Your search keyword '"GTPBP3"' showing total 30 results

1. Expanding the phenotypic and genetic spectrum of GTPBP3 deficiency: findings from nine Chinese pedigrees.

Author

Xie, Yaojun, Li, Keyi, Yang, Li, Zeng, Xiaofei, Chen, Zhehui, Ma, Xue, Zhang, Luyi, Zhou, Yuwei, Jin, Liqin, Yang, Yanling, and Lou, Xiaoting

Abstract

Background: GTPBP3 catalyzes τm5(s2) U biosynthesis at the 34th wobble position of mitochondrial tRNAs, the hypomodification of τm5U leads to mitochondrial disease. While twenty-three variants of GTPBP3 have been reported worldwide, the genetic landscape in China remains uncertain. Methods: By using whole-exome sequencing, the candidate individuals carrying GTPBP3 variants were screened and identified. Pathogenicity analysis of variants was biochemically verified by patients-derived immortalized lymphocytes and cell models. Results: Through whole-exome sequencing, thirteen variants associated with GTPBP3 were identified in nine Chinese pedigrees, with eight of these variants being newly reported. Affected individuals displayed classic neurologic phenotypes and heart complications including developmental delay, seizures, hypotonia, exercise intolerance, and hypertrophic cardiomyopathy. Additionally, they displayed new symptoms such as eye problems like strabismus and heart issues related to valve function. Studies conducted on patient-derived cells provided evidence of reduced levels of GTPBP3 and impairment in mitochondrial energetic biogenesis. Re-expressing GTPBP3 variants in knockout cell lines further defined the pathogenicity of the novel variants. Analysis of the genetic spectrum in the Chinese population highlighted a concentration in exons 4 and 6, with c.689A > C being the prominent hotspot. Conclusion: Our findings emphasize the extensive clinical and genetic implications of GTPBP3-related mitochondrial disorders, particularly within the Chinese population, but further investigations are needed to explore the phenotype-genotype correlation. [ABSTRACT FROM AUTHOR]

Published

2024

2. Novel insights on GTPBP3‐associated hypertrophic cardiomyopathy.

Author

Angelova, Petya, Velchev, Vasil, Stoyanov, Nikolay, Atemin, Slavena, Todorov, Tihomir, Tourtourikov, Ivan, Mitev, Vanyo, and Todorova, Albena

Abstract

About 100 genes have been associated with cardiomyopathies with genotype–phenotype correlations often hard to establish. Genetic testing may help to confirm the genetic diagnosis and assess the risk of inheritance in the family. A 25‐year old male with hypertrophic cardiomyopathy and fasciculoventricular accessory pathway was referred for genetic testing by his cardiologist. Targeted PRKAG2 screening and whole‐exome sequencing were performed, followed by Sanger sequencing segregation analysis in the family. The PRKAG2 gene screening was negative. Whole‐exome sequencing revealed the following four variants in the patient: c.181G>C (p.Ala61Pro) and c.1199C>T (p.Thr400Met) in the GTPBP3 gene, as well as c.752C>T (p.Thr251Ile) and c.1760C>T (p.Pro587Leu) in the POLG gene. Family segregation analysis showed that the patient's mother is a carrier of variant c.181G>C and the patient's paternal grandmother is a carrier of variant c.1199C>T in the GTPBP3 gene, which is in accordance with an autosomal recessive model of inheritance of the disease. Both variants in the POLG are found paternally inherited in the patient's healthy half‐brother, thus are not considered disease‐causing. GTPBP3 variants have been reported in patients with hypertrophic cardiomyopathy, associated with combined oxidative phosphorylation deficiency 23. These novel variants represent the probable cause of the observed clinical symptoms in the patient. [ABSTRACT FROM AUTHOR]

Published

2023

3. Pathogenicity Analysis of a Novel Variant in GTPBP3 Causing Mitochondrial Disease and Systematic Literature Review.

Author

Zhang, Qin, Ouyang, Qianqian, Xiang, Jingjing, Li, Hong, Lv, Haitao, and An, Yu

Subjects

*TRANSFER RNA, *GUANOSINE triphosphate, *CONGESTIVE heart failure, *MITOCHONDRIA, *HYPERTROPHIC cardiomyopathy, *DEVELOPMENTAL disabilities, *DEVELOPMENTAL delay

Abstract

Defect of GTPBP3, the human mitochondrial tRNA-modifying enzyme, can lead to Combined Oxidative Phosphorylation Deficiency 23 (COXPD23). Up to now, about 20 different variants of the GTPBP3 gene have been reported; however, genotype–phenotype analysis has rarely been described. Here, we reported a 9-year-old boy with COXPD23 who presented with hyperlactatemia, hypertrophic cardiomyopathy, seizures, feeding difficulties, intellectual disability and motor developmental delay, and abnormal visual development. Biallelic pathogenic variants of the GTPBP3 gene were identified in this boy, one novel variant c.1102dupC (p. Arg368Profs*22) inherited from the mother and the other known variant c.689A>C (p. Gln230Pro) inherited from father. We curated 18 COXPD23 patients with GTPBP3 variants to investigate the genotype–phenotype correlation. We found that hyperlactatemia and cardiomyopathy were critical clinical features in COXPD23 and the average onset age was 1.7 years (3 months of age for the homozygote). Clinical classification of COXPD23 for the two types, severe and mild, was well described in this study. We observed arrhythmia and congestive heart failure frequently in the severe type with early childhood mortality, while developmental delay was mainly observed in the mild type. The proportion of homozygous variants (71.4%) significantly differed from that of compound heterozygous variants (18.1%) in the severe type. Compared with the variants in gnomAD, the proportion of LOFVs in GTPBP3 was higher in COXPD23 patients (48.6% versus 8.9%, p < 0.0001 ****), and 31% of them were frameshift variants, showing the LOF mechanism of GTPBP3. Additionally, the variants in patients were significantly enriched in the TrmE-type G domain, indicating that the G domain was crucial for GTPBP3 protein function. The TrmE-type G domain contained several significant motifs involved in the binding of guanine nucleotides and Mg2+, the hydrolysis of GTP, and the regulation of the functional status of GTPases. In conclusion, we reported a mild COXPD23 case with typical GTPBP3-related symptoms, including seizures and abnormal visual development seldom observed previously. Our study provides novel insight into understanding the clinical diagnosis and genetic counseling of patients with COXPD23 by exploring the genetic pathogenesis and genotype–phenotype correlation of COXPD23. [ABSTRACT FROM AUTHOR]

Published

2023

4. Taurine protects R28 cells from hypoxia/re-oxygenation-induced damage via regulation of mitochondrial energy metabolism.

Author

Lu, Wei, Yang, Yuting, Gao, Shunxiang, Wu, Jihong, and Sun, Xinghuai

Subjects

*TRANSFER RNA, *TAURINE, *RESPIRATION, *ENERGY metabolism, *DAMAGE models, *MITOCHONDRIA, *MITOCHONDRIAL membranes, *MEMBRANE potential

Abstract

Oxidative-induced damage and hypoxia/re-oxygenation (H/R) injury are common causes of irreversible visual impairment. The goals of this study were to explore the effects of taurine on R28 cells under the two damage models and the underlying mechanisms. Low doses of taurine supplementation promoted cell viability, mitochondrial membrane potential (MMP), SOD levels, ATP contents and attenuated cytotoxicity and intracellular ROS generation of the R28 cells under the two kinds of damage. The expression level of GTPBP3, a mitochondrial-tRNA (mt-tRNA) modification enzyme that catalyzes the taurine involved modification, was decreased under the two damage and taurine could reverse the reduction. After knocking down GTPBP3, the R28 cells become vulnerable to damage. The viability, cytotoxicity, MMP and intracellular ROS level of knockdown cells changed more obviously under the H/R injury than those of control cell. We also found that knockdown of GTPBP3 significantly decreased mitochondrial energy metabolism by measuring the oxidative respiration rate by the Seahorse XFe24 extracellular flux analyzer. The protection of low doses of taurine disappeared on knockdown R28 cells, indicating that GTPBP3 is crucial in the protection mechanisms of taurine. However, the impacts of the reduction of GTPBP3 level can be reversed by relatively high doses of taurine, implying the protection effects of taurine were dose-dependent, and there were more complicated mechanisms remain to be explored. This study explored a new mechanism of the neuroprotective effects of taurine, which depend on the GTPBP3-mediated taurine modification of mt-tRNAs and the promotion of mitochondrial energy metabolism. [ABSTRACT FROM AUTHOR]

Published

2022

5. Taurine mechanism in preventing retinal cell damage from acute ocular hypertension through GTPBP3 regulation.

Author

Lu W, Yang Y, Gao S, Wu J, and Sun X

Abstract

We aimed to explore the protective effects and underlying mechanisms of taurine on retinal cells during acute ocular hypertension (AOH)-induced damage. Retinal morphology, apoptosis, mitochondrial structure, electroretinography, expression of GTP binding protein 3 (GTPBP3), and molecules in the unfolded protein response (UPR) were examined in an AOH mouse model and wild-type (WT) mice with or without intravitreal injection of taurine. For in vitro experiments, the GTPBP3 expression and endoplasmic reticulum (ER) stress were examined in R28 cell line under hydrogen peroxide (H 2 O 2 )-induced damage or hypoxia/reoxygenation (H/R)-induced damage, with or without taurine pretreatment. Taurine pretreatment alleviated retinal damage caused by AOH modeling. The GTPBP3 expression level decreased after AOH injury, and taurine pretreatment reversed this reduction. Retinas with decreased GTPBP3 expression showed reduced retinal ganglion cell (RGC) function, which could be reversed by intravitreal taurine injection. In H 2 O 2- , H/R-, and AOH-induced damage, UPR were activated and alleviated by taurine pretreatment. GTPBP3 knockdown in R28 cells also activated the UPR, which was alleviated by taurine. A UPR activator downregulated GTPBP3 levels in normal R28 cells, whereas a UPR inhibitor upregulated GTPBP3 levels in GTPBP3 knockdown R28 cells. In conclusion, this study provides important evidence that taurine prevents retinal cell damage in mice exposed to AOH and modulates GTPBP3 expression via the UPR pathway. Interventions targeting this mechanism can be used as potential therapeutic targets for AOH damage., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Ltd.)

Published

2024

6. Coding Variants in HOOK2 and GTPBP3 May Contribute to Risk of Primary Angle Closure Glaucoma.

Author

Qiao, Chunyan, Jia, Hongyan, Zhang, Hui, Wang, Hui, Liang, Jing, Song, Jing, Li, Liang, Duan, Xiaoming, Cao, Kai, and Hu, Jianping

Subjects

*CHINESE people, *SALMONELLA diseases, *GLAUCOMA

Abstract

Primary angle closure glaucoma (PACG) is a major cause of blindness worldwide. This study proposed to screen candidate PACG-associated variants in Chinese Han people. Whole exome sequencing was applied to five confirmed PACG patients and two primary angle closure suspect individuals within a PACG-enriched Chinese Han family. A series of bioinformatics analyses were implemented to obtain high-risk single nucleotide variant (SNV) loci for PACG, which were subsequently used for linkage analysis for identifying linkage genome regions. In addition, MassARRAY SNV genotyping was applied to high-risk PACG loci as well as those within linkage regions in another independent cohort including 251 PACG and 251 normal samples to further screen high-confidence SNVs. A total of 27 loci in 19 genes remained after linkage analysis. The 19 genes were significantly enriched in biological processes tightly related to PACG, including retinol metabolism and salmonella infection. Two nonsynonymous SNV loci, rs897804 in exon15 of HOOK2 and rs3745193 in exon7 of GTPBP3, were recognized with higher variant frequency in PACG samples than that in control samples after association analysis of MassARRAY SNV genotyping data. This study sheds new light on the understanding of PACG incidence among Chinese Han people. [ABSTRACT FROM AUTHOR]

Published

2020

7. Pathogenicity Analysis of a Novel Variant in GTPBP3 Causing Mitochondrial Disease and Systematic Literature Review

Author

Qin Zhang, Qianqian Ouyang, Jingjing Xiang, Hong Li, Haitao Lv, and Yu An

Subjects

variants, mitochondrial diseases, Genetics, COXPD23, GTPBP3, Genetics (clinical), taurine modification

Abstract

Defect of GTPBP3, the human mitochondrial tRNA-modifying enzyme, can lead to Combined Oxidative Phosphorylation Deficiency 23 (COXPD23). Up to now, about 20 different variants of the GTPBP3 gene have been reported; however, genotype–phenotype analysis has rarely been described. Here, we reported a 9-year-old boy with COXPD23 who presented with hyperlactatemia, hypertrophic cardiomyopathy, seizures, feeding difficulties, intellectual disability and motor developmental delay, and abnormal visual development. Biallelic pathogenic variants of the GTPBP3 gene were identified in this boy, one novel variant c.1102dupC (p. Arg368Profs*22) inherited from the mother and the other known variant c.689A>C (p. Gln230Pro) inherited from father. We curated 18 COXPD23 patients with GTPBP3 variants to investigate the genotype–phenotype correlation. We found that hyperlactatemia and cardiomyopathy were critical clinical features in COXPD23 and the average onset age was 1.7 years (3 months of age for the homozygote). Clinical classification of COXPD23 for the two types, severe and mild, was well described in this study. We observed arrhythmia and congestive heart failure frequently in the severe type with early childhood mortality, while developmental delay was mainly observed in the mild type. The proportion of homozygous variants (71.4%) significantly differed from that of compound heterozygous variants (18.1%) in the severe type. Compared with the variants in gnomAD, the proportion of LOFVs in GTPBP3 was higher in COXPD23 patients (48.6% versus 8.9%, p < 0.0001 ****), and 31% of them were frameshift variants, showing the LOF mechanism of GTPBP3. Additionally, the variants in patients were significantly enriched in the TrmE-type G domain, indicating that the G domain was crucial for GTPBP3 protein function. The TrmE-type G domain contained several significant motifs involved in the binding of guanine nucleotides and Mg2+, the hydrolysis of GTP, and the regulation of the functional status of GTPases. In conclusion, we reported a mild COXPD23 case with typical GTPBP3-related symptoms, including seizures and abnormal visual development seldom observed previously. Our study provides novel insight into understanding the clinical diagnosis and genetic counseling of patients with COXPD23 by exploring the genetic pathogenesis and genotype–phenotype correlation of COXPD23.

Published

2023

8. The human tRNA taurine modification enzyme GTPBP3 is an active GTPase linked to mitochondrial diseases

Author

Yong Zhang, Hong Xu, Qingrun Li, Qin-Qin Wang, Xiao-Long Zhou, Gui-Xin Peng, and En-Duo Wang

Subjects

Models, Molecular, Cytoplasm, TRNA modification, Mitochondrial Diseases, AcademicSubjects/SCI00010, Mutant, GTPase, Mitochondrion, Biology, medicine.disease_cause, GTP-Binding Proteins, Catalytic Domain, Sf9 Cells, Genetics, medicine, Animals, Humans, chemistry.chemical_classification, Mutation, Nucleic Acid Enzymes, RNA-Binding Proteins, Mitochondria, Isoenzymes, Protein Transport, HEK293 Cells, Enzyme, chemistry, Biochemistry, Transfer RNA, GTPBP3

Abstract

GTPBP3 and MTO1 cooperatively catalyze 5-taurinomethyluridine (τm5U) biosynthesis at the 34th wobble position of mitochondrial tRNAs. Mutations in tRNAs, GTPBP3 or MTO1, causing τm5U hypomodification, lead to various diseases. However, efficient in vitro reconstitution and mechanistic study of τm5U modification have been challenging, in part due to the lack of pure and active enzymes. A previous study reported that purified human GTPBP3 (hGTPBP3) is inactive in GTP hydrolysis. Here, we identified the mature form of hGTPBP3 and showed that hGTPBP3 is an active GTPase in vitro that is critical for tRNA modification in vivo. Unexpectedly, the isolated G domain and a mutant with the N-terminal domain truncated catalyzed GTP hydrolysis to only a limited extent, exhibiting high Km values compared with that of the mature enzyme. We further described several important pathogenic mutations of hGTPBP3, associated with alterations in hGTPBP3 localization, structure and/or function in vitro and in vivo. Moreover, we discovered a novel cytoplasm-localized isoform of hGTPBP3, indicating an unknown potential noncanonical function of hGTPBP3. Together, our findings established, for the first time, the GTP hydrolysis mechanism of hGTPBP3 and laid a solid foundation for clarifying the τm5U modification mechanism and etiology of τm5U deficiency-related diseases.

Published

2021

9. Deletion of Gtpbp3 in zebrafish revealed the hypertrophic cardiomyopathy manifested by aberrant mitochondrial tRNA metabolism

Author

Danni Chen, Qingxian Yang, Chao Chen, Zengming Zhang, Cheng Ai, Meng Wang, Shihao Yao, Xiao He, Min-Xin Guan, and Feng Li

Subjects

Protein Conformation, Respiratory chain, Mitochondrion, Biology, medicine.disease_cause, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, RNA, Transfer, GTP-Binding Proteins, RNA and RNA-protein complexes, Genetics, medicine, Animals, Aminoacylation, Myocytes, Cardiac, Transgenes, Zebrafish, In Situ Hybridization, 030304 developmental biology, 0303 health sciences, Mutation, Cardiomyopathy, Hypertrophic, Zebrafish Proteins, biology.organism_classification, Mitochondria, Cell biology, Phenotype, Proteostasis, Mitochondrial biogenesis, Transfer RNA, CRISPR-Cas Systems, GTPBP3, Gene Deletion, 030217 neurology & neurosurgery

Abstract

GTPBP3 is a highly conserved tRNA modifying enzyme for the biosynthesis of τm5U at the wobble position of mitochondrial tRNAGlu, tRNAGln, tRNALys, tRNATrp and tRNALeu(UUR). The previous investigations showed that GTPBP3 mutations were associated with hypertrophic cardiomyopathy (HCM). However, the pathophysiology of GTPBP3 deficiency remains elusively. Using the gtpbp3 knockout zebrafish generated by CRISPR/Cas9 system, we demonstrated the aberrant mitochondrial tRNA metabolism in gtpbp3 knock-out zebrafish. The deletion of gtpbp3 may alter functional folding of tRNA, indicated by conformation changes and sensitivity to S1-mediated digestion of tRNAGlu, tRNALys, tRNATrp and tRNALeu(UUR). Strikingly, gtpbp3 knock-out zebrafish displayed the global increases in the aminoacylated efficiencies of mitochondrial tRNAs. The aberrant mitochondrial tRNA metabolisms impaired mitochondrial translation, produced proteostasis stress and altered activities of respiratory chain complexes. These mitochondria dysfunctions caused the alterations in the embryonic heart development and reduced fractional shortening of ventricles in mutant zebrafish. Notably, the gtpbp3 knock-out zebrafish exhibited hypertrophy of cardiomyocytes and myocardial fiber disarray in ventricles. These cardiac defects in the gtpbp3 knock-out zebrafish recapitulated the clinical phenotypes in HCM patients carrying the GTPBP3 mutation(s). Our findings highlight the fundamental role of defective nucleotide modifications of tRNAs in mitochondrial biogenesis and their pathological consequences in hypertrophic cardiomyopathy.

Published

2019

10. Modification of the wobble uridine in bacterial and mitochondrial tRNAs reading NNA/NNG triplets of 2-codon boxes.

Author

Armengod, M Eugenia, Meseguer, Salvador, Villarroya, Magda, Prado, Silvia, Moukadiri, Ismaïl, Ruiz-Partida, Rafael, Garzón, M José, Navarro-González, Carmen, and Martínez-Zamora, Ana

Published

2014

11. Metabolic and chemical regulation of tRNA modification associated with taurine deficiency and human disease

Author

Kazuhito Tomizawa, Yoshihito Kishita, Ryou Tanaka, Tomoyuki Numata, Takanobu Goto, Takeshi Yamamoto, Kei Murayama, Akira Ohtake, Kana Asano, Takeo Suzuki, Ayaka Saito, Yasushi Okazaki, Yoshiho Ikeuchi, Tsutomu Suzuki, Yuriko Sakaguchi, Yoshihisa Yamane, and Fan Yan Wei

Subjects

0301 basic medicine, Taurine, TRNA modification, Mitochondrial Diseases, Mitochondrial translation, NAR Breakthrough Article, Biology, Mitochondrion, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, RNA, Transfer, GTP-Binding Proteins, Genetics, Animals, Humans, Uridine, RNA-Binding Proteins, RNA, Mitochondria, HEK293 Cells, 030104 developmental biology, Biochemistry, chemistry, Child, Preschool, Transfer RNA, Cats, Female, Carrier Proteins, GTPBP3, 030217 neurology & neurosurgery, Biogenesis, HeLa Cells

Abstract

Modified uridine containing taurine, 5-taurinomethyluridine (τm5U), is found at the anticodon first position of mitochondrial (mt-)transfer RNAs (tRNAs). Previously, we reported that τm5U is absent in mt-tRNAs with pathogenic mutations associated with mitochondrial diseases. However, biogenesis and physiological role of τm5U remained elusive. Here, we elucidated τm5U biogenesis by confirming that 5,10-methylene-tetrahydrofolate and taurine are metabolic substrates for τm5U formation catalyzed by MTO1 and GTPBP3. GTPBP3-knockout cells exhibited respiratory defects and reduced mitochondrial translation. Very little τm5U34 was detected in patient’s cells with the GTPBP3 mutation, demonstrating that lack of τm5U results in pathological consequences. Taurine starvation resulted in downregulation of τm5U frequency in cultured cells and animal tissues (cat liver and flatfish). Strikingly, 5-carboxymethylaminomethyluridine (cmnm5U), in which the taurine moiety of τm5U is replaced with glycine, was detected in mt-tRNAs from taurine-depleted cells. These results indicate that tRNA modifications are dynamically regulated via sensing of intracellular metabolites under physiological condition.

Published

2018

12. Defects in the mitochondrial-tRNA modification enzymes MTO1 and GTPBP3 promote different metabolic reprogramming through a HIF-PPARγ-UCP2-AMPK axis

Author

Salvador Meseguer, Elena Martín-Hernández, Rachid Boutoual, Magda Villarroya, Mohammed Errami, Miguel Martín, M.-Eugenia Armengod, Marta Casado, and Ministerio de Economía y Competitividad (España)

Subjects

0301 basic medicine, Primary Cell Culture, lcsh:Medicine, Oxidative phosphorylation, AMP-Activated Protein Kinases, Article, Oxidative Phosphorylation, 03 medical and health sciences, chemistry.chemical_compound, RNA, Transfer, GTP-Binding Proteins, Lipid droplet, Humans, Uncoupling Protein 2, Glycolysis, lcsh:Science, Beta oxidation, Multidisciplinary, Fatty acid metabolism, lcsh:R, RNA-Binding Proteins, Mitochondrial tRNA modification, AMPK, Cardiomyopathy, Hypertrophic, Fibroblasts, Hypoxia-Inducible Factor 1, alpha Subunit, Lipid Metabolism, Mitochondria, Cell biology, PPAR gamma, 030104 developmental biology, Gene Expression Regulation, chemistry, Mutation, lcsh:Q, Acidosis, Lactic, Carrier Proteins, GTPBP3, Signal Transduction

Abstract

18 páginas 8 figuras. Supplementary information accompanies this paper at https://doi.org/10.1038/s41598-018-19587-5., Human proteins MTO1 and GTPBP3 are thought to jointly catalyze the modification of the wobble uridine in mitochondrial tRNAs. Defects in each protein cause infantile hypertrophic cardiomyopathy with lactic acidosis. However, the underlying mechanisms are mostly unknown. Using fibroblasts from an MTO1 patient and MTO1 silenced cells, we found that the MTO1 deficiency is associated with a metabolic reprogramming mediated by inactivation of AMPK, down regulation of the uncoupling protein 2 (UCP2) and transcription factor PPARγ, and activation of the hypoxia inducible factor 1 (HIF-1). As a result, glycolysis and oxidative phosphorylation are uncoupled, while fatty acid metabolism is altered, leading to accumulation of lipid droplets in MTO1 fibroblasts. Unexpectedly, this response is different from that triggered by the GTPBP3 defect, as GTPBP3-depleted cells exhibit AMPK activation, increased levels of UCP2 and PPARγ, and inactivation of HIF-1. In addition, fatty acid oxidation and respiration are stimulated in these cells. Therefore, the HIF-PPARγ-UCP2-AMPK axis is operating differently in MTO1- and GTPBP3-defective cells, which strongly suggests that one of these proteins has an additional role, besides mitochondrial-tRNA modification. This work provides new and useful information on the molecular basis of the MTO1 and GTPBP3 defects and on putative targets for therapeutic intervention., Tis work has been supported by grants from the Spanish Ministry of Economy and Competitiveness (grants BFU2010-19737 and BFU2014-58673-P to M.-E.A.; and SAF2016-75004-R to M.C.), Instituto de Salud Carlos III (FIS-ISCIII PI 14/0431 to M.A.M) and Generalitat Valenciana (ACOMP/2012/065 and PROMETEO/2012/061 to M.-E.A. Contribution to COST Action CA15203 MITOEAGLE. R.B. is a recipient of a fellowship from the Generalitat Valenciana (grant GRISOLIA/2014/038). Te authors thank Dr. E. Knecht and Dr. C. Aguado (CIPF, Valencia, Spain) for their valuable advice and for providing facilities in our research work, and Dr. M. Morán (Hospital 12 de Octubre, Madrid, Spain) for growth and maintenance of patient fbroblasts.

Published

2018

13. Modification of the wobble uridine in bacterial and mitochondrial tRNAs reading NNA/NNG triplets of 2-codon boxes

Author

Carmen Navarro-González, Silvia Prado, Salvador Meseguer, M.-Eugenia Armengod, Ismaïl Moukadiri, Ana Martínez-Zamora, Magda Villarroya, M.-José Garzón, and Rafael Ruiz-Partida

Subjects

TRNA modification, RNA, Mitochondrial, MTO1, MnmA, Review, Wobble base pair, Biology, Mitochondrion, Oxidative Phosphorylation, GTP Phosphohydrolases, GTPBP3, Conserved sequence, Multienzyme Complexes, TRMU, Anticodon, Escherichia coli, MTU1, RNA Processing, Post-Transcriptional, Codon, Uridine, Molecular Biology, One-Carbon Group Transferases, TrmL, Cell Nucleus, Genetics, mitochondrial diseases, Escherichia coli Proteins, Translation (biology), Cell Biology, RNA, Transfer, Amino Acid-Specific, Mitochondria, MnmG, MnmE, MELAS, MnmC, Transfer RNA, Retrograde signaling, RNA, tRNA modification, Signal Transduction

Abstract

Posttranscriptional modification of the uridine located at the wobble position (U34) of tRNAs is crucial for optimization of translation. Defects in the U34 modification of mitochondrial-tRNAs are associated with a group of rare diseases collectively characterized by the impairment of the oxidative phosphorylation system. Retrograde signaling pathways from mitochondria to nucleus are involved in the pathophysiology of these diseases. These pathways may be triggered by not only the disturbance of the mitochondrial (mt) translation caused by hypomodification of tRNAs, but also as a result of nonconventional roles of mt-tRNAs and mt-tRNA-modifying enzymes. The evolutionary conservation of these enzymes supports their importance for cell and organismal functions. Interestingly, bacterial and eukaryotic cells respond to stress by altering the expression or activity of these tRNA-modifying enzymes, which leads to changes in the modification status of tRNAs. This review summarizes recent findings about these enzymes and sets them within the previous data context.

Published

2014

14. microRNA-mediated differential expression of TRMU, GTPBP3 and MTO1 in cell models of mitochondrial-DNA diseases

Author

Olga Boix, Salvador Meseguer, Julio Montoya, Sonia Emperador, Magda Villarroya, Rachid Boutoual, Elena García-Arumí, Carmen Navarro-González, and M.-Eugenia Armengod

Subjects

0301 basic medicine, Mitochondrial DNA, Mitochondrial Diseases, Science, Bone Neoplasms, Mitochondrion, Biology, medicine.disease_cause, DNA, Mitochondrial, Oxidative Phosphorylation, Article, Mitochondrial Proteins, 03 medical and health sciences, GTP-Binding Proteins, medicine, Tumor Cells, Cultured, Humans, Cell Proliferation, Regulation of gene expression, Genetics, Mutation, Osteosarcoma, tRNA Methyltransferases, Multidisciplinary, 030102 biochemistry & molecular biology, RNA-Binding Proteins, Phenotype, TRNA Methyltransferases, Mitochondria, Gene Expression Regulation, Neoplastic, MicroRNAs, 030104 developmental biology, Retrograde signaling, Medicine, GTPBP3, Carrier Proteins, Signal Transduction

Abstract

Mitochondrial diseases due to mutations in the mitochondrial (mt) DNA are heterogeneous in clinical manifestations but usually include OXPHOS dysfunction. Mechanisms by which OXPHOS dysfunction contributes to the disease phenotype invoke, apart from cell energy deficit, maladaptive responses to mitochondria-to-nucleus retrograde signaling. Here we used five different cybrid models of mtDNA diseases to demonstrate that the expression of the nuclear-encoded mt-tRNA modification enzymes TRMU, GTPBP3 and MTO1 varies in response to specific pathological mtDNA mutations, thus altering the modification status of mt-tRNAs. Importantly, we demonstrated that the expression of TRMU, GTPBP3 and MTO1 is regulated by different miRNAs, which are induced by retrograde signals like ROS and Ca2+ via different pathways. Our data suggest that the up- or down-regulation of the mt-tRNA modification enzymes is part of a cellular response to cope with a stoichiometric imbalance between mtDNA- and nuclear-encoded OXPHOS subunits. However, this miRNA-mediated response fails to provide full protection from the OXPHOS dysfunction; rather, it appears to aggravate the phenotype since transfection of the mutant cybrids with miRNA antagonists improves the energetic state of the cells, which opens up options for new therapeutic approaches.

Published

2017

15. Mutations in the Caenorhabditis elegans orthologs of human genes required for mitochondrial tRNA modification cause similar electron transport chain defects but different nuclear responses

Author

M.-Eugenia Armengod, Magda Villarroya, Simon Tuck, Ernesto Lopez-Pascual, Ismaïl Moukadiri, and Carmen Navarro-González

Subjects

0301 basic medicine, Cancer Research, Life Cycles, Mitochondrial Diseases, Nematoda, ved/biology.organism_classification_rank.species, Mutant, Gene Expression, Yeast and Fungal Models, Mitochondrion, medicine.disease_cause, Biochemistry, Oxidative Phosphorylation, 0302 clinical medicine, Larvae, RNA, Transfer, Medicine and Health Sciences, Genetics (clinical), Caenorhabditis elegans, Energy-Producing Organelles, Genetics, Mutation, tRNA Methyltransferases, biology, Mitochondrial tRNA modification, RNA-Binding Proteins, Animal Models, Phenotype, Mitochondria, Nucleic acids, Mutant Strains, Experimental Organism Systems, Caenorhabditis Elegans, Saccharomyces Cerevisiae, Cellular Structures and Organelles, Transfer RNA, Anatomy, GTPBP3, Medical Genetics, Genital Anatomy, Cell Nucleolus, Research Article, Signal Transduction, lcsh:QH426-470, Bioenergetics, Research and Analysis Methods, Electron Transport, Mitochondrial Proteins, 03 medical and health sciences, Saccharomyces, Model Organisms, GTP-Binding Proteins, medicine, Animals, Humans, Model organism, Non-coding RNA, Gonads, Caenorhabditis elegans Proteins, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Medicinsk genetik, ved/biology, Organisms, Fungi, Reproductive System, Biology and Life Sciences, Cell Biology, biology.organism_classification, Invertebrates, Yeast, lcsh:Genetics, Disease Models, Animal, 030104 developmental biology, Caenorhabditis, RNA, Carrier Proteins, 030217 neurology & neurosurgery, Developmental Biology

Abstract

Several oxidative phosphorylation (OXPHOS) diseases are caused by defects in the post-transcriptional modification of mitochondrial tRNAs (mt-tRNAs). Mutations in MTO1 or GTPBP3 impair the modification of the wobble uridine at position 5 of the pyrimidine ring and cause heart failure. Mutations in TRMU affect modification at position 2 and cause liver disease. Presently, the molecular basis of the diseases and why mutations in the different genes lead to such different clinical symptoms is poorly understood. Here we use Caenorhabditis elegans as a model organism to investigate how defects in the TRMU, GTPBP3 and MTO1 orthologues (designated as mttu-1, mtcu-1, and mtcu-2, respectively) exert their effects. We found that whereas the inactivation of each C. elegans gene is associated with a mild OXPHOS dysfunction, mutations in mtcu-1 or mtcu-2 cause changes in the expression of metabolic and mitochondrial stress response genes that are quite different from those caused by mttu-1 mutations. Our data suggest that retrograde signaling promotes defect-specific metabolic reprogramming, which is able to rescue the OXPHOS dysfunction in the single mutants by stimulating the oxidative tricarboxylic acid cycle flux through complex II. This adaptive response, however, appears to be associated with a biological cost since the single mutant worms exhibit thermosensitivity and decreased fertility and, in the case of mttu-1, longer reproductive cycle. Notably, mttu-1 worms also exhibit increased lifespan. We further show that mtcu-1; mttu-1 and mtcu-2; mttu-1 double mutants display severe growth defects and sterility. The animal models presented here support the idea that the pathological states in humans may initially develop not as a direct consequence of a bioenergetic defect, but from the cell’s maladaptive response to the hypomodification status of mt-tRNAs. Our work highlights the important association of the defect-specific metabolic rewiring with the pathological phenotype, which must be taken into consideration in exploring specific therapeutic interventions., Author summary Post-transcriptional modification of tRNAs is a universal process, thought to be essential for optimizing the functions of tRNAs. In humans, defects in the modification at position 2 (performed by protein TRMU) and 5 (carried out by proteins GTPBP3 and MTO1) of the uridine located at the wobble position of mitochondrial tRNAs (mt-tRNAs) cause oxidative phosphorylation (OXPHOS) dysfunction, and lead to liver and heart failure, respectively. However, the underlying mechanisms leading to pathogenesis are not well-known, and hence there is no molecular explanation for the different clinical phenotypes. We use Caenorhabditis elegans to compare in the same animal model and genetic background the effects of inactivating the TRMU, GTPBP3 and MTO1 orthologues on the phenotype and gene expression pattern of nuclear and mitochondrial DNA. Our data show that C. elegans responds to mt-tRNA hypomodification by changing in a defect-specific manner the expression of nuclear and mitochondrial genes, which leads, in all single mutants, to a rescue of the OXPHOS dysfunction that is associated with a biological cost. Our work suggests that pathology may develop as a consequence of the cell’s maladaptive response to the hypomodification status of mt-tRNAs.

Published

2017

16. Mutations of the Mitochondrial-tRNA Modifier MTO1 Cause Hypertrophic Cardiomyopathy and Lactic Acidosis

Author

Enrico Baruffini, Holger Prokisch, Thomas Meitinger, Tim M. Strom, Cristina Dallabona, Ileana Ferrero, Massimo Zeviani, Tobias B. Haack, Alberto Burlina, Daniele Ghezzi, Rossella Parini, Laura Melchionda, and Federica Invernizzi

Subjects

Mitochondrial translation, Paromomycin, Mutant, DNA Mutational Analysis, Respiratory chain, Mitochondrion, medicine.disease_cause, Oxidative Phosphorylation, RNA, Transfer, Genetics(clinical), Phosphorylation, Genetics (clinical), Genetics, Mutation, Lactic, Respiration, Homozygote, RNA-Binding Proteins, Mitochondrial, Mitochondria, Phenotype, Acidosis, Lactic, Acidosis, GTPBP3, Mitochondrial DNA, Cardiomyopathy, Molecular Sequence Data, Mutation, Missense, Mothers, Saccharomyces cerevisiae, Biology, DNA, Mitochondrial, Frameshift mutation, Base Sequence, Cardiomyopathy, Hypertrophic, Carrier Proteins, Fibroblasts, Humans, Nucleic Acid Conformation, RNA, Ribosomal, Report, medicine, Ribosomal, DNA, Transfer, Hypertrophic, RNA, Missense

Abstract

Dysfunction of mitochondrial respiration is an increasingly recognized cause of isolated hypertrophic cardiomyopathy. To gain insight into the genetic origin of this condition, we used next-generation exome sequencing to identify mutations in MTO1, which encodes mitochondrial translation optimization 1. Two affected siblings carried a maternal c.1858dup (p.Arg620Lysfs(star)8) frameshift and a paternal c.1282G>A (p.Ala428Thr) missense mutation. A third unrelated individual was homozygous for the latter change. In both humans and yeast, MTO1 increases the accuracy and efficiency of mtDNA translation by catalyzing the 5-carboxymethylaminomethylation of the wobble uridine base in three mitochondrial tRNAs (mt-tRNAs). Accordingly, mutant muscle and fibroblasts showed variably combined reduction in mt DNA-dependent respiratory chain activities. Reduced respiration in mutant cells was corrected by expressing a wild-type MTO1 cDNA. Conversely, defective respiration of a yeast mto1 Delta strain failed to be corrected by an Mto1(Pro622 star) variant, equivalent to human MTO1(Arg620Lysfs star 8) whereas incomplete correction was achieved by an Mto1(Ala431Thr) variant, corresponding to human MTO1(Ala28Thr). The respiratory yeast phenotype was dramatically worsened in stress conditions and in the presence of a paromomycin-resistant (P-R) mitochondrial rRNA mutation. Lastly, in vivo mtDNA translation was impaired in the mutant yeast strains.

Published

2012

17. Characterization of Human GTPBP3, a GTP-Binding Protein Involved in Mitochondrial tRNA Modification

Author

Magda Villarroya, Juan M. Esteve, David Perez-Martinez, Silvia Prado, Carmen Aguado, Miguel A. Soriano, Lucía Yim, Victor M. Victor, Erwin Knecht, Asunción Montaner, M.-Eugenia Armengod, Elvira Cebolla, and José I. Martínez-Ferrandis

Subjects

TRNA modification, Protein family, GTPase, Mitochondrion, Biology, Cell Line, GTP Phosphohydrolases, Gene Knockout Techniques, Mice, Oxygen Consumption, GTP-binding protein regulators, RNA, Transfer, GTP-Binding Proteins, Animals, Humans, Protein Isoforms, RNA, Small Interfering, Binding site, Molecular Biology, Molecular Structure, Escherichia coli Proteins, Mitochondrial tRNA modification, Exons, Articles, Cell Biology, Guanine Nucleotides, Introns, Mitochondria, Alternative Splicing, Gene Expression Regulation, Biochemistry, GTPBP3

Abstract

Human GTPBP3 is an evolutionarily conserved, multidomain protein involved in mitochondrial tRNA modification. Characterization of its biochemical properties and the phenotype conferred by GTPBP3 inactivation is crucial to understanding the role of this protein in tRNA maturation and its effects on mitochondrial respiration. We show that the two most abundant GTPBP3 isoforms exhibit moderate affinity for guanine nucleotides like their bacterial homologue, MnmE, although they hydrolyze GTP at a 100-fold lower rate. This suggests that regulation of the GTPase activity, essential for the tRNA modification function of MnmE, is different in GTPBP3. In fact, potassium-induced dimerization of the G domain leads to stimulation of the GTPase activity in MnmE but not in GTPBP3. The GTPBP3 N-terminal domain mediates a potassium-independent dimerization, which appears as an evolutionarily conserved property of the protein family, probably related to the construction of the binding site for the one-carbon-unit donor in the modification reaction. Partial inactivation of GTPBP3 by small interfering RNA reduces oxygen consumption, ATP production, and mitochondrial protein synthesis, while the degradation of these proteins slightly increases. It also results in mitochondria with defective membrane potential and increased superoxide levels. These phenotypic traits suggest that GTPBP3 defects contribute to the pathogenesis of some oxidative phosphorylation diseases.

Published

2008

18. Defective Expression of the Mitochondrial-tRNA Modifying Enzyme GTPBP3 Triggers AMPK-Mediated Adaptive Responses Involving Complex I Assembly Factors, Uncoupling Protein 2, and the Mitochondrial Pyruvate Carrier

Author

Salvador Meseguer, Ana Martínez-Zamora, M.-Eugenia Armengod, Juan M. Esteve, Magda Villarroya, Carmen Aguado, Erwin Knecht, J. Antonio Enríquez, Ministerio de Economía y Competitividad (España), Generalitat Valenciana (España), and Instituto de Salud Carlos III

Subjects

Monocarboxylic Acid Transporters, FATTY-ACID OXIDATION, CELL-SURVIVAL, Mitochondrial translation, Pyruvate transport, Anion Transport Proteins, lcsh:Medicine, Oxidative phosphorylation, Biology, Mitochondrion, AMP-Activated Protein Kinases, ROS PRODUCTION, Mitochondrial Membrane Transport Proteins, Ion Channels, Oxidative Phosphorylation, Mitochondrial Proteins, Adenosine Triphosphate, H2O2 GENERATION, GTP-Binding Proteins, Escherichia coli, Uncoupling protein, Humans, Glycolysis, Uncoupling Protein 2, LACTIC-ACIDOSIS, lcsh:Science, Beta oxidation, Multidisciplinary, Electron Transport Complex I, HYPERTROPHIC CARDIOMYOPATHY, lcsh:R, Fatty Acids, PHYSIOLOGICALLY RELEVANT, Ribonuclease, Pancreatic, Mitochondria, HEK293 Cells, Biochemistry, Gene Expression Regulation, ESCHERICHIA-COLI, GLUTAMINE OXIDATION, RNA, Transfer, Lys, lcsh:Q, Calmodulin-Binding Proteins, GTPBP3, RESPIRATORY-CHAIN DEFICIENCY, Research Article

Abstract

GTPBP3 is an evolutionary conserved protein presumably involved in mitochondrial tRNA (mt-tRNA) modification. In humans, GTPBP3 mutations cause hypertrophic cardiomyopathy with lactic acidosis, and have been associated with a defect in mitochondrial translation, yet the pathomechanism remains unclear. Here we use a GTPBP3 stable-silencing model (shGTPBP3 cells) for a further characterization of the phenotype conferred by the GTPBP3 defect. We experimentally show for the first time that GTPBP3 depletion is associated with an mt-tRNA hypomodification status, as mt-tRNAs from shGTPBP3 cells were more sensitive to digestion by angiogenin than tRNAs from control cells. Despite the effect of stable silencing of GTPBP3 on global mitochondrial translation being rather mild, the steady-state levels and activity of Complex I, and cellular ATP levels were 50\% of those found in the controls. Notably, the ATPase activity of Complex V increased by about 40\% in GTPBP3 depleted cells suggesting that mitochondria consume ATP to maintain the membrane potential. Moreover, shGTPBP3 cells exhibited enhanced antioxidant capacity and a nearly 2-fold increase in the uncoupling protein UCP2 levels. Our data indicate that stable silencing of GTPBP3 triggers an AMPK-dependent retrograde signaling pathway that down-regulates the expression of the NDUFAF3 and NDUFAF4 Complex I assembly factors and the mitochondrial pyruvate carrier (MPC), while up-regulating the expression of UCP2. We also found that genes involved in glycolysis and oxidation of fatty acids are up-regulated. These data are compatible with a model in which high UCP2 levels, together with a reduction in pyruvate transport due to the down-regulation of MPC, promote a shift from pyruvate to fatty acid oxidation, and to an uncoupling of glycolysis and oxidative phosphorylation. These metabolic alterations, and the low ATP levels, may negatively affect heart function. This work has been supported by grants from the Spanish Ministry of Economy and Competitiveness (http://www.mineco.gob.es/portal/site/mineco/) (grant numbers BFU2010-19737 and BFU2014-58673-P to M.-E. A., BFU2011-22630 and SAF2014-54604-C3-2-R to E.K.) and the Generalitat Valenciana (http://www.gva.es/va/inicio/presentacion) (grant numbers ACOMP/2012/065 to M.-E. A., and PROMETEO/2012/061 to M.-E. A. and E.K.), and a PhD fellowship from the Instituto de Salud Carlos III (http://www.isciii.es/) to A.M.-Z. The funders had no role in study design, data collection and analysis, decision to publish, or preparation of the manuscript. Sí

Published

2015

19. Mitochondria-specific RNA-modifying Enzymes Responsible for the Biosynthesis of the Wobble Base in Mitochondrial tRNAs

Author

Kimitsuna Watanabe, Heisaburo Shindo, Takeo Suzuki, Masashi Yukawa, Noriko Umeda, Yoshikazu Ohya, and Tsutomu Suzuki

Subjects

Mutation, RNA, Cell Biology, Wobble base pair, Biology, Mitochondrion, medicine.disease_cause, Biochemistry, Uridine, chemistry.chemical_compound, chemistry, Transfer RNA, medicine, GTPBP3, Molecular Biology, Gene

Abstract

Human mitochondrial (mt) tRNALys has a taurine-containing modified uridine, 5-taurinomethyl-2-thiouridine (τm5s2U), at its anticodon wobble position. We previously found that the mt tRNALys, carrying the A8344G mutation from cells of patients with myoclonus epilepsy associated with ragged-red fibers (MERRF), lacks the τm5s2U modification. Here we describe the identification and characterization of a tRNA-modifying enzyme MTU1 (mitochondrial tRNA-specific 2-thiouridylase 1) that is responsible for the 2-thiolation of the wobble position in human and yeast mt tRNAs. Disruption of the yeast MTU1 gene eliminated the 2-thio modification of mt tRNAs and impaired mitochondrial protein synthesis, which led to reduced respiratory activity. Furthermore, when MTO1 or MSS1, which are responsible for the C5 substituent of the modified uridine, was disrupted along with MTU1, a much more severe reduction in mitochondrial activity was observed. Thus, the C5 and 2-thio modifications act synergistically in promoting efficient cognate codon decoding. Partial inactivation of MTU1 in HeLa cells by small interference RNA also reduced their oxygen consumption and resulted in mitochondria with defective membrane potentials, which are similar phenotypic features observed in MERRF., This work was supported by grants-in-aid for scientific research on priority areas from the Ministry of Education, Science, Sports, and Culture of Japan, and by a grant from the New Energy and Industrial Technology Development Organization (to T. S.).

Published

2005

20. Phenotype of non-syndromic deafness associated with the mitochondrial A1555G mutation is modulated by mitochondrial RNA modifying enzymes MTO1 and GTPBP3

Author

Huiying Yang, Xavier Estivill, Dai Wang, Yelena Bykhovskaya, Nathan Fischel-Ghodsian, Mordechai Shohat, and Emebet Mengesha

Subjects

Linkage disequilibrium, Endocrinology, Diabetes and Metabolism, Deafness, Biology, MT-RNR1, Polymorphism, Single Nucleotide, Biochemistry, Linkage Disequilibrium, Mitochondrial Proteins, Endocrinology, RRNA modification, GTP-Binding Proteins, Genetic linkage, Genetics, Humans, Computer Simulation, Israel, RNA Processing, Post-Transcriptional, Molecular Biology, Gene, TFB1M, Nuclear Proteins, RNA-Binding Proteins, Sequence Analysis, DNA, Mitochondrial RNA modification, Molecular biology, Mitochondria, Pedigree, DNA-Binding Proteins, Gene Components, Phenotype, Italy, RNA, Ribosomal, Spain, Mutation, Carrier Proteins, GTPBP3, Chromosomes, Human, Pair 8, Microsatellite Repeats, Transcription Factors

Abstract

Phenotypic expression of the deafness-associated mitochondrial A1555G mutation in the 12S rRNA gene is influenced by aminoglycosides and complex inheritance of nuclear-encoded modifier genes. The position of a major nuclear modifier gene has been localized to chromosome 8p23.1, but the identification of this gene has remained elusive. Recently, we identified a second modifier gene, mitochondrial transcription factor B1 (TFB1M), involved in mitochondrial rRNA modification. In the present study, we tested three genes involved in mitochondrial tRNA or rRNA modification, and two genes associated with non-syndromic deafness, for linkage and linkage disequilibrium (LD) in 214 DNA samples from Spanish, Italian, and Arab-Israeli families with maternally inherited non-syndromic hearing loss. The multipoint non-parametric linkage analysis and transmission disequilibrium test testing were done using all families combined as well as divided based on linkage to the chromosome 8 locus and ethnicity. Two genes, MTO1 and GTPBP3, showed strongly suggestive linkage and significant LD results. Since both genes, as well as TFB1M, are involved in the process of mitochondrial RNA modification, it appears that the modification of mitochondrial RNA is an important regulatory pathway in the phenotypic expression of the deafness-associated mitochondrial A1555G mutation. This conclusion was supported by comparing linkage results of simulated genotypes with actual results for the four genes involved in mitochondrial RNA modification.

Published

2004

21. Identification and characterization of mouse GTPBP3 gene encoding a mitochondrial GTP-binding protein involved in tRNA modification

Author

Xiaoming Li and Min-Xin Guan

Subjects

TRNA modification, Translational efficiency, Molecular Sequence Data, Biophysics, Mitochondrion, Biology, Biochemistry, Gene Expression Regulation, Enzymologic, Mice, RNA, Transfer, Species Specificity, GTP-Binding Proteins, Complementary DNA, Mitochondrial ribosome, Animals, Humans, Tissue Distribution, Amino Acid Sequence, Molecular Biology, HSPA9, Sequence Homology, Amino Acid, Gene Expression Profiling, Nuclear Proteins, Cell Biology, Fusion protein, Molecular biology, Mitochondria, Cell biology, Organ Specificity, NIH 3T3 Cells, GTPBP3, Sequence Alignment

Abstract

We report here the identification and characterization of mouse GTPBP3 encoding a mitochondrial GTPase. A full-length GTPBP3 cDNA has been isolated and the genomic organization of GTPBP3 has been elucidated. The mouse GTPBP3 gene containing 9 exons encodes a 486 residue protein with a strong homology to the GTPBP3-like proteins of bacteria, yeast, and other homologs, related to tRNA modification. The mouse GTPBP3 is ubiquitously expressed in various tissues, but abundantly in tissues with high metabolic rates including heart, liver, and brain. Surprisingly, this gene, unlike its human homolog, exhibited a low expression in skeletal muscle. Furthermore, immunofluorescence analysis of NIH3T3 cells expressing GTPBP3-GFP fusion protein demonstrated that the mouse Gtpbp3 localizes in mitochondrion. These observations suggest that the mouse Gtpbp3 is an evolutionarily conserved mitochondrial GTP-binding protein involved in the tRNA modification. Thus, it may modulate the translational efficiency and accuracy of codon-anticodon base pairings on the decoding region of mitochondrial ribosomes.

Published

2003

22. Caracterización funcional de GTPBP3: una proteína G implicada en la modificación de tRNAs mitocondriales

Author

Martínez Zamora, Ana, Armengod González, María Eugenia, Knecht Roberto, Erwin Carlos, Esteve Esteve, Juan Miguel, and Departament de Bioquímica i Biologia Molecular

Subjects

metabolismo mitocondrial, tRNA mitocondrial, UNESCO::CIENCIAS DE LA VIDA, gtpbp3, CIENCIAS DE LA VIDA [UNESCO], oxphos, modificación trna

Abstract

Determinadas enfermedades mitocondriales, como MELAS (mitochondrial myopathy, encephalopathy, lactic acidosis and stroke-like episodes), MERRF (myoclonus epilepsy associated with ragged-red-fibers), cardiomiopatía hipertrófica y acidosis láctica dependiente de GTPBP3, cardiomiopatía hipertrófica infantil y acidosis láctica dependiente de MTO1 y fallo hepático infantil agudo dependiente de TRMU, están asociadas con una disfunción severa del sistema de fosforilación oxidativa (OXPHOS) que, se cree, podría ser resultado de defectos en la modificación postranscripcional de la uridina localizada en la posición de tambaleo (U34) de ciertos tRNAs mitocondriales (mt-tRNAs) y, por consiguiente, de un mal funcionamiento de la traducción mitocondrial. A partir de la alta conservación evolutiva del proceso de modificación de la U34 se ha sugerido que las proteínas humanas TRMU, GTPBP3 y MTO1 desempeñan las mismas funciones que sus homólogas en levaduras y bacterias. GTPBP3 y MTO1 se encargarían de introducir el grupo taurinometil en la posición 5 de la U34 en los mt-tRNAs Leu, Lys, Glu, Gln y Trp, mientras que, TRMU introduce el grupo tiol en la posición 2 de la U34 de los mt-tRNAs Lys, Glu y Gln. En humanos, mutaciones en GTPBP3 causan cardiomiopatía hipertrófica y acidosis láctica, y han sido asociadas con defecto en la traducción mitocondrial, aunque el mecanismo patogénico no está claro. En esta tesis utilizamos un sistema modelo donde GTPBP3 se encuentra silenciado establemente (células shGTPBP3) para conseguir una caracterización más profunda del fenotipo conferido por la deficiencia de GTPBP3 y poder estudiar el mecanismo molecular subyacente. Usando un ensayo de sensibilidad a la digestión por angiogenina de los mt-tRNAs, que validamos con tRNAs de Escherichia coli, demostramos experimentalmente por primera vez que la falta de GTPBP3 está asociada con hipomodificación del mt-tRNA, puesto que los mt-tRNAs de las células silenciadas para GTPBP3 son más sensibles a la digestión con angiogenina que los de las células control. A pesar de que el efecto del silenciamiento estable de GTPBP3 sobre la síntesis mitocondrial de proteínas global es bastante suave, observamos una disminución del 50% en los niveles estacionarios y actividad del Complejo I del sistema OXPHOS, así como en los niveles de ATP celular en las células shGTPBP3 respecto a las células control. Llamativamente, la actividad ATPasa del Complejo V se encuentra incrementada un 40% en las células shGTPBP3, sugiriendo que la mitocondria consume ATP para mantener el potencial de membrana mitocondrial. Además, las células shGTPBP3 exhiben una capacidad antioxidante aumentada y un incremento de casi dos veces en los niveles de la proteína desacoplante UCP2. Los datos obtenidos indican que el silenciamiento estable de GTPBP3 inicia una señalización retrógrada dependiente de AMPK que disminuye los niveles de mRNA de los factores de ensamblaje del Complejo I NDUFAF3 y NDUFAF4 y la expresión (a nivel de mRNA y de proteína) del transportador del piruvato (MPC), mientras que favorece la sobreexpresión de UCP2. Además, hemos observado sobreexpresión de algunos genes implicados en glucólisis y oxidación de ácidos grasos. Estos datos son compatibles con un modelo donde los altos niveles de UCP2 junto con la reducción del transportador del piruvato MPC promueven un cambio metabólico, disminuyendo la oxidación del piruvato en la mitocondria y favoreciendo su utilización por parte de lactato deshidrogenasa mientras que se estimula la oxidación de ácidos grasos. Este cambio metabólico produciría un desacople entre la glucólisis y la fosforilación oxidativa y esta alteración metabólica, junto con los bajos niveles de ATP, puede afectar negativamente la función del corazón. GTPBP3 is an evolutionary conserved protein presumably involved in mitochondrial tRNA (mt-tRNA) modification. In humans, GTPBP3 mutations cause hypertrophic cardiomyopathy with lactic acidosis, and have been associated with a defect in mitochondrial translation, yet the pathomechanism remains unclear. Here we use a GTPBP3 stable-silencing model (shGTPBP3 cells) for a further characterization of the phenotype conferred by the GTPBP3 defect. We experimentally show for the first time that GTPBP3 depletion is associated with an mt-tRNA hypomodification status, as mt-tRNAs from shGTPBP3 cells were more sensitive to digestion by angiogenin than tRNAs from control cells. Despite the effect of stable silencing of GTPBP3 on global mitochondrial translation being rather mild, the steady-state levels and activity of Complex I, and cellular ATP levels were 50% of those found in the controls. Notably, the ATPase activity of Complex V increased by about 40% in GTPBP3 depleted cells suggesting that mitochondria consume ATP to maintain the membrane potential. Moreover, shGTPBP3 cells exhibited enhanced antioxidant capacity and a nearly 2-fold increase in the uncoupling protein UCP2 levels. Our data indicate that stable silencing of GTPBP3 triggers an AMPK-dependent retrograde signaling pathway that down-regulates the expression of the NDUFAF3 and NDUFAF4 Complex I assembly factors and the mitochondrial pyruvate carrier (MPC), while up-regulating the expression of UCP2. We also found that genes involved in glycolysis and oxidation of fatty acids are up-regulated. These data are compatible with a model in which high UCP2 levels, together with a reduction in pyruvate transport due to the down-regulation of MPC, promote a shift from pyruvate to fatty acid oxidation, and to an uncoupling of glycolysis and oxidative phosphorylation. These metabolic alterations, and the low ATP levels, may negatively affect heart functi

Published

2015

23. The ROS-sensitive microRNA-9/9*controls the expression of mitochondrial tRNA-modifying enzymes and is involved in the molecular mechanism of MELAS syndrome

Author

Antonio L. Andreu, Salvador Meseguer, Ana Martínez-Zamora, M.-Eugenia Armengod, and Elena García-Arumí

Subjects

RNA, Transfer, Leu, RNA, Mitochondrial, Down-Regulation, Mitochondrion, Biology, MELAS syndrome, Mitochondrial Proteins, GTP-Binding Proteins, Genetics, Transcriptional regulation, medicine, MELAS Syndrome, Humans, Molecular Biology, Gene, Genetics (clinical), Cells, Cultured, Cell Nucleus, tRNA Methyltransferases, NF-kappa B, RNA-Binding Proteins, General Medicine, medicine.disease, Phenotype, Mitochondria, MicroRNAs, Oxidative Stress, Transfer RNA, RNA, Signal transduction, GTPBP3, Carrier Proteins, Reactive Oxygen Species, Signal Transduction

Abstract

Mitochondrial dysfunction activates mitochondria-to-nucleus signaling pathways whose components are mostly unknown. Identification of these components is important to understand the molecular mechanisms underlying mitochondrial diseases and to discover putative therapeutic targets. MELAS syndrome is a rare neurodegenerative disease caused by mutations in mitochondrial (mt) DNA affecting mt-tRNA(Leu(UUR)). Patient and cybrid cells exhibit elevated oxidative stress. Moreover, mutant mt-tRNAs(Leu(UUR)) lack the taurine-containing modification normally present at the wobble uridine (U34) of wild-type mt-tRNA(Leu(UUR)), which is considered an etiology of MELAS. However, the molecular mechanism is still unclear. We found that MELAS cybrids exhibit a significant decrease in the steady-state levels of several mt-tRNA-modification enzymes, which is not due to transcriptional regulation. We demonstrated that oxidative stress mediates an NFkB-dependent induction of microRNA-9/9*, which acts as a post-transcriptional negative regulator of the mt-tRNA-modification enzymes GTPBP3, MTO1 and TRMU. Down-regulation of these enzymes by microRNA-9/9* affects the U34 modification status of non-mutant tRNAs and contributes to the MELAS phenotype. Anti-microRNA-9 treatments of MELAS cybrids reverse the phenotype, whereas miR-9 transfection of wild-type cells mimics the effects of siRNA-mediated down-regulation of GTPBP3, MTO1 and TRMU. Our data represent the first evidence that an mt-DNA disease can directly affect microRNA expression. Moreover, we demonstrate that the modification status of mt-tRNAs is dynamic and that cells respond to stress by modulating the expression of mt-tRNA-modifying enzymes. microRNA-9/9* is a crucial player in mitochondria-to-nucleus signaling as it regulates expression of nuclear genes in response to changes in the functional state of mitochondria.

Published

2015

24. A Human Mitochondrial GTP Binding Protein Related to tRNA Modification May Modulate Phenotypic Expression of the Deafness-Associated Mitochondrial 12S rRNA Mutation

Author

Xiaoming Li and Min-Xin Guan

Subjects

Glycerol, TRNA modification, DNA, Complementary, Saccharomyces cerevisiae Proteins, Molecular Sequence Data, Mutant, Gene Expression, Saccharomyces cerevisiae, Deafness, Mitochondrion, Biology, medicine.disease_cause, GTP Phosphohydrolases, RNA, Transfer, GTP-Binding Proteins, Escherichia coli, medicine, Humans, Tissue Distribution, Amino Acid Sequence, RNA, Messenger, Cloning, Molecular, Molecular Biology, Alleles, Suppressor mutation, Genetics, Mutation, Base Sequence, Models, Genetic, Sequence Homology, Amino Acid, Genetic Complementation Test, Nuclear Proteins, Mitochondrial tRNA modification, Cell Biology, Mitochondria, Glucose, Phenotype, Microscopy, Fluorescence, RNA, Ribosomal, DNAJA3, Nucleic Acid Conformation, GTPBP3, Protein Binding

Abstract

Human mitochondrial 12S rRNA A1555G mutation has been found to be associated with deafness. However, putative nuclear modifier gene(s) has been proposed to regulate the phenotypic expression of this mutation. In yeast cells, mutant alleles of MSS1, encoding a mitochondrial GTP-binding protein, manifest a respiratory-deficient phenotype only when coupled with mitochondrial 15S rRNA P(R)(454) mutation corresponding to human A1555G mutation. This suggests that an MSS1-like modifier gene may influence the phenotypic expression of the A1555G mutation. We report here the identification and characterization of human MSS1 homolog, GTPBP3, the first identified vertebrate gene related to mitochondrial tRNA modification. The Gtpbp3 is the mitochondrial GTPase evolutionarily conserved from bacteria to mammals. Functional conservation of this protein is supported by the observation that isolated human GTPBP3 cDNA can complement the respiratory-deficient phenotype of yeast mss1 cells carrying P(R)(454) mutation. GTPBP3 is ubiquitously expressed in various tissues as multiple transcripts, but with a markedly elevated expression in tissues of high metabolic rates. We showed that Gtpbp3 localizes in mitochondrion. These observations suggest that the human GTPBP3 is a structural and functional homolog of yeast MSS1. Thus, allelic variants in GTPBP3 could, if they exist, modulate the phenotypic manifestation of human mitochondrial A1555G mutation.

Published

2002

25. Isolation and Characterization of the Putative Nuclear Modifier Gene MTO1 Involved in the Pathogenesis of Deafness-associated Mitochondrial 12 S rRNA A1555G Mutation

Author

Xinhua Lin, Xiaoming Li, Ronghua Li, and Min-Xin Guan

Subjects

Glycerol, DNA, Complementary, Saccharomyces cerevisiae Proteins, Molecular Sequence Data, Mutant, Saccharomyces cerevisiae, Biology, Transfection, medicine.disease_cause, Biochemistry, Protein Structure, Secondary, Mitochondrial Proteins, RNA, Transfer, Complementary DNA, Tumor Cells, Cultured, medicine, Humans, Tissue Distribution, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, Gene, Alleles, Suppressor mutation, Expressed Sequence Tags, Genetics, Mutation, Models, Genetic, Sequence Homology, Amino Acid, Reverse Transcriptase Polymerase Chain Reaction, Genetic Complementation Test, RNA-Binding Proteins, Mitochondrial tRNA modification, Exons, Cell Biology, Introns, Mitochondria, Alternative Splicing, Glucose, Phenotype, Microscopy, Fluorescence, RNA, Ribosomal, Transfer RNA, Carrier Proteins, GTPBP3

Abstract

The human mitochondrial 12 S rRNA A1555G mutation has been found to be associated with aminoglycoside-induced and non-syndromic deafness. However, putative nuclear modifier gene(s) have been proposed to regulate the phenotypic expression of this mutation. In yeast, the mutant alleles of MTO1, encoding a mitochondrial protein, manifest respiratory-deficient phenotype only when coupled with the mitochondrial 15 S rRNA P(R)454 mutation corresponding to human A1555G mutation. This suggests that the MTO1-like modifier gene may influence the phenotypic expression of human A1555G mutation. Here we report the identification of full-length cDNA and elucidation of genomic organization of the human MTO1 homolog. Human Mto1 is an evolutionarily conserved protein that implicates a role in the mitochondrial tRNA modification. Functional conservation of this protein is supported by the observation that isolated human MTO1 cDNA can complement the respiratory deficient phenotype of yeast mto1 cells carrying P(R)454 mutation. MTO1 is ubiquitously expressed in various tissues, but with a markedly elevated expression in tissues of high metabolic rates including cochlea. These observations suggest that human MTO1 is a structural and functional homolog of yeast MTO1. Thus, it may play an important role in the pathogenesis of deafness-associated A1555G mutation in 12 S rRNA gene or mutations in tRNA genes.

Published

2002

26. Mutations in GTPBP3 cause a mitochondrial translation defect associated with hypertrophic cardiomyopathy, lactic acidosis, and encephalopathy

Author

Rosalba Carrozzo, Abraham Lorber, Kei Murayama, Michal Minczuk, Tom Sante, Björn Menten, Joél Smet, Massimo Zeviani, Dominique Chretien, Marlène Rio, Sarah F. Pearce, Joanna Rorbach, Yoshimi Tokuzawa, Thomas Schwarzmayr, Daniele Ghezzi, Agnès Rötig, Patrick F. Chinnery, Asaad Khoury, Yoshihito Kishita, Ellen Crushell, François Feillet, Enrico Bertini, Peter Freisinger, Robert W. Taylor, Ewen W. Sommerville, Thomas Meitinger, Luc Régal, Arnold Munnich, Thomas Wieland, Thomas Klopstock, Robert Kopajtich, Johannes A. Mayr, Holger Prokisch, Bénédict Mousson de Camaret, Rudy Van Coster, Tim M. Strom, Hanna Mandel, Yasushi Okazaki, Zahra Assouline, Angela Pyle, Arnaud Vanlander, Tobias B. Haack, Masakazu Kohda, Metodi D. Metodiev, Thomas J. Nicholls, Christopher A. Powell, Akira Ohtake, Federica Invernizzi, Klaus Marquard, Eleonora Lamantea, Ann Saada, Helmholtz-Zentrum München (HZM), MRC Mitochondrial Biology Unit, University of Cambridge [UK] (CAM), Imagine - Institut des maladies génétiques (IMAGINE - U1163), Centre National de la Recherche Scientifique (CNRS)-Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM), Reutlingen University, Rambam Health Care Campus, Department of Pediatric Neurology and Metabolism [Ghent], Ghent University Hospital, Fondazione IRCCS Istituto Neurologico 'Carlo Besta', Dipartimento di Neuroscienze [IRCCS Gesù Roma], IRCCS Ospedale Pediatrico Bambino Gesù [Roma], Wellcome Trust Centre for Mitochondrial Research, Newcastle University [Newcastle]-International Centre for Life-Institute of Genetic Medicine, Klinikum Stuttgart, Department of Metabolism [Chiba], Children's Hospital Chiba, Institute of Human Genetics, Technische Universität München [München] (TUM)-Helmholtz-Zentrum München (HZM)-German Research Center for Environmental Health, Paracelsus Medical University and Universitätsklinikum Salzburg, Department of Genetics and Metabolic Diseases and the Monique and Jacques Roboh Department of Genetic Research, Hadassah Hebrew University Medical Center [Jerusalem], Saitama Medical University, National Centre for Inherited Metabolic Disorders [Dublin], Temple Street Children's University Hospital [Dublin], Saitama University, Service de Génétique Médicale [CHU Necker], Assistance publique - Hôpitaux de Paris (AP-HP) (APHP)-CHU Necker - Enfants Malades [AP-HP], Nutrition-Génétique et Exposition aux Risques Environnementaux (NGERE), Université de Lorraine (UL)-Institut National de la Santé et de la Recherche Médicale (INSERM), Service de Médecine Infantile I [CHRU Nancy], Centre Hospitalier Régional Universitaire de Nancy (CHRU Nancy), Service des Maladies Héréditaires du Métabolisme, Hospices Civils de Lyon (HCL)-Centre de Biologie et de pathologie Est, Center for Medical Genetics [Ghent], Hôpitaux universitaires de Louvain, German Center for Cardiovascular Research (DZHK), Berlin Institute of Health (BIH), Munich Heart Alliance, Munich Cluster for systems neurology [Munich] (SyNergy), Technische Universität München [München] (TUM)-Ludwig-Maximilians-Universität München (LMU), German Research Center for Neurodegenerative Diseases - Deutsches Zentrum für Neurodegenerative Erkrankungen (DZNE), Friedrich-Baur Institute, Ludwig-Maximilians-Universität München (LMU), Université Paris Descartes - Paris 5 (UPD5)-Institut National de la Santé et de la Recherche Médicale (INSERM), Technische Universität Munchen - Université Technique de Munich [Munich, Allemagne] (TUM)-Helmholtz-Zentrum München (HZM)-German Research Center for Environmental Health, CHU Necker - Enfants Malades [AP-HP], Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP)-Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Lorraine (UL), Centre de Biologie et de pathologie Est-Hospices Civils de Lyon (HCL), and Technische Universität Munchen - Université Technique de Munich [Munich, Allemagne] (TUM)-Ludwig-Maximilians-Universität München (LMU)

Subjects

Male, Mitochondrial translation, [SDV]Life Sciences [q-bio], Respiratory chain, medicine.disease_cause, Consanguinity, RNA, Transfer, pathology [Brain], Genetics(clinical), Child, metabolism [GTP-Binding Proteins], metabolism [RNA, Transfer], Genetics (clinical), Genetics, Mutation, physiopathology [Acidosis, Lactic], Brain Diseases, genetics [Cardiomyopathy, Hypertrophic], Lactic, Respiratory chain complex, genetics [Brain Diseases], Brain, 3. Good health, Pedigree, genetics [Acidosis, Lactic], Lactic acidosis, Child, Preschool, genetics [RNA, Transfer], Acidosis, Lactic, Female, RNA Interference, GTPBP3, Acidosis, GTPBP3 protein, human, Mitochondrial DNA, genetics [GTP-Binding Proteins], Cardiomyopathy, Molecular Sequence Data, Biology, Human mitochondrial genetics, Cell Line, GTP-Binding Proteins, ddc:570, Report, medicine, Humans, Amino Acid Sequence, Preschool, Protein Processing, physiopathology [Cardiomyopathy, Hypertrophic], Post-Translational, Infant, Newborn, Infant, Cardiomyopathy, Hypertrophic, Fibroblasts, medicine.disease, Newborn, Transfer, Protein Biosynthesis, Sequence Alignment, Protein Processing, Post-Translational, Hypertrophic, physiopathology [Brain Diseases], RNA

Abstract

International audience; Respiratory chain deficiencies exhibit a wide variety of clinical phenotypes resulting from defective mitochondrial energy production through oxidative phosphorylation. These defects can be caused by either mutations in the mtDNA or mutations in nuclear genes coding for mitochondrial proteins. The underlying pathomechanisms can affect numerous pathways involved in mitochondrial physiology. By whole-exome and candidate gene sequencing, we identified 11 individuals from 9 families carrying compound heterozygous or homozygous mutations in GTPBP3, encoding the mitochondrial GTP-binding protein 3. Affected individuals from eight out of nine families presented with combined respiratory chain complex deficiencies in skeletal muscle. Mutations in GTPBP3 are associated with a severe mitochondrial translation defect, consistent with the predicted function of the protein in catalyzing the formation of 5-taurinomethyluridine (τm(5)U) in the anticodon wobble position of five mitochondrial tRNAs. All case subjects presented with lactic acidosis and nine developed hypertrophic cardiomyopathy. In contrast to individuals with mutations in MTO1, the protein product of which is predicted to participate in the generation of the same modification, most individuals with GTPBP3 mutations developed neurological symptoms and MRI involvement of thalamus, putamen, and brainstem resembling Leigh syndrome. Our study of a mitochondrial translation disorder points toward the importance of posttranscriptional modification of mitochondrial tRNAs for proper mitochondrial function.

Published

2014

27. A complete landscape of post-transcriptional modifications in mammalian mitochondrial tRNAs

Author

Tsutomu Suzuki and Takeo Suzuki

Subjects

Genetics, Mitochondrial DNA, RNA, Mitochondrial, Respiratory chain, RNA, Oxidative phosphorylation, Mitochondrion, Biology, environment and public health, Biochemistry, RNA, Transfer, Transcription (biology), Transfer RNA, Animals, Cattle, RNA Processing, Post-Transcriptional, GTPBP3

Abstract

In mammalian mitochondria, 22 species of tRNAs encoded in mitochondrial DNA play crucial roles in the translation of 13 essential subunits of the respiratory chain complexes involved in oxidative phosphorylation. Following transcription, mitochondrial tRNAs are modified by nuclear-encoded tRNA-modifying enzymes. These modifications are required for the proper functioning of mitochondrial tRNAs (mt tRNAs), and the absence of these modifications can cause pathological consequences. To date, however, the information available about these modifications has been incomplete. To address this issue, we isolated all 22 species of mt tRNAs from bovine liver and comprehensively determined the post-transcriptional modifications in each tRNA by mass spectrometry. Here, we describe the primary structures with post-transcriptional modifications of seven species of mt tRNAs which were previously uncharacterized, and provide revised information regarding base modifications in five other mt tRNAs. In the complete set of bovine mt tRNAs, we found 15 species of modified nucleosides at 118 positions (7.48% of total bases). This result provides insight into the molecular mechanisms underlying the decoding system in mammalian mitochondria and enables prediction of candidate tRNA-modifying enzymes responsible for each modification of mt tRNAs.

Published

2014

28. MTO1 Codes for a Mitochondrial Protein Required for Respiration in Paromomycin-resistant Mutants of Saccharomyces cerevisiae

Author

Geoffrey P. Colby, Mian Wu, and Alexander Tzagoloff

Subjects

Mitochondrial DNA, Saccharomyces cerevisiae Proteins, Paromomycin, Mitochondrial translation, Protein subunit, Genes, Fungal, Saccharomyces cerevisiae, Mutant, Cytochrome a Group, DNA, Mitochondrial, Biochemistry, GTP Phosphohydrolases, Electron Transport, Electron Transport Complex IV, Mitochondrial Proteins, Oxygen Consumption, GTP-Binding Proteins, Cytochrome c oxidase, Cloning, Molecular, RNA Processing, Post-Transcriptional, Molecular Biology, Gene, biology, Genetic Complementation Test, RNA-Binding Proteins, Drug Resistance, Microbial, NADH Dehydrogenase, Sequence Analysis, DNA, Cell Biology, Cytochrome b Group, biology.organism_classification, Anti-Bacterial Agents, Cell Compartmentation, Mitochondria, Phenotype, biology.protein, Succinate Cytochrome c Oxidoreductase, Carrier Proteins, GTPBP3, Protein Binding

Abstract

Mutations in MTO1 express a respiratory defect only in the context of a mitochondrial genome with a paromomycin-resistance allele. This phenotype is similar to that described previously for mss1 mutants by Decoster, E., Vassal, A., and Faye, G. (1993) J. Mol. Biol. 232, 79–88. We present evidence that Mto1p and Mss1p are mitochondrial proteins and that they form a heterodimer complex. In a paromomycin-resistant background, mss1 and mto1 mutants are inefficient in processing the mitochondrial COX1 transcript for subunit 1 of cytochrome oxidase. The mutants also fail to synthesize subunit 1 and show a pleiotropic absence of cytochromes a, a 3, and b. In vivo pulse labeling of an mto1 mutant, however, indicate increased rates of synthesis of other mitochondrial translation products. The respiratory defective phenotype of mto1 and mss1 mutants is not seen in a paromomycin-sensitive genetic background. The visible absorption spectra of such strains indicate a higher ratio of cytochromes b/a and elevated NADH- and succinate-cytochromec reductase activities. To explain these phenotypic characteristics, we proposed that the Mto1p·Mss1p complex plays a role in optimizing mitochondrial protein synthesis in yeast, possibly by a proofreading mechanism.

Published

1998

29. MTO1 mutations are associated with hypertrophic cardiomyopathy and lactic acidosis and cause respiratory chain deficiency in humans and yeast

Author

Saikat Santra, Emma L. Blakely, Enrico Baruffini, Daniele Ghezzi, Robert W. Taylor, Cristina Dallabona, Holger Prokisch, Claudia Donnini, Suresh Vijayaraghavan, Helen Roper, Tobias B. Haack, Tim M. Strom, Ileana Ferrero, Alberto Burlina, Laura Melchionda, Massimo Zeviani, Eleonora Lamantea, Anett Walther, John W. Yarham, Robert Kopajtich, and Federica Invernizzi

Subjects

Male, Models, Molecular, Candidate gene, Protein Conformation, MTO1, DNA Mutational Analysis, yeast, medicine.disease_cause, 0302 clinical medicine, Models, Yeasts, Missense mutation, Age of Onset, Child, Genetics (clinical), Exome sequencing, Research Articles, 2. Zero hunger, Genetics, 0303 health sciences, Mutation, Lactic, Brain, RNA-Binding Proteins, Phenotype, Magnetic Resonance Imaging, 3. Good health, Pedigree, lactic acidosis, Mitochondrial respiratory chain, Lactic acidosis, Child, Preschool, Acidosis, Lactic, Female, GTPBP3, Acidosis, Adolescent, Cardiomyopathy, Molecular Sequence Data, Biology, 03 medical and health sciences, Young Adult, mitochondrial disorder, medicine, Humans, Amino Acid Sequence, Preschool, Mto1, Hypertrophic Cardiomyopathy, Lactic Acidosis, Mitochondrial Disorder, Yeast, 030304 developmental biology, Infant, Newborn, Molecular, Infant, Cardiomyopathy, Hypertrophic, medicine.disease, Newborn, hypertrophic cardiomyopathy, Electron Transport Chain Complex Proteins, Hypertrophic, Carrier Proteins, Sequence Alignment, 030217 neurology & neurosurgery, Hypertrophic cardiomyopathy, Mitochondrial disorder

Abstract

We report three families presenting with hypertrophic cardiomyopathy, lactic acidosis, and multiple defects of mitochondrial respiratory chain activities. By direct sequencing of the candidate gene MTO1, encoding the mitochondrial-tRNA modifier 1, or whole exome sequencing analysis, we identified novel missense mutations. All MTO1 mutations were predicted to be deleterious on MTO1 function. Their pathogenic role was experimentally validated in a recombinant yeast model, by assessing oxidative growth, respiratory activity, mitochondrial protein synthesis and complex IV activity. In one case, we also demonstrated that expression of wt MTO1 could rescue the respiratory defect in mutant fibroblasts. The severity of the yeast respiratory phenotypes partly correlated with the different clinical presentations observed in MTO1 mutant patients, although the clinical outcome was highly variable in patients with the same mutation and seemed also to depend on timely start of pharmacological treatment, centered on the control of lactic acidosis by dichloroacetate. Our results indicate that MTO1 mutations are commonly associated with a presentation of hypertrophic cardiomyopathy, lactic acidosis and mitochondrial respiratory chain deficiency, and that ad hoc recombinant yeast models represent a useful system to test the pathogenic potential of uncommon variants, and provide insight into their effects on the expression of a biochemical phenotype.

Published

2013

30. Acute Infantile Liver Failure Due to Mutations in the TRMU Gene

Author

Avraham Shaag, Daphna Marom, Anne-Marie Mager-Heckel, Hanna Mandel, Reeval Segel, Marine Beinat, Orly Elpeleg, Agnès Rötig, Olga Karicheva, Ivan Tarassov, Ann Saada, Orit Pappo, Avraham Zeharia, and Noa Ofek

Subjects

medicine.medical_specialty, Mitochondrial DNA, Methyltransferase, Genotype, Biology, Mitochondrion, medicine.disease_cause, DNA, Mitochondrial, Mitochondrial Proteins, RNA, Transfer, Report, Internal medicine, Genetics, medicine, Humans, Genetics(clinical), Sulfhydryl Compounds, Genetics (clinical), tRNA Methyltransferases, Mutation, Infant, Newborn, Infant, Fibroblasts, Liver Failure, Acute, Disease gene identification, Mitochondria, TRNA Methyltransferases, Endocrinology, Liver, Protein Biosynthesis, Erratum, GTPBP3

Abstract

Acute liver failure in infancy accompanied by lactic acidemia was previously shown to result from mtDNA depletion. We report on 13 unrelated infants who presented with acute liver failure and lactic acidemia with normal mtDNA content. Four died during the acute episodes, and the survivors never had a recurrence. The longest follow-up period was 14 years. Using homozygosity mapping, we identified mutations in the TRMU gene, which encodes a mitochondria-specific tRNA-modifying enzyme, tRNA 5-methylaminomethyl-2-thiouridylate methyltransferase. Accordingly, the 2-thiouridylation levels of the mitochondrial tRNAs were markedly reduced. Given that sulfur is a TRMU substrate and its availability is limited during the neonatal period, we propose that there is a window of time whereby patients with TRMU mutations are at increased risk of developing liver failure.

Published

2010