CHCHD4 confers metabolic vulnerabilities to tumour cells through its control of the mitochondrial respiratory chain

Thomas, Luke W.; Stephen, Jenna M.; Esposito, Cinzia; Hoer, Simon; Antrobus, Robin; Ahmed, Alaa A.; Al-Habib, Hasan; Ashcroft, Margaret

doi:10.1101/513770

Cited by 5 publications

(16 citation statements)

References 48 publications

(80 reference statements)

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“…2a). Notably, we and others have shown that loss of CHCHD4 leads to reduced levels of apoptosis-inducing factor (AIF) [30,32,33], a CHCHD4-interacting protein [33]. However, we found no obvious effect on the expression of AIF in CHCHD4 overexpressing cells (Additional file 2: Figure S2a).…”

Section: Chchd4-mediated Tumour Cell Growth and Mtorc1 Signalling Is mentioning

confidence: 63%

“…However, we found no obvious effect on the expression of AIF in CHCHD4 overexpressing cells (Additional file 2: Figure S2a). We and others have shown that CHCHD4 is a critical regulator of CI expression [30,33]. Further examination of CI activity using an in-gel nitrotetrazolium blue assay demonstrated increased CI activity in mitochondrial extracts from CHCHD4 (WT)-expressing cells (WT.cl1, WT.cl3), while whole CI activity was reduced in CHCHD4 (C66A/C68A)-expressing cells, compared to control U2OS cells ( Fig.…”

Section: Chchd4-mediated Tumour Cell Growth and Mtorc1 Signalling Is mentioning

confidence: 65%

“…CHCHD4 expression positively correlates with OXPHOS and proliferative pathways in tumours Recently, we have shown that elevated CHCHD4 expression in tumour cells increases tumour cell proliferation irrespective of oxygen levels [30]. To better understand the relationship between CHCHD4 and tumour cell proliferation, we carried out GSEA on genes that were significantly correlated with CHCHD4 expression in transcriptomic data from a panel of 967 tumour cell lines (Novartis/Broad Institute Tumour Cell Line Encyclopaedia).…”

Section: Resultsmentioning

confidence: 99%

“…Thus, we next investigated the relationship between CHCHD4-mediated regulation of OXPHOS and tumour cell growth. To do this, we used U2OS cells stably expressing wild-type CHCHD4 [CHCHD4 (WT)-expressing cells, clones WT.cl1, WT.cl3], or stably expressing a mutant form of CHCHD4 in which the substrate-binding cysteines of the CPC motif have been mutated to alanines (C66A/ C68A) described by us previously [28][29][30]. Consistent with our previous study [30], we found that elevated CHCHD4 expression led to increased expression of individual subunits of CI (NDUFS3), CII (SDHA), CIII (UQCRC2) and CIV (COXIV) ( Fig.…”

Section: Chchd4-mediated Tumour Cell Growth and Mtorc1 Signalling Is mentioning

confidence: 99%

“…One such pathway, the disulfide relay system (DRS), is responsible for the import and oxidative folding of small intermembrane space (IMS) proteins, which include subunits of CI and CIV, as well as assembly factors for CIII and CIV [25][26][27]. The substrate-binding oxidoreductase of the DRS is the redox-sensitive protein CHCHD4, which we have shown to regulate cellular oxygen consumption rate, and hypoxia-inducible factor (HIF) signalling [28][29][30]. We have shown that increased CHCHD4 expression in tumours correlates with increased tumour progression, and is associated with decreased patient survival and disease recurrence [28].…”

Section: Introductionmentioning

confidence: 99%

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CHCHD4 regulates tumour proliferation and EMT-related phenotypes, through respiratory chain-mediated metabolism

et al. 2019

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Background Mitochondrial oxidative phosphorylation (OXPHOS) via the respiratory chain is required for the maintenance of tumour cell proliferation and regulation of epithelial to mesenchymal transition (EMT)-related phenotypes through mechanisms that are not fully understood. The essential mitochondrial import protein coiled-coil helix coiled-coil helix domain-containing protein 4 (CHCHD4) controls respiratory chain complex activity and oxygen consumption, and regulates the growth of tumours in vivo. In this study, we interrogate the importance of CHCHD4-regulated mitochondrial metabolism for tumour cell proliferation and EMT-related phenotypes, and elucidate key pathways involved. Results Using in silico analyses of 967 tumour cell lines, and tumours from different cancer patient cohorts, we show that CHCHD4 expression positively correlates with OXPHOS and proliferative pathways including the mTORC1 signalling pathway. We show that CHCHD4 expression significantly correlates with the doubling time of a range of tumour cell lines, and that CHCHD4-mediated tumour cell growth and mTORC1 signalling is coupled to respiratory chain complex I (CI) activity. Using global metabolomics analysis, we show that CHCHD4 regulates amino acid metabolism, and that CHCHD4-mediated tumour cell growth is dependent on glutamine. We show that CHCHD4-mediated tumour cell growth is linked to CI-regulated mTORC1 signalling and amino acid metabolism. Finally, we show that CHCHD4 expression in tumours is inversely correlated with EMT-related gene expression, and that increased CHCHD4 expression in tumour cells modulates EMT-related phenotypes. Conclusions CHCHD4 drives tumour cell growth and activates mTORC1 signalling through its control of respiratory chain mediated metabolism and complex I biology, and also regulates EMT-related phenotypes of tumour cells. Electronic supplementary material The online version of this article (10.1186/s40170-019-0200-4) contains supplementary material, which is available to authorized users.

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Section: Chchd4-mediated Tumour Cell Growth and Mtorc1 Signalling Is mentioning

confidence: 63%

Section: Chchd4-mediated Tumour Cell Growth and Mtorc1 Signalling Is mentioning

confidence: 65%

Section: Resultsmentioning

confidence: 99%

Section: Chchd4-mediated Tumour Cell Growth and Mtorc1 Signalling Is mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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CHCHD4 regulates tumour proliferation and EMT-related phenotypes, through respiratory chain-mediated metabolism

et al. 2019

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USF1-CHCHD4 axis promotes lung adenocarcinoma progression partially via activating the MYC pathway

Zhou

Zhao

et al. 2022

Discov Onc

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Background This study aimed to identify genes related to lung adenocarcinoma (LUAD) and investigate the effects and molecular mechanisms of coiled-coil-helix-coiled-coil-helix domain containing 4 (CHCHD4) in the progression of LUAD. Methods The GEPIA database was used to evaluate the differential expression of CHCHD4 and the survival data of LUAD patients compared to controls. TCGA-LUAD database, JASPAR website, and GSEA were used to analyse the relationship between CHCHD4 and the upstream stimulating factor 1 (USF1) or MYC pathways. The proliferation, apoptosis, migration, and invasion of LUAD cells were evaluated using cell counting kit-8, 5-ethynyl-2′-deoxyuridine, colony formation, flow cytometry, wound healing, and transwell assays. qRT-PCR, western blotting, and immunohistochemistry were used to detect the mRNA and protein expression, respectively. Furthermore, xenograft tumours from nude mice were used to verify the effect of CHCHD4 on LUAD in vivo. Results CHCHD4 overexpression was found in LUAD tumor tissues and cells, and high CHCHD4 was associated with a poor prognosis. Interestingly, CHCHD4 knockdown suppressed the malignant phenotype of the LUAD cells. Moreover, we found that USF1 upregulated CHCHD4 and promoted LUAD progression. CHCHD4 knockdown also inhibited the progression of LUAD. In addition, CHCHD4 knockdown suppressed xenograft tumour growth. Conclusion USF1-CHCHD4 axis can promote LUAD progress, which may be through activating MYC pathway.

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Glutathionylated and Fe–S cluster containing hMIA40 (CHCHD4) regulates ROS and mitochondrial complex III and IV activities of the electron transport chain

et al. 2020

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Human MIA40, an i nter m embrane s pace (IMS) import receptor of mitochondria harbors twin CX9C motifs for stability while its CPC motif is known to facilitate the import of IMS bound proteins. Site-directed mutagenesis complemented by MALDI on in vivo hMIA40 protein shows that a portion of MIA40 undergoes reversible S-glutathionylation at three cysteines in the twin CX9C motifs and the lone cysteine 4 residue. We find that HEK293T cells expressing hMIA40 mutant defective for glutathionylation are compromised in the activities of complexes III and IV of the Electron Transport Chain (ETC) and enhance Reactive Oxygen Species (ROS) levels. Immunocapture studies show MIA40 interacting with complex III. Interestingly, glutathionylated MIA40 can transfer electrons to cytochrome C directly. However, Fe–S clusters associated with the CPC motif are essential to facilitate the two-electron to one-electron transfer for reducing cytochrome C. These results suggest that hMIA40 undergoes glutathionylation to maintain ROS levels and for optimum function of complexes III and IV of ETC. Our studies shed light on a novel post-translational modification of hMIA40 and its ability to act as a redox switch to regulate the ETC and cellular redox homeostasis.

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CHCHD4 confers metabolic vulnerabilities to tumour cells through its control of the mitochondrial respiratory chain

Cited by 5 publications

References 48 publications

CHCHD4 regulates tumour proliferation and EMT-related phenotypes, through respiratory chain-mediated metabolism

CHCHD4 regulates tumour proliferation and EMT-related phenotypes, through respiratory chain-mediated metabolism

USF1-CHCHD4 axis promotes lung adenocarcinoma progression partially via activating the MYC pathway

Glutathionylated and Fe–S cluster containing hMIA40 (CHCHD4) regulates ROS and mitochondrial complex III and IV activities of the electron transport chain

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