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DRP1 levels determine the apoptotic threshold during embryonic differentiation through a mitophagy-dependent mechanism.

Title: DRP1 levels determine the apoptotic threshold during embryonic differentiation through a mitophagy-dependent mechanism.
Authors: Pernaute, B; Pérez-Montero, S; Sánchez Nieto, JM; Di Gregorio, A; Lima, A; Lawlor, K; Bowling, S; Liccardi, G; Tomás, A; Meier, P; Sesaki, H; Rutter, GA; Barbaric, I; Rodríguez, TA
Contributors: Meier, Pascal
Publisher Information: CELL PRESS
Publication Year: 2022
Collection: The Institute of Cancer Research (ICR): Publications Repository
Subject Terms: apoptosis; early development; embryonic stem cell differentiation; mitochondrial dynamics; mitophagy; pluripotency; Animals; Dynamins; Mammals; Mice; Mitochondria
Subject Geographic: United States
Description: The changes that drive differentiation facilitate the emergence of abnormal cells that need to be removed before they contribute to further development or the germline. Consequently, in mice in the lead-up to gastrulation, ∼35% of embryonic cells are eliminated. This elimination is caused by hypersensitivity to apoptosis, but how it is regulated is poorly understood. Here, we show that upon exit of naive pluripotency, mouse embryonic stem cells lower their mitochondrial apoptotic threshold, and this increases their sensitivity to cell death. We demonstrate that this enhanced apoptotic response is induced by a decrease in mitochondrial fission due to a reduction in the activity of dynamin-related protein 1 (DRP1). Furthermore, we show that in naive pluripotent cells, DRP1 prevents apoptosis by promoting mitophagy. In contrast, during differentiation, reduced mitophagy levels facilitate apoptosis. Together, these results indicate that during early mammalian development, DRP1 regulation of mitophagy determines the apoptotic response.
Document Type: article in journal/newspaper
File Description: Print-Electronic; 1330.e7; application/pdf
Language: English
ISSN: 1878-1551; 1534-5807
Relation: S1534-5807(22)00306-9; Developmental Cell, 2022, 57 (11), pp. 1316 - 1330.e7; https://repository.icr.ac.uk/handle/internal/5303
DOI: 10.1016/j.devcel.2022.04.020
Availability: https://doi.org/10.1016/j.devcel.2022.04.020; https://repository.icr.ac.uk/handle/internal/5303
Rights: http://creativecommons.org/licenses/by/4.0/
Accession Number: edsbas.E4893853
Database: BASE