, Mice, Mitochondrial Membranes, Animals, Fibroblasts, Article, Mitochondria
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