Subcellular origin of mitochondrial DNA deletions in human skeletal muscle

Amy E. Vincent; Hannah S. Rosa; Kamil Pabis; Conor Lawless; Chun Chen; Anne Grünewald; Karolina A. Rygiel; Mariana C. Rocha; Amy K. Reeve; Gavin Falkous; Valentina Perissi; Kathryn White; Tracey Davey; Basil J. Petrof; Avan A. Sayer; Cyrus Cooper; David Deehan; Robert W. Taylor; Doug M. Turnbull; Martin Picard

doi:10.1002/ana.25288

Subcellular origin of mitochondrial DNA deletions in human skeletal muscle

Amy E. Vincent, Hannah S. Rosa, Kamil Pabis, Conor Lawless, Chun Chen, Anne Grünewald, Karolina A. Rygiel, Mariana C. Rocha, Amy K. Reeve, Gavin Falkous, Valentina Perissi, Kathryn White, Tracey Davey, Basil J. Petrof, Avan A. Sayer, Cyrus Cooper, David Deehan, Robert W. Taylor, Doug M. Turnbull^*, Martin Picard

^*Korrespondierende/r Autor/-in für diese Arbeit

Klinik für Neurologie

44 Zitate (Scopus)

Abstract

Objective: In patients with mitochondrial DNA (mtDNA) maintenance disorders and with aging, mtDNA deletions sporadically form and clonally expand within individual muscle fibers, causing respiratory chain deficiency. This study aimed to identify the sub-cellular origin and potential mechanisms underlying this process. Methods: Serial skeletal muscle cryosections from patients with multiple mtDNA deletions were subjected to subcellular immunofluorescent, histochemical, and genetic analysis. Results: We report respiratory chain–deficient perinuclear foci containing mtDNA deletions, which show local elevations of both mitochondrial mass and mtDNA copy number. These subcellular foci of respiratory chain deficiency are associated with a local increase in mitochondrial biogenesis and unfolded protein response signaling pathways. We also find that the commonly reported segmental pattern of mitochondrial deficiency is consistent with the three-dimensional organization of the human skeletal muscle mitochondrial network. Interpretation: We propose that mtDNA deletions first exceed the biochemical threshold causing biochemical deficiency in focal regions adjacent to the myonuclei, and induce mitochondrial biogenesis before spreading across the muscle fiber. These subcellular resolution data provide new insights into the possible origin of mitochondrial respiratory chain deficiency in mitochondrial myopathy. Ann Neurol 2018;84:289–301.

Originalsprache	Englisch
Zeitschrift	Annals of Neurology
Jahrgang	84
Ausgabenummer	2
Seiten (von - bis)	289-301
Seitenumfang	13
ISSN	0364-5134
DOIs	https://doi.org/10.1002/ana.25288
Publikationsstatus	Veröffentlicht - 08.2018

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This work was supported by the Wellcome Centre for Mitochondrial Research (203105/Z/16/Z), the Medical Research Council (MRC) Centre for Translational Research in Neuromuscular Disease Mitochondrial Disease Patient Cohort G0800674, the UK National Institute for Health Research Biomedical Research Centre in Age and Age Related Diseases award to the Newcastle upon Tyne Hospitals National Health Service (NHS) Foundation Trust, the MRC/Engineering and Physical Sciences Research Council Molecular Pathology Node, the Lily Foundation, and the UK NHS Specialist Commissioners “Rare Mitochondrial Disorders of Adults and Children” Service. A.E.V. was funded by an MRC studentship (MR/K501074/1) as part of the MRC Centre for Neuromuscular Disease (MR/K000608/1) and is now funded by the MRC as part of the Centre for Ageing and Vitality (MR/L016354/1). A.G. is the recipient of an ATTRACT career development grant from the National Research Fund of Luxembourg. H.S.R. was supported by the Bar-bour Foundation. M.P. is supported by the Wharton Fund and NIH grant R35GM119793. A.K.R. is supported by a senior Parkinson’s UK fellowship (F-1401).

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Forschungsschwerpunkt: Gehirn, Hormone, Verhalten - Center for Brain, Behavior and Metabolism (CBBM)

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10.1002/ana.25288

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Vincent, A. E., Rosa, H. S., Pabis, K., Lawless, C., Chen, C., Grünewald, A., Rygiel, K. A., Rocha, M. C., Reeve, A. K., Falkous, G., Perissi, V., White, K., Davey, T., Petrof, B. J., Sayer, A. A., Cooper, C., Deehan, D., Taylor, R. W., Turnbull, D. M., & Picard, M. (2018). Subcellular origin of mitochondrial DNA deletions in human skeletal muscle. Annals of Neurology, 84(2), 289-301. https://doi.org/10.1002/ana.25288

@article{b31b9032d59b4ba7bdac65b0112c5a56,

title = "Subcellular origin of mitochondrial DNA deletions in human skeletal muscle",

abstract = "Objective: In patients with mitochondrial DNA (mtDNA) maintenance disorders and with aging, mtDNA deletions sporadically form and clonally expand within individual muscle fibers, causing respiratory chain deficiency. This study aimed to identify the sub-cellular origin and potential mechanisms underlying this process. Methods: Serial skeletal muscle cryosections from patients with multiple mtDNA deletions were subjected to subcellular immunofluorescent, histochemical, and genetic analysis. Results: We report respiratory chain–deficient perinuclear foci containing mtDNA deletions, which show local elevations of both mitochondrial mass and mtDNA copy number. These subcellular foci of respiratory chain deficiency are associated with a local increase in mitochondrial biogenesis and unfolded protein response signaling pathways. We also find that the commonly reported segmental pattern of mitochondrial deficiency is consistent with the three-dimensional organization of the human skeletal muscle mitochondrial network. Interpretation: We propose that mtDNA deletions first exceed the biochemical threshold causing biochemical deficiency in focal regions adjacent to the myonuclei, and induce mitochondrial biogenesis before spreading across the muscle fiber. These subcellular resolution data provide new insights into the possible origin of mitochondrial respiratory chain deficiency in mitochondrial myopathy. Ann Neurol 2018;84:289–301.",

author = "Vincent, \{Amy E.\} and Rosa, \{Hannah S.\} and Kamil Pabis and Conor Lawless and Chun Chen and Anne Gr{\"u}newald and Rygiel, \{Karolina A.\} and Rocha, \{Mariana C.\} and Reeve, \{Amy K.\} and Gavin Falkous and Valentina Perissi and Kathryn White and Tracey Davey and Petrof, \{Basil J.\} and Sayer, \{Avan A.\} and Cyrus Cooper and David Deehan and Taylor, \{Robert W.\} and Turnbull, \{Doug M.\} and Martin Picard",

year = "2018",

month = aug,

doi = "10.1002/ana.25288",

language = "English",

volume = "84",

pages = "289--301",

journal = "Annals of Neurology",

issn = "0364-5134",

publisher = "John Wiley \& Sons Inc.",

number = "2",

}

Vincent, AE, Rosa, HS, Pabis, K, Lawless, C, Chen, C, Grünewald, A, Rygiel, KA, Rocha, MC, Reeve, AK, Falkous, G, Perissi, V, White, K, Davey, T, Petrof, BJ, Sayer, AA, Cooper, C, Deehan, D, Taylor, RW, Turnbull, DM & Picard, M 2018, 'Subcellular origin of mitochondrial DNA deletions in human skeletal muscle', Annals of Neurology, Jg. 84, Nr. 2, S. 289-301. https://doi.org/10.1002/ana.25288

TY - JOUR

T1 - Subcellular origin of mitochondrial DNA deletions in human skeletal muscle

AU - Vincent, Amy E.

AU - Rosa, Hannah S.

AU - Pabis, Kamil

AU - Lawless, Conor

AU - Chen, Chun

AU - Grünewald, Anne

AU - Rygiel, Karolina A.

AU - Rocha, Mariana C.

AU - Reeve, Amy K.

AU - Falkous, Gavin

AU - Perissi, Valentina

AU - White, Kathryn

AU - Davey, Tracey

AU - Petrof, Basil J.

AU - Sayer, Avan A.

AU - Cooper, Cyrus

AU - Deehan, David

AU - Taylor, Robert W.

AU - Turnbull, Doug M.

AU - Picard, Martin

PY - 2018/8

Y1 - 2018/8

N2 - Objective: In patients with mitochondrial DNA (mtDNA) maintenance disorders and with aging, mtDNA deletions sporadically form and clonally expand within individual muscle fibers, causing respiratory chain deficiency. This study aimed to identify the sub-cellular origin and potential mechanisms underlying this process. Methods: Serial skeletal muscle cryosections from patients with multiple mtDNA deletions were subjected to subcellular immunofluorescent, histochemical, and genetic analysis. Results: We report respiratory chain–deficient perinuclear foci containing mtDNA deletions, which show local elevations of both mitochondrial mass and mtDNA copy number. These subcellular foci of respiratory chain deficiency are associated with a local increase in mitochondrial biogenesis and unfolded protein response signaling pathways. We also find that the commonly reported segmental pattern of mitochondrial deficiency is consistent with the three-dimensional organization of the human skeletal muscle mitochondrial network. Interpretation: We propose that mtDNA deletions first exceed the biochemical threshold causing biochemical deficiency in focal regions adjacent to the myonuclei, and induce mitochondrial biogenesis before spreading across the muscle fiber. These subcellular resolution data provide new insights into the possible origin of mitochondrial respiratory chain deficiency in mitochondrial myopathy. Ann Neurol 2018;84:289–301.

AB - Objective: In patients with mitochondrial DNA (mtDNA) maintenance disorders and with aging, mtDNA deletions sporadically form and clonally expand within individual muscle fibers, causing respiratory chain deficiency. This study aimed to identify the sub-cellular origin and potential mechanisms underlying this process. Methods: Serial skeletal muscle cryosections from patients with multiple mtDNA deletions were subjected to subcellular immunofluorescent, histochemical, and genetic analysis. Results: We report respiratory chain–deficient perinuclear foci containing mtDNA deletions, which show local elevations of both mitochondrial mass and mtDNA copy number. These subcellular foci of respiratory chain deficiency are associated with a local increase in mitochondrial biogenesis and unfolded protein response signaling pathways. We also find that the commonly reported segmental pattern of mitochondrial deficiency is consistent with the three-dimensional organization of the human skeletal muscle mitochondrial network. Interpretation: We propose that mtDNA deletions first exceed the biochemical threshold causing biochemical deficiency in focal regions adjacent to the myonuclei, and induce mitochondrial biogenesis before spreading across the muscle fiber. These subcellular resolution data provide new insights into the possible origin of mitochondrial respiratory chain deficiency in mitochondrial myopathy. Ann Neurol 2018;84:289–301.

UR - https://www.scopus.com/pages/publications/85052390354

U2 - 10.1002/ana.25288

DO - 10.1002/ana.25288

M3 - Journal articles

C2 - 30014514

AN - SCOPUS:85052390354

SN - 0364-5134

VL - 84

SP - 289

EP - 301

JO - Annals of Neurology

JF - Annals of Neurology

IS - 2

ER -

Subcellular origin of mitochondrial DNA deletions in human skeletal muscle

Abstract

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