TBK1-Mediated DRP1 Targeting Confers Nucleic Acid Sensing to Reprogram Mitochondrial Dynamics and Physiology

Overview

Journal Mol Cell

Publisher Cell Press

Specialty Cell Biology

Date 2020 Nov 10

PMID 33171123

Citations 29

Authors

Shasha Chen

Shengduo Liu

Junxian Wang

Qirou Wu

Ailian Wang

Hongxin Guan

Qian Zhang

Dan Zhang

Xiaojian Wang

Hai Song

Jun Qin

Jian Zou

Zhengfan Jiang

Songying Ouyang

Xin-Hua Feng

Tingbo Liang

Pinglong Xu

Affiliations

Soon will be listed here.

Abstract

Mitochondrial morphology shifts rapidly to manage cellular metabolism, organelle integrity, and cell fate. It remains unknown whether innate nucleic acid sensing, the central and general mechanisms of monitoring both microbial invasion and cellular damage, can reprogram and govern mitochondrial dynamics and function. Here, we unexpectedly observed that upon activation of RIG-I-like receptor (RLR)-MAVS signaling, TBK1 directly phosphorylated DRP1/DNM1L, which disabled DRP1, preventing its high-order oligomerization and mitochondrial fragmentation function. The TBK1-DRP1 axis was essential for assembly of large MAVS aggregates and healthy antiviral immunity and underlay nutrient-triggered mitochondrial dynamics and cell fate determination. Knockin (KI) strategies mimicking TBK1-DRP1 signaling produced dominant-negative phenotypes reminiscent of human DRP1 inborn mutations, while interrupting the TBK1-DRP1 connection compromised antiviral responses. Thus, our findings establish an unrecognized function of innate immunity governing both morphology and physiology of a major organelle, identify a lacking loop during innate RNA sensing, and report an elegant mechanism of shaping mitochondrial dynamics.

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