MNRR1, a Biorganellar Regulator of Mitochondria

Grossman, Lawrence I.; Purandare, Neeraja; Arshad, Rooshan; Gladyck, Stephanie; Somayajulu, Mallika; Hüttemann, Maik; Aras, Siddhesh

doi:10.1155/2017/6739236

Cited by 23 publications

(17 citation statements)

References 92 publications

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“…FGF21 and HTRA2 orthologous genes ( fgf21 , htra2 ) were also significantly upregulated in the double chchd10 -/- & chchd2 -/- model (Fig. 7 B) as was the previously described oxygen responsive transcript, cox4i2 (25–27) (Fig. 7 C).…”

Section: Resultssupporting

confidence: 56%

“…CHCHD2 and CHCHD10 share 58% sequence identity and have a common ancestor in yeast, suggesting that these proteins might have partially overlapping function (15). In vitro studies have reported that loss of either CHCHD2, CHCHD10 or both, impacts mitochondrial respiration (10, 16), survival/growth following exposure to various cellular stressors (9, 10, 16, 17), the mitochondrial integrated stress response (mt-ISR) (18–22), apoptosis (23, 24), as well as the transcription of the oxygen responsive gene COX4I2 (25–27).…”

Section: Introductionmentioning

confidence: 99%

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Loss of mitochondrial Chchd10 or Chchd2 in zebrafish leads to an ALS-like phenotype and Complex I deficiency independent of the mt-ISR

Légaré¹,

Rampal²,

Aaltonen

et al. 2022

Preprint

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Mutations in CHCHD10 and CHCHD2, coding for two paralogous mitochondrial proteins, have been identified in amyotrophic lateral sclerosis (ALS), frontotemporal lobar degeneration (FTD), and Parkinson's disease (PD). Here we investigated the biological roles of these proteins during vertebrate development using knockout (KO) models in zebrafish. We demonstrate that loss of either or both proteins leads to a motor impairment, reduced survival, and compromised neuromuscular junction (NMJ) integrity in larval zebrafish. Compensation by Chchd10 was observed in the chchd2-/- model, but not by Chchd2 in the chchd10 -/- model. The assembly of mitochondrial respiratory chain Complex I was impaired in chchd10 -/- and chchd2 -/- zebrafish larvae, but unexpectedly not in the double chchd10 -/- & chchd2 -/- model, suggesting that reduced mitochondrial Complex I cannot be solely responsible for the observed phenotypes, which are generally more severe in the double KO. Activation of the mitochondrial integrated stress response (mt-ISR) was only observed in the double KO model, possibly implicating this pathway in the recovery of the Complex I defect, and suggesting that Complex I assembly defect in our single KO is independent of the mt-ISR. Our results demonstrate that both proteins are required for normal vertebrate development, but their precise molecular function in the mitochondrial biology of motor neurons remains to be discovered.

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Section: Resultssupporting

confidence: 56%

Section: Introductionmentioning

confidence: 99%

Loss of mitochondrial Chchd10 or Chchd2 in zebrafish leads to an ALS-like phenotype and Complex I deficiency independent of the mt-ISR

Légaré¹,

Rampal²,

Aaltonen

et al. 2022

Preprint

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“…Exosome Hypoxia also downregulated the expression levels of Mtfp1, a participant in Dox-induced cardiac injury [64]. While, exosome Hypoxia increased the expression levels of Hspa1a (autophagy inducer) [65], Cox4i2 (the modulator of mitochondrial response) [66], and ATP1B2 (cardiac oxidative stress inhibitor) [67], accompanied by cellular rejuvenation. Also, these metabolism-related genes were the target genes of miR-92a-3p to maintain cardiac metabolism homeo-stasis [23].…”

Section: Discussionmentioning

confidence: 99%

Long-noncoding RNA MALAT1 sponges microRNA-92a-3p to inhibit doxorubicin-induced cardiac senescence by targeting ATG4a

Xia

Chen

Xie

et al. 2020

Aging

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The clinical application of doxorubicin (Dox) is limited due to its undesirable cardiotoxicity side effects. Cellular senescence plays an important role in Dox-induced cardiotoxicity. Exosomes derived from stem cells showed a therapeutic effect in Dox-induced cardiomyopathy (DIC). Hypoxia-preconditioned exosomes (exosome Hypoxia ) display pro-metabolism and pro-survival abilities. Several long-noncoding RNAs/microRNAs act as competing endogenous RNAs (ceRNAs) modulating DIC. No study investigated whether exosome Hypoxia could attenuate DIC through modulating ceRNAs. Treatment of the human adipose-derived mesenchymal stem cells with hypoxia induced lncRNA-MALAT1 accumulation in the secreted exosomes. In addition, the lncRNA-MALAT1 was identified as an exosomal transfer RNA to repress miR-92a-3p expression. Silencing the lncRNA-MALAT1 in MSCs or miR-92a-3p overexpression in cardiomyocytes significantly impaired the rejuvenation induced by exosome Hypoxia . TargetScan and luciferase assay showed that miR-92a-3p targeted the ATG4a 3' untranslated region. Silencing ATG4a blocked the anti-senescent effect of exosome Hypoxia . This study identified the lncRNA-MALAT1 that functioned as ceRNA binding to miR-92a-3p, leading to ATG4a activation, thus improving mitochondrial metabolism. LncRNA-MALAT1/miR-92a-3p/ATG4a partially mediates the cardioprotective roles of exosome Hypoxia in Dox-induced cardiac damage. Exosome Hypoxia may serve as a potential therapeutic target against DIC.

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“…Next, CHCHD2 was identified as a prime candidate linking Bcl-xL to the transcriptomic changes, because it is consistently downregulated in mutant cells and the protein binds Bcl-xL, resulting in a decreased oligomerization of Bax (Liu et al., 2015). This downregulation may be through a self-regulatory feedback loop, as CHCHD2 is able to translocate to the nucleus to transactivate itself as well as other genes that contain oxygen-responsive element sequences in their promoter region (Aras et al., 2013, Grossman et al., 2017). Another interesting function of CHCHD2 is its capacity to interact with the SMADs (2/3/4) and thus modulate the transcription of TGF-β-mediated target genes (Zhu et al., 2016).…”

Section: Discussionmentioning

confidence: 99%

Gain of 20q11.21 in Human Pluripotent Stem Cells Impairs TGF-β-Dependent Neuroectodermal Commitment

et al. 2019

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Summary Gain of 20q11.21 is one of the most common recurrent genomic aberrations in human pluripotent stem cells. Although it is known that overexpression of the antiapoptotic gene Bcl-xL confers a survival advantage to the abnormal cells, their differentiation capacity has not been fully investigated. RNA sequencing of mutant and control hESC lines, and a line transgenically overexpressing Bcl-xL , shows that overexpression of Bcl-xL is sufficient to cause most transcriptional changes induced by the gain of 20q11.21. Moreover, the differentially expressed genes in mutant and Bcl-xL overexpressing lines are enriched for genes involved in TGF-β- and SMAD-mediated signaling, and neuron differentiation. Finally, we show that this altered signaling has a dramatic negative effect on neuroectodermal differentiation, while the cells maintain their ability to differentiate to mesendoderm derivatives. These findings stress the importance of thorough genetic testing of the lines before their use in research or the clinic.

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MNRR1, a Biorganellar Regulator of Mitochondria

Cited by 23 publications

References 92 publications

Loss of mitochondrial Chchd10 or Chchd2 in zebrafish leads to an ALS-like phenotype and Complex I deficiency independent of the mt-ISR

Loss of mitochondrial Chchd10 or Chchd2 in zebrafish leads to an ALS-like phenotype and Complex I deficiency independent of the mt-ISR

Long-noncoding RNA MALAT1 sponges microRNA-92a-3p to inhibit doxorubicin-induced cardiac senescence by targeting ATG4a

Gain of 20q11.21 in Human Pluripotent Stem Cells Impairs TGF-β-Dependent Neuroectodermal Commitment

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