Mitochondrial Bcl-xL promotes brain synaptogenesis by controlling non-lethal caspase activation - CRCL-Signalisation, métabolisme et progression tumorale
Article Dans Une Revue iScience Année : 2023

Mitochondrial Bcl-xL promotes brain synaptogenesis by controlling non-lethal caspase activation

Résumé

Non-lethal caspase activation (NLCA) has been linked to neurodevelopmental processes. However, how neurons control NLCA remains elusive. Here, we focused on Bcl-xL, a Bcl-2 homolog regulating caspase activation through the mitochondria. We generated a mouse model, referred to as ER-xL, in which Bcl-xL is absent in the mitochondria, yet present in the endoplasmic reticulum. Unlike bclx knockout mice that died at E13.5, ER-xL mice survived embryonic development but died post-partum because of altered feeding behavior. Enhanced caspase-3 activity was observed in the brain and the spinal cord white matter, but not the gray matter. No increase in cell death was observed in ER-xL cortical neurons, suggesting that the observed caspase-3 activation was apoptosis-independent. ER-xL neurons displayed increased caspase-3 activity in the neurites, resulting in impaired axon arborescence and synaptogenesis. Together, our findings suggest that mitochondrial Bcl-xL finely tunes caspase-3 through Drp-1-dependent mitochondrial fission, which is critical to neural network design.
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Dates et versions

hal-04121358 , version 1 (21-08-2023)

Identifiants

Citer

Trang Thi Minh Nguyen, Rudy Gadet, Marine Lanfranchi, Romane Lahaye, Sozerko Yandiev, et al.. Mitochondrial Bcl-xL promotes brain synaptogenesis by controlling non-lethal caspase activation. iScience, 2023, 26 (5), pp.106674. ⟨10.1016/j.isci.2023.106674⟩. ⟨hal-04121358⟩
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