TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies

Christopher A. Powell; Robert Kopajtich; Aaron R. D'Souza; Joanna Rorbach; Laura S. Kremer; Ralf A. Husain; Cristina Dallabona; Claudia Donnini; Charlotte L. Alston; Helen Griffin; Angela Pyle; Patrick F. Chinnery; Tim M. Strom; Thomas Meitinger; Richard J. Rodenburg; Gudrun Schottmann; Markus Schuelke; Nadine Romain; Ronald G. Haller; Ileana Ferrero; Tobias B. Haack; Robert W. Taylor; Holger Prokisch; Michal Minczuk

doi:10.1016/j.ajhg.2015.06.011

TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies

Christopher A. Powell, Robert Kopajtich, Aaron R. D'Souza, Joanna Rorbach, Laura S. Kremer, Ralf A. Husain, Cristina Dallabona, Claudia Donnini, Charlotte L. Alston, Helen Griffin, Angela Pyle, Patrick F. Chinnery, Tim M. Strom, Thomas Meitinger, Richard J. Rodenburg, Gudrun Schottmann, Markus Schuelke, Nadine Romain, Ronald G. Haller, Ileana FerreroTobias B. Haack, Robert W. Taylor, Holger Prokisch, Michal Minczuk

Medicine and Health

Research output: Contribution to journal › Article › peer-review

85 Scopus citations

Abstract

Deficiencies in respiratory-chain complexes lead to a variety of clinical phenotypes resulting from inadequate energy production by the mitochondrial oxidative phosphorylation system. Defective expression of mtDNA-encoded genes, caused by mutations in either the mitochondrial or nuclear genome, represents a rapidly growing group of human disorders. By whole-exome sequencing, we identified two unrelated individuals carrying compound heterozygous variants in TRMT5 (tRNA methyltransferase 5). TRMT5 encodes a mitochondrial protein with strong homology to members of the class I-like methyltransferase superfamily. Both affected individuals presented with lactic acidosis and evidence of multiple mitochondrial respiratory-chain-complex deficiencies in skeletal muscle, although the clinical presentation of the two affected subjects was remarkably different; one presented in childhood with failure to thrive and hypertrophic cardiomyopathy, and the other was an adult with a life-long history of exercise intolerance. Mutations in TRMT5 were associated with the hypomodification of a guanosine residue at position 37 (G37) of mitochondrial tRNA; this hypomodification was particularly prominent in skeletal muscle. Deficiency of the G37 modification was also detected in human cells subjected to TRMT5 RNAi. The pathogenicity of the detected variants was further confirmed in a heterologous yeast model and by the rescue of the molecular phenotype after re-expression of wild-type TRMT5 cDNA in cells derived from the affected individuals. Our study highlights the importance of post-transcriptional modification of mitochondrial tRNAs for faithful mitochondrial function.

Original language	English
Article number	1910
Pages (from-to)	319-328
Number of pages	10
Journal	American Journal of Human Genetics
Volume	97
Issue number	2
DOIs	https://doi.org/10.1016/j.ajhg.2015.06.011
State	Published - 6 Aug 2015

Access to Document

10.1016/j.ajhg.2015.06.011

Cite this

Powell, C. A., Kopajtich, R., D'Souza, A. R., Rorbach, J., Kremer, L. S., Husain, R. A., Dallabona, C., Donnini, C., Alston, C. L., Griffin, H., Pyle, A., Chinnery, P. F., Strom, T. M., Meitinger, T., Rodenburg, R. J., Schottmann, G., Schuelke, M., Romain, N., Haller, R. G., ... Minczuk, M. (2015). TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies. American Journal of Human Genetics, 97(2), 319-328. Article 1910. https://doi.org/10.1016/j.ajhg.2015.06.011

@article{d351640e36d1492d9c375d83ecb35c2d,

title = "TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies",

abstract = "Deficiencies in respiratory-chain complexes lead to a variety of clinical phenotypes resulting from inadequate energy production by the mitochondrial oxidative phosphorylation system. Defective expression of mtDNA-encoded genes, caused by mutations in either the mitochondrial or nuclear genome, represents a rapidly growing group of human disorders. By whole-exome sequencing, we identified two unrelated individuals carrying compound heterozygous variants in TRMT5 (tRNA methyltransferase 5). TRMT5 encodes a mitochondrial protein with strong homology to members of the class I-like methyltransferase superfamily. Both affected individuals presented with lactic acidosis and evidence of multiple mitochondrial respiratory-chain-complex deficiencies in skeletal muscle, although the clinical presentation of the two affected subjects was remarkably different; one presented in childhood with failure to thrive and hypertrophic cardiomyopathy, and the other was an adult with a life-long history of exercise intolerance. Mutations in TRMT5 were associated with the hypomodification of a guanosine residue at position 37 (G37) of mitochondrial tRNA; this hypomodification was particularly prominent in skeletal muscle. Deficiency of the G37 modification was also detected in human cells subjected to TRMT5 RNAi. The pathogenicity of the detected variants was further confirmed in a heterologous yeast model and by the rescue of the molecular phenotype after re-expression of wild-type TRMT5 cDNA in cells derived from the affected individuals. Our study highlights the importance of post-transcriptional modification of mitochondrial tRNAs for faithful mitochondrial function.",

author = "Powell, {Christopher A.} and Robert Kopajtich and D'Souza, {Aaron R.} and Joanna Rorbach and Kremer, {Laura S.} and Husain, {Ralf A.} and Cristina Dallabona and Claudia Donnini and Alston, {Charlotte L.} and Helen Griffin and Angela Pyle and Chinnery, {Patrick F.} and Strom, {Tim M.} and Thomas Meitinger and Rodenburg, {Richard J.} and Gudrun Schottmann and Markus Schuelke and Nadine Romain and Haller, {Ronald G.} and Ileana Ferrero and Haack, {Tobias B.} and Taylor, {Robert W.} and Holger Prokisch and Michal Minczuk",

note = "Publisher Copyright: {\textcopyright} 2015 The Authors.",

year = "2015",

month = aug,

day = "6",

doi = "10.1016/j.ajhg.2015.06.011",

language = "English",

volume = "97",

pages = "319--328",

journal = "American Journal of Human Genetics",

issn = "0002-9297",

publisher = "Cell Press",

number = "2",

}

Powell, CA, Kopajtich, R, D'Souza, AR, Rorbach, J, Kremer, LS, Husain, RA, Dallabona, C, Donnini, C, Alston, CL, Griffin, H, Pyle, A, Chinnery, PF, Strom, TM, Meitinger, T, Rodenburg, RJ, Schottmann, G, Schuelke, M, Romain, N, Haller, RG, Ferrero, I, Haack, TB, Taylor, RW, Prokisch, H & Minczuk, M 2015, 'TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies', American Journal of Human Genetics, vol. 97, no. 2, 1910, pp. 319-328. https://doi.org/10.1016/j.ajhg.2015.06.011

TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies. / Powell, Christopher A.; Kopajtich, Robert; D'Souza, Aaron R. et al.
In: American Journal of Human Genetics, Vol. 97, No. 2, 1910, 06.08.2015, p. 319-328.

Research output: Contribution to journal › Article › peer-review

TY - JOUR

T1 - TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies

AU - Powell, Christopher A.

AU - Kopajtich, Robert

AU - D'Souza, Aaron R.

AU - Rorbach, Joanna

AU - Kremer, Laura S.

AU - Husain, Ralf A.

AU - Dallabona, Cristina

AU - Donnini, Claudia

AU - Alston, Charlotte L.

AU - Griffin, Helen

AU - Pyle, Angela

AU - Chinnery, Patrick F.

AU - Strom, Tim M.

AU - Meitinger, Thomas

AU - Rodenburg, Richard J.

AU - Schottmann, Gudrun

AU - Schuelke, Markus

AU - Romain, Nadine

AU - Haller, Ronald G.

AU - Ferrero, Ileana

AU - Haack, Tobias B.

AU - Taylor, Robert W.

AU - Prokisch, Holger

AU - Minczuk, Michal

PY - 2015/8/6

Y1 - 2015/8/6

N2 - Deficiencies in respiratory-chain complexes lead to a variety of clinical phenotypes resulting from inadequate energy production by the mitochondrial oxidative phosphorylation system. Defective expression of mtDNA-encoded genes, caused by mutations in either the mitochondrial or nuclear genome, represents a rapidly growing group of human disorders. By whole-exome sequencing, we identified two unrelated individuals carrying compound heterozygous variants in TRMT5 (tRNA methyltransferase 5). TRMT5 encodes a mitochondrial protein with strong homology to members of the class I-like methyltransferase superfamily. Both affected individuals presented with lactic acidosis and evidence of multiple mitochondrial respiratory-chain-complex deficiencies in skeletal muscle, although the clinical presentation of the two affected subjects was remarkably different; one presented in childhood with failure to thrive and hypertrophic cardiomyopathy, and the other was an adult with a life-long history of exercise intolerance. Mutations in TRMT5 were associated with the hypomodification of a guanosine residue at position 37 (G37) of mitochondrial tRNA; this hypomodification was particularly prominent in skeletal muscle. Deficiency of the G37 modification was also detected in human cells subjected to TRMT5 RNAi. The pathogenicity of the detected variants was further confirmed in a heterologous yeast model and by the rescue of the molecular phenotype after re-expression of wild-type TRMT5 cDNA in cells derived from the affected individuals. Our study highlights the importance of post-transcriptional modification of mitochondrial tRNAs for faithful mitochondrial function.

AB - Deficiencies in respiratory-chain complexes lead to a variety of clinical phenotypes resulting from inadequate energy production by the mitochondrial oxidative phosphorylation system. Defective expression of mtDNA-encoded genes, caused by mutations in either the mitochondrial or nuclear genome, represents a rapidly growing group of human disorders. By whole-exome sequencing, we identified two unrelated individuals carrying compound heterozygous variants in TRMT5 (tRNA methyltransferase 5). TRMT5 encodes a mitochondrial protein with strong homology to members of the class I-like methyltransferase superfamily. Both affected individuals presented with lactic acidosis and evidence of multiple mitochondrial respiratory-chain-complex deficiencies in skeletal muscle, although the clinical presentation of the two affected subjects was remarkably different; one presented in childhood with failure to thrive and hypertrophic cardiomyopathy, and the other was an adult with a life-long history of exercise intolerance. Mutations in TRMT5 were associated with the hypomodification of a guanosine residue at position 37 (G37) of mitochondrial tRNA; this hypomodification was particularly prominent in skeletal muscle. Deficiency of the G37 modification was also detected in human cells subjected to TRMT5 RNAi. The pathogenicity of the detected variants was further confirmed in a heterologous yeast model and by the rescue of the molecular phenotype after re-expression of wild-type TRMT5 cDNA in cells derived from the affected individuals. Our study highlights the importance of post-transcriptional modification of mitochondrial tRNAs for faithful mitochondrial function.

UR - http://www.scopus.com/inward/record.url?scp=84939001025&partnerID=8YFLogxK

U2 - 10.1016/j.ajhg.2015.06.011

DO - 10.1016/j.ajhg.2015.06.011

M3 - Article

C2 - 26189817

AN - SCOPUS:84939001025

SN - 0002-9297

VL - 97

SP - 319

EP - 328

JO - American Journal of Human Genetics

JF - American Journal of Human Genetics

IS - 2

M1 - 1910

ER -

TRMT5 Mutations Cause a Defect in Post-transcriptional Modification of Mitochondrial tRNA Associated with Multiple Respiratory-Chain Deficiencies

Abstract

Access to Document

Other files and links

Fingerprint

Cite this