Loss of function CHCHD10 mutations in cytoplasmic TDP-43 accumulation and synaptic integrity

Woo, Jung A.; Liu, Tian; Trotter, Courtney; Fang, Cenxiao; Narvaez, Emillio De; LePochat, Patrick; Maslar, Drew; Bukhari, Anusha; Zhao, Xiaona; Deonarine, Andrew; Westerheide, Sandy D.; Kang, David E.

doi:10.1038/ncomms15558

Cited by 90 publications

(152 citation statements)

References 45 publications

(99 reference statements)

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“…Even stronger clustering was observed for G66V and E127K in nearly all cells. Other variants in the hydrophobic domain had little (G58R and G66S) or no effect (V57E) on CHCHD10 localization but may have subtle effects on mitochondrial morphology similar to reports for S59L (Bannwarth et al , ; Woo et al , ). The other variants showed no gross abnormalities in expression level and localization by immunofluorescence (Fig EV3), highlighting the importance of the hydrophobic region and the CHCH domain.…”

Section: Resultssupporting

confidence: 74%

“…Patient fibroblasts with the S59L mutation show an altered mitochondrial network structure, but as mitochondrial fusion is normal, this may be secondary to instability of mitochondrial DNA (Bannwarth et al , ). Overexpression of human wild‐type but not R15L or S59L CHCHD10 rescues the shorter lifespan of Caenorhabditis elegans lacking the CHCHD10 homolog har‐1 (Woo et al , ). The reported inhibition of apoptosis by CHCHD10 S59L (Genin et al , ) has not been replicated by others (Woo et al , ) and is difficult to reconcile with a neurodegenerative process.…”

Section: Introductionmentioning

confidence: 99%

“…Overexpression of human wild‐type but not R15L or S59L CHCHD10 rescues the shorter lifespan of Caenorhabditis elegans lacking the CHCHD10 homolog har‐1 (Woo et al , ). The reported inhibition of apoptosis by CHCHD10 S59L (Genin et al , ) has not been replicated by others (Woo et al , ) and is difficult to reconcile with a neurodegenerative process. The neuropathological features of CHCHD10 cases have not been comprehensively characterized, but CHCHD10 was recently linked to synaptic integrity and nuclear retention of TDP‐43 (Woo et al , ), although the latter has not been replicated (Brockmann et al , ).…”

Section: Introductionmentioning

confidence: 99%

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A novel CHCHD10 mutation implicates a Mia40‐dependent mitochondrial import deficit in ALS

et al. 2018

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CHCHD10 mutations are linked to amyotrophic lateral sclerosis, but their mode of action is unclear. In a 29‐year‐old patient with rapid disease progression, we discovered a novel mutation (Q108P) in a conserved residue within the coiled‐coil‐helix‐coiled‐coil‐helix (CHCH) domain. The aggressive clinical phenotype prompted us to probe its pathogenicity. Unlike the wild‐type protein, mitochondrial import of CHCHD10 Q108P was blocked nearly completely resulting in diffuse cytoplasmic localization and reduced stability. Other CHCHD10 variants reported in patients showed impaired mitochondrial import (C122R) or clustering within mitochondria (especially G66V and E127K) often associated with reduced expression. Truncation experiments suggest mitochondrial import of CHCHD10 is mediated by the CHCH domain rather than the proposed N‐terminal mitochondrial targeting signal. Knockdown of Mia40, which introduces disulfide bonds into CHCH domain proteins, blocked mitochondrial import of CHCHD10. Overexpression of Mia40 rescued mitochondrial import of CHCHD10 Q108P by enhancing disulfide‐bond formation. Since reduction in CHCHD10 inhibits respiration, mutations in its CHCH domain may cause aggressive disease by impairing mitochondrial import. Our data suggest Mia40 upregulation as a potential therapeutic salvage pathway.

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Section: Resultssupporting

confidence: 74%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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A novel CHCHD10 mutation implicates a Mia40‐dependent mitochondrial import deficit in ALS

et al. 2018

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“…In the nucleus CHCHD10 colocalizes with DAPI as suggested by a positive Pearson correlation coefficient. A recent study also showed nuclear localization (21). We further validated the nuclear signal by use of a stable knockdown of CHCHD10 in HEK293 cells (Fig.…”

Section: Chchd10 Is a Hypoxia-sensitive Genementioning

confidence: 87%

“…Thus, even in the presence of elevated levels of MNRR1 the two mutant versions of CHCHD10 prevent phosphorylation of MNRR1, giving rise to the mitochondrial phenotype seen. A recent study also showed that CHCHD10 is localized to both the mitochondria and the nucleus and that its normal function prevents the neurotoxic mitochondrial localization of the protein TDP-43 whereas two other disease associated mutations, R15L and S59L, promote its cytoplasmic mislocalization (21). These mutations have also been shown to accumulate excessive mitochondrial iron (37).…”

Section: Discussionmentioning

confidence: 99%

The cellular stress proteins CHCHD10 and MNRR1 (CHCHD2): Partners in mitochondrial and nuclear function and dysfunction

Purandare

Somayajulu

Hüttemann

et al. 2018

Journal of Biological Chemistry

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Coiled-coil-helix-coiled-coil-helix domaincontaining 10 (CHCHD10) and CHCHD2 (MNRR1) are homologous proteins with 58% sequence identity and belong to the twin CX 9 C family of proteins that mediate cellular stress responses. Despite the identification of several neurodegeneration-associated mutations in the CHCHD10 gene, few studies have assessed its physiological role. Here, we investigated CHCHD10's function as a regulator of oxidative phosphorylation in the mitochondria and the nucleus. We show that CHCHD10 co-purifies with cytochrome c oxidase (COX) and up-regulates COX activity by serving as a scaffolding protein required for MNRR1 phosphorylation, mediated by ARG (ABL proto-oncogene 2, non-receptor tyrosine kinase [ABL2]). The CHCHD10 gene was maximally transcribed in cultured cells at 8% oxygen, unlike MNRR1, which was maximally expressed at 4%, suggesting a fine-tuned oxygen-sensing system that adapts to the varying oxygen concentrations in the human body under physiological conditions. We show that nuclear CHCHD10 protein down-regulates the expression of genes harboring the oxygenresponsive element (ORE) in their promoters by interacting with and augmenting the activity of the largely uncharacterized transcriptional repressor CXXC finger protein 5 (CXXC5). We further show that two genetic CHCHD10 disease variants, G66V and P80L, in the mitochondria exhibit faulty interactions with MNRR1 and COX, reducing respiration and increasing reactive oxygen species (ROS), and in the nucleus abrogating transcriptional repression of ORE-containing genes. Our results reveal that CHCHD10 positively regulates mitochondrial respiration and contributes to transcriptional repression of ORE-containing genes in the nucleus, and that genetic CHCHD10 variants are impaired in these activities.CHCHD10 is a member of the twin CX 9 C family of proteins. This family, of which a number of members have displayed roles in disease (1), consists of proteins that contain two pairs of cysteine residues separated by 9 amino acids. These 4 cysteines form 2 disulfide bonds that stabilize the prototypical Coiled-coil Helix Coiled-coil Helix Domain (CHCHD) that traps CHCHD10 and other twin CX 9 C family members in the mitochondrial intermembrane space (IMS). Other members of this family include CHCHD4 (also called Mia40), necessary for import and proper folding of twin CX 9 C proteins in the IMS (2), and CHCHD3, which acts with CHCHD6 to stabilize mitochondrial cristae (3, 4). Another recently characterized member of this family is MNRR1 (Mitochondrial Nuclear Retrograde Regulator 1; also called CHCHD2), a protein that is upregulated under hypoxic stress, and maximally so at 4% oxygen. 2Besides residing in the mitochondria, MNRR1 is also present in the nucleus. Mitochondrial MNRR1 interacts with cytochrome c oxidase (COX) and is required for optimal enzyme function. A stable knockdown of MNRR1 resembles a mitochondrial disease phenotype with decreased oxygen consumption, decreased cellular growth and mitochondrial membrane potential,...

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mPOS is a novel mitochondrial trigger of cell death – implications for neurodegeneration

Coyne

Chen

2017

FEBS Letters

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In addition to its central role in energy metabolism, the mitochondrion has many other functions essential for cell survival. When stressed, the multifunctional mitochondria are expected to engender multifaceted cell stress with complex physiological consequences. Potential extra-mitochondrial proteostatic burdens imposed by inefficient protein import have been largely overlooked. Accumulating evidence suggests that a diverse range of pathogenic mitochondrial stressors, which do not directly target the core protein import machinery, can reduce cell fitness by disrupting the proteostatic network in the cytosol. The resulting stress, named mitochondrial precursor overaccumulation stress (mPOS), is characterized by the toxic accumulation of unimported mitochondrial proteins in the cytosol. Here, we review our current understanding of how mitochondrial dysfunction can impact the cytosolic proteome and proteostatic signaling. We also discuss the intriguing possibility that the mPOS model may help untangle the cause-effect relationship between mitochondrial dysfunction and cytosolic protein aggregation, which are probably the two most prominent molecular hallmarks of neurodegenerative disease.

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Loss of function CHCHD10 mutations in cytoplasmic TDP-43 accumulation and synaptic integrity

Cited by 90 publications

References 45 publications

A novel CHCHD10 mutation implicates a Mia40‐dependent mitochondrial import deficit in ALS

A novel CHCHD10 mutation implicates a Mia40‐dependent mitochondrial import deficit in ALS

The cellular stress proteins CHCHD10 and MNRR1 (CHCHD2): Partners in mitochondrial and nuclear function and dysfunction

mPOS is a novel mitochondrial trigger of cell death – implications for neurodegeneration

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