Apoptotic caspases cleave DRP1 to promote mitochondrial fusion and anti-viral immune responses

  1. Yujie Fang
  2. Zihan Guan
  3. Xiangtao Zhu
  4. Zhenqiong Guan
  5. Shufen Li
  6. Ke Peng

  • Curated by eLife

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    This manuscript describes an unexpected role of cellular caspases in cleaving Drp1, a protein involved in mitochondrial fission, in virus-infected cells. Drp1 cleavage augments mitochondrial fission, reinforcing MAVS-dependent type-1 IFN response against multiple viruses. The findings presented in this manuscript are important and the strength of evidence is solid. Additional studies may allow for more robust mechanistic substantiation of the proposed model.

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Abstract

Apoptosis has been recognized as a suicidal host-defense programmed cell death pathway against invading pathogens. However, recent evidences showed that viruses can employ caspases to cleave and inactivate immune signaling molecules to facilitate infection. Whether caspases can promote anti-viral immune responses is currently unknown. Here, we demonstrated that the NSs protein of RVFV triggers activation of apoptotic caspases, which cleave the mitochondrial fission factor DRP1 resulting in mitochondrial elongation. Elongated mitochondria promote MAVS aggregation leading to enhanced anti-viral immunity. Apoptotic caspases, including caspase-3, -6, -7 and -8, cleave DRP1 at the motifs of D 500 FAD 503 and/or AEAD 556 , suggesting that this cleavage event may occur during infection of different viruses. Indeed, infection of H1N1, SeV and HSV-1 all triggered apoptotic caspases activation to cleave DRP1 promoting anti-viral immune responses. Compared with wild-type DRP1, introduction of caspase-resistant DRP1 strongly attenuated immune responses triggered by virus infection. These results revealed a novel mechanism through which apoptotic caspases promote anti-viral immunity by regulating mitochondrial morphodynamics.

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  1. Version published to 10.7554/elife.101190.1 on eLife
  2. Version published to 10.7554/elife.101190 on eLife
  3. eLife

    eLife assessment

    This manuscript describes an unexpected role of cellular caspases in cleaving Drp1, a protein involved in mitochondrial fission, in virus-infected cells. Drp1 cleavage augments mitochondrial fission, reinforcing MAVS-dependent type-1 IFN response against multiple viruses. The findings presented in this manuscript are important and the strength of evidence is solid. Additional studies may allow for more robust mechanistic substantiation of the proposed model.

  4. eLife

    Reviewer #1 (Public Review):

    Drp1 supports mitochondrial fission (doi: 10.1038/s41586-019-1296-y). Viral sensing triggers mitochondrial fusion, leading to MAVS aggregation and improved type-1 IFN response. It was suggested that impairment of Drp1 upon phosphorylation by Tbk1 enhances mitochondrial fusion in virus-infected cells (doi.org/10.1016/j.molcel.2020.10.018). In this manuscript, Fang et al. describe an unexpected role of caspases activated upon Rift Valley fever virus (RVFV) infection in inactivating Drp1. They show that Drp1 is targeted by multiple caspases, including caspase-3, -6, -7 and -8. Indeed, cleavage of Drp1 leads to mitochondrial elongation, boosting the type-1 IFN response of infected cells. Finally, the authors establish the generalisability of the proposed mechanism in the context of cellular infections with H1N1, SeV, and HSV-1. Caspase-dependent and independent cell death processes provide important host defence mechanisms against obligatorily intracellular viral pathogens. This work suggests that caspases reinforce antiviral response involving also the mitochondria-type 1 IFN axis. As such, the manuscript is well written, and the proposal pertaining to caspase-mediated targeting of Drp1 may have implications beyond host-virus interaction studies. However, several loose ends remain, and these concerns need to be addressed to substantiate the mechanistic model.

  5. eLife

    Reviewer #2 (Public Review):

    In the present study, authors report the role of virus-induced apoptosis in positively regulating the innate immune response. Upon infection, host cell apoptosis is triggered as a defence mechanism against virus replication. Culmination of infected-cell death impairs replicative potential for viruses, hence attenuating virus propagation. Reports exist denoting the inhibitory effect of apoptosis upon innate immune signalling. Contrary to that, the findings of this manuscript underscore the possible role of apoptosis in enhancing innate immune signalling and effector response. Infection-induced activation of caspases (3, 6, 7, and 8) has been demonstrated to cleave DRP1 protein. DRP1, a positive regulator for mitochondrial fission, degradation leads to altered mitochondrial morphology (elongation).

    Mitochondria, being a hub for innate immune signalling (via operation of RLR-MAVS-downstream effector molecule-axis), upon elongation as a result of DRP1 depletion, results in greater innate immune signal flux and interferon induction. Increased interferon induction thus acts to inhibit virus propagation, as demonstrated by the authors using cell-culture models.

    Strengths:

    (1) The findings presented by the authors have been validated by employing elaborate biochemical experimental approaches. The study entails extensive biochemical characterization of DRP1 residues targeted by activated caspases, in vitro assays validating caspase-mediated DRP1 cleavage & caspase-DRP1 interaction.

    (2) This study possesses broad implications since the authors demonstrate the role of caspase-mediated DRP1 cleavage in promoting innate immunity in the context of infection by diverse viruses (both RNA and DNA viruses).

    Weaknesses:

    Although the authors undertook a thorough experimental approach attempting to validate their findings, all the experiments were performed using either cell-culture models for infection or in vitro biochemical assays (cleavage and protein-protein interaction). Additional experimentation using animal models (in vivo) will further help strengthen the biological significance of their findings under more physiological settings.

  6. eLife

    Reviewer #3 (Public Review):

    Summary:

    The authors demonstrated that the NSs protein of RVFV triggers the activation of apoptotic caspases, which cleave the mitochondrial fission factor DRP1 resulting in mitochondrial elongation.

    Strengths:

    The manuscript provides an insightful investigation into a novel mechanism through which apoptotic caspases promote anti-viral immunity by regulating mitochondrial morphodynamics.

  7. Version published to 10.1101/2024.07.13.603409v1 on bioRxiv