Your search keyword '"genetics [DNA, Mitochondrial]"' showing total 22 results

1. Mitochondrial haplogroups and cognitive progression in Parkinson's disease

Author

Liu, Ganqiang, Ni, Chunming, Zhan, Jiamin, Li, Weimin, Luo, Junfeng, Liao, Zhixiang, Locascio, Joseph J, Xian, Wenbiao, Chen, Ling, Pei, Zhong, Corvol, Jean-Christophe, Maple-Grødem, Jodi, Campbell, Meghan C, Elbaz, Alexis, Lesage, Suzanne, Brice, Alexis, Hung, Albert Y, Schwarzschild, Michael A, Hayes, Michael T, Wills, Anne-Marie, Ravina, Bernard, Shoulson, Ira, Taba, Pille, Kõks, Sulev, Beach, Thomas G, Cormier-Dequaire, Florence, Alves, Guido, Tysnes, Ole-Bjørn, Perlmutter, Joel S, Heutink, Peter, Van Hilten, Jacobus J, Barker, Roger A, Williams-Gray, Caroline H, Scherzer, Clemens R, International Genetics Of Parkinson Disease Progression (IGPP) Consortium, Liu, Ganqiang [0000-0002-1921-9542], Pei, Zhong [0000-0002-8425-2867], Elbaz, Alexis [0000-0001-9724-5490], Apollo - University of Cambridge Repository, Liu, Ganqiang, Valentino, Rebecca R, Peng, Jiajie, Liao, Zhixiang, Locascio, Joseph J, Corvol, Jean-Christophe, Dong, Xianjun, Maple-Grødem, Jodi, Campbell, Meghan C, Elbaz, Alexis, Lesage, Suzanne, Brice, Alexis, Mangone, Graziella, Growdon, John H, Hung, Albert Y, Schwarzchild, Michael A, Hayes, Michael T, Wills, Anne-Marie, Herrington, Todd M, Ravian, Bernard, Shoulson, Ira, Taba, Pille, Kõks, Sulev, Beach, Thomas G, Cormier-Dequaire, Florence, Alves, Guido, Tysnes, Ole-Bjørn, Perlmutter, Joel S, Heutink, Peter, van Hilten, Jacobus J, Kasten, Meike, Mollenhauer, Brit, Trenkwalder, Claudia, Klein, Christine, Barker, Roger A, Williams-Gray, Caroline H, Marinus, Johan, and Scherzer, Clemens R

Subjects

mitochondrial haplogroups, Parkinson's disease, cognitive progression, Parkinson Disease, genetics [DNA, Mitochondrial], DNA, Mitochondrial, Mitochondria, Cognition, Haplotypes, genetics [Parkinson Disease], Report, Parkinson’s disease, Disease Progression, Humans, Neurology (clinical), ddc:610, epidemiology [Parkinson Disease], genetics [Mitochondria]

Abstract

Liu et al. report that specific mitochondrial haplogroups are associated with the progression of cognitive decline in patients with Parkinson's disease, but not with the progression of motor impairment. Mitochondrial haplotypes may thus be useful for stratifying patients according to their risk of cognitive decline.Mitochondria are a culprit in the onset of Parkinson's disease, but their role during disease progression is unclear. Here we used Cox proportional hazards models to exam the effect of variation in the mitochondrial genome on longitudinal cognitive and motor progression over time in 4064 patients with Parkinson's disease. Mitochondrial macro-haplogroup was associated with reduced risk of cognitive disease progression in the discovery and replication population. In the combined analysis, patients with the super macro-haplogroup J, T, U-# had a 41% lower risk of cognitive progression with P = 2.42 x 10(-6) compared to those with macro-haplogroup H. Exploratory analysis indicated that the common mitochondrial DNA variant, m.2706A>G, was associated with slower cognitive decline with a hazard ratio of 0.68 (95% confidence interval 0.56-0.81) and P = 2.46 x 10(-5). Mitochondrial haplogroups were not appreciably linked to motor progression. This initial genetic survival study of the mitochondrial genome suggests that mitochondrial haplogroups may be associated with the pace of cognitive progression in Parkinson's disease over time.

Published

2023

2. Mitochondrial damage activates the NLRP10 inflammasome

Author

Tomasz Próchnicki, Matilde B. Vasconcelos, Kim S. Robinson, Matthew S. J. Mangan, Dennis De Graaf, Kateryna Shkarina, Marta Lovotti, Lena Standke, Romina Kaiser, Rainer Stahl, Fraser G. Duthie, Maximilian Rothe, Kateryna Antonova, Lea-Marie Jenster, Zhi Heng Lau, Sarah Rösing, Nora Mirza, Clarissa Gottschild, Dagmar Wachten, Claudia Günther, Thomas A. Kufer, Florian I. Schmidt, Franklin L. Zhong, and Eicke Latz

Subjects

genetics [NLR Family, Pyrin Domain-Containing 3 Protein], NLRP10 protein, human, metabolism [Apoptosis Regulatory Proteins], Cell Death, Inflammasomes, metabolism [NLR Family, Pyrin Domain-Containing 3 Protein], Immunology, metabolism [Caspase 1], Caspase 1, Interleukin-1beta, metabolism [Cytokines], genetics [DNA, Mitochondrial], DNA, Mitochondrial, metabolism [Adaptor Proteins, Signal Transducing], metabolism [Interleukin-1beta], NLR Family, Pyrin Domain-Containing 3 Protein, Immunology and Allergy, Humans, Cytokines, ddc:610, Apoptosis Regulatory Proteins, metabolism [Inflammasomes], Adaptor Proteins, Signal Transducing

Abstract

Upon detecting pathogens or cell stress, several NOD-like receptors (NLRs) form inflammasome complexes with the adapter ASC and caspase-1, inducing gasdermin D (GSDMD)-dependent cell death and maturation and release of IL-1β and IL-18. The triggers and activation mechanisms of several inflammasome-forming sensors are not well understood. Here we show that mitochondrial damage activates the NLRP10 inflammasome, leading to ASC speck formation and caspase-1-dependent cytokine release. While the AIM2 inflammasome can also sense mitochondrial demise by detecting mitochondrial DNA (mtDNA) in the cytosol, NLRP10 monitors mitochondrial integrity in an mtDNA-independent manner, suggesting the recognition of distinct molecular entities displayed by the damaged organelles. NLRP10 is highly expressed in differentiated human keratinocytes, in which it can also assemble an inflammasome. Our study shows that this inflammasome surveils mitochondrial integrity. These findings might also lead to a better understanding of mitochondria-linked inflammatory diseases.

Published

2023

3. Mitochondrial disease in adults: recent advances and future promise

Author

Robert McFarland, Cornelia Kornblum, David R. Thorburn, Anu Suomalainen, Laurence A. Bindoff, Michelangelo Mancuso, Grainne S. Gorman, Thomas Klopstock, Y.S. Ng, Robert W. Taylor, Douglass M. Turnbull, and Carolyn M. Sue

Subjects

0301 basic medicine, methods [High-Throughput Nucleotide Sequencing], Mitochondrial Diseases, genetics [Mitochondrial Diseases], Mitochondrial disease, Symptomatic treatment, therapy [Mitochondrial Diseases], genetics [Mutation], Reproductive technology, Bioinformatics, DNA, Mitochondrial, 03 medical and health sciences, 0302 clinical medicine, methods [Genetic Therapy], physiopathology [Mitochondrial Diseases], medicine, Humans, ddc:610, trends [Genetic Therapy], Repurposing, Transmission (medicine), business.industry, High-Throughput Nucleotide Sequencing, Genetic Therapy, medicine.disease, genetics [DNA, Mitochondrial], 3. Good health, Natural history, 030104 developmental biology, Current management, Mutation, Neurology (clinical), business, 030217 neurology & neurosurgery

Abstract

Mitochondrial diseases are some of the most common inherited neurometabolic disorders, and major progress has been made in our understanding, diagnosis, and treatment of these conditions in the past 5 years. Development of national mitochondrial disease cohorts and international collaborations has changed our knowledge of the spectrum of clinical phenotypes and natural history of mitochondrial diseases. Advances in high-throughput sequencing technologies have altered the diagnostic algorithm for mitochondrial diseases by increasingly using a genetics-first approach, with more than 350 disease-causing genes identified to date. While the current management strategy for mitochondrial disease focuses on surveillance for multisystem involvement and effective symptomatic treatment, new endeavours are underway to find better treatments, including repurposing current drugs, use of novel small molecules, and gene therapies. Developments made in reproductive technology offer women the opportunity to prevent transmission of DNA-related mitochondrial disease to their children.

Published

2021

4. Cross-Sectional Analysis of Baseline Visual Parameters in Subjects Recruited Into the RESCUE and REVERSE ND4-LHON Gene Therapy Studies

Author

Moster, Mark L, Sergott, Robert C, Sadun, Alfredo A, DeBusk, Adam A, Carbonelli, Michele, Hage, Rabih, Priglinger, Siegfried, Karanjia, Rustum, Blouin, Laure, Taiel, Magali, Katz, Barrett, Sahel, José Alain, Newman, Nancy J, group, LHON study, Yu-Wai-Man, Patrick, Carelli, Valerio, Bryan, Molly Scannell, Smits, Gerard, Biousse, Valérie, Vignal-Clermont, Catherine, Klopstock, Thomas, Moster M.L., Sergott R.C., Newman N.J., Yu-Wai-Man P., Carelli V., Bryan M.S., Smits G., Biousse V., Vignal-Clermont C., Klopstock T., Sadun A.A., DeBusk A.A., Carbonelli M., Hage R., Priglinger S., Karanjia R., Blouin L., Taiel M., Katz B., and Sahel J.A.

Subjects

Male, Retinal Ganglion Cells, methods [Tomography, Optical Coherence], Visual acuity, genetic structures, Cross-sectional study, physiology [Visual Fields], Genetic enhancement, Nerve fiber layer, Visual Acuity, Phases of clinical research, Retinal Ganglion Cell, chemistry.chemical_compound, Medicine, Contrast (vision), media_common, physiopathology [Optic Atrophy, Hereditary, Leber], Middle Aged, genetics [DNA, Mitochondrial], medicine.anatomical_structure, Clinical Research: Epidemiology Meets Neuro-Ophthalmology, Female, medicine.symptom, Tomography, Optical Coherence, Human, Adult, LEBER HEREDITARY OPTIC NEUROPATHY, medicine.medical_specialty, Adolescent, media_common.quotation_subject, Visual Field, Optic Atrophy, Hereditary, Leber, therapy [Optic Atrophy, Hereditary, Leber], pathology [Retinal Ganglion Cells], DNA, Mitochondrial, Young Adult, methods [Genetic Therapy], Double-Blind Method, Ophthalmology, Humans, ddc:610, Aged, Cross-Sectional Studie, business.industry, Retinal, Genetic Therapy, eye diseases, Cross-Sectional Studies, chemistry, genetics [Optic Atrophy, Hereditary, Leber], Neurology (clinical), Visual Fields, business

Abstract

OBJECTIVE: This report presents a cross-sectional analysis of the baseline characteristics of subjects with Leber hereditary optic neuropathy enrolled in the gene therapy trials RESCUE and REVERSE, to illustrate the evolution of visual parameters over the first year after vision loss. METHODS: RESCUE and REVERSE were 2 phase III clinical trials designed to assess the efficacy of rAAV2/2-ND4 gene therapy in ND4-LHON subjects. At enrollment, subjects had vision loss for ≤6 months in RESCUE, and between 6 and 12 months in REVERSE. Functional visual parameters (best-corrected visual acuity [BCVA], contrast sensitivity [CS], and Humphrey Visual Field [HVF]) and structural parameters assessed by spectral-domain optical coherence tomography were analyzed in both cohorts before treatment. The cross-sectional analysis of functional and anatomic parameters included the baseline values collected in all eyes at 2 different visits (Screening and Inclusion). RESULTS: Seventy-six subjects were included in total, 39 in RESCUE and 37 in REVERSE. Mean BCVA was significantly worse in RESCUE subjects compared with REVERSE subjects (1.29 and 1.61 LogMAR respectively, P = 0.0029). Similarly, mean CS and HVF were significantly more impaired in REVERSE vs RESCUE subjects (P < 0.005). The cross-sectional analysis showed that the monthly decrease in BCVA, ganglion cell layer macular volume, and retinal nerve fiber layer thickness was much more pronounced in the first 6 months after onset (+0.24 LogMAR, -0.06 mm3, and -6.00 μm respectively) than between 6 and 12 months after onset (+0.02 LogMAR, -0.01 mm3, and -0.43 μm respectively). CONCLUSION: LHON progresses rapidly in the first months following onset during the subacute phase, followed by relative stabilization during the dynamic phase.

Published

2021

5. Long-Term Follow-Up After Unilateral Intravitreal Gene Therapy for Leber Hereditary Optic Neuropathy: The RESTORE Study

Author

Biousse, Valérie, Newman, Nancy J, Esposti, Simona, La Morgia, Chiara, Priglinger, Claudia, Karanja, Rustum, Blouin, Laure, Taiel, Magali, Sahel, José-Alain, Group, LHON Study, Yu-Wai-Man, Patrick, Carelli, Valerio, Moster, Mark L, Vignal-Clermont, Catherine, Klopstock, Thomas, Sadun, Alfredo A, Sergott, Robert C, Hage, Rabih, Biousse V., Newman N.J., Yu-Wai-Man P., Carelli V., Moster M.L., Vignal-Clermont C., Klopstock T., Sadun A.A., Sergott R.C., Hage R., Esposti S., La Morgia C., Priglinger C., Karanja R., Blouin L., Taiel M., Sahel J.-A., Emory University School of Medicine, Emory University [Atlanta, GA], University College of London [London] (UCL), Istituti di Ricovero e Cura a Carattere Scientifico (IRCCS), Jefferson (Philadelphia University + Thomas Jefferson University), Centre Hospitalier National d'Ophtalmologie des Quinze-Vingts (CHNO), Ludwig-Maximilians-Universität München (LMU), University of California [Los Angeles] (UCLA), University of California, National Institute for Health Research Moorfields Biomedical Research Centre at Moorfields Eye Hospital and UCL Institute of Ophthalmology, London, GenSight Biologics, Institut de la Vision, and Centre National de la Recherche Scientifique (CNRS)-Sorbonne Université (SU)-Institut National de la Santé et de la Recherche Médicale (INSERM)

Subjects

Male, Visual acuity, Time Factors, genetic structures, Genetic enhancement, Visual Acuity, NADH dehydrogenase subunit 4, 0302 clinical medicine, Quality of life, education.field_of_study, metabolism [NADH Dehydrogenase], physiopathology [Optic Atrophy, Hereditary, Leber], Original Contribution, Recombinant Protein, Middle Aged, genetics [DNA, Mitochondrial], Recombinant Proteins, Intravitreal Injections, ComputingMethodologies_DOCUMENTANDTEXTPROCESSING, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Female, medicine.symptom, Tomography, Optical Coherence, Human, Adult, medicine.medical_specialty, LEBER HEREDITARY OPTIC NEUROPATHY, Composite score, Time Factor, Adolescent, Long term follow up, Population, Optic Atrophy, Hereditary, Leber, therapy [Optic Atrophy, Hereditary, Leber], DNA, Mitochondrial, Follow-Up Studie, 03 medical and health sciences, Young Adult, methods [Genetic Therapy], Double-Blind Method, Ophthalmology, administration & dosage [Recombinant Proteins], medicine, Humans, ddc:610, [SDV.MHEP.OS]Life Sciences [q-bio]/Human health and pathology/Sensory Organs, education, Aged, business.industry, Intravitreal Injection, NADH Dehydrogenase, Genetic Therapy, eye diseases, Clinical trial, genetics [Optic Atrophy, Hereditary, Leber], Mutation, 030221 ophthalmology & optometry, Quality of Life, Neurology (clinical), Visual Fields, genetics [NADH Dehydrogenase], business, 030217 neurology & neurosurgery, Follow-Up Studies

Abstract

Supplemental Digital Content is Available in the Text., Background: RESCUE and REVERSE were 2 Phase 3 clinical trials that assessed the efficacy and safety of intravitreal gene therapy with lenadogene nolparvovec (rAAV2/2-ND4) for the treatment of Leber hereditary optic neuropathy (LHON). RESTORE is the long-term follow-up study of subjects treated in the RESCUE and REVERSE trials. Methods: In RESCUE and REVERSE, 76 subjects with LHON because of the m.11778 G>A mutation in the mitochondrial gene ND4 received a single unilateral intravitreal injection of lenadogene nolparvovec. After 96 weeks, 61 subjects were enrolled in the long-term follow-up study RESTORE. The best-corrected visual acuity (BCVA) was assessed over a period of up to 52 months after onset of vision loss. A locally estimated scatterplot smoothing regression model was used to analyze changes in BCVA over time. Vision-related quality of life was reported using the visual function questionnaire-25 (VFQ-25). Results: The population of MT-ND4 subjects enrolled in RESTORE was representative of the combined cohorts of RESCUE and REVERSE for mean age (35.1 years) and gender distribution (79% males). There was a progressive and sustained improvement of BCVA up to 52 months after the onset of vision loss. The final mean BCVA was 1.26 logarithm of the minimal angle of resolution 48 months after the onset of vision loss. The mean VFQ-25 composite score increased by 7 points compared with baseline. Conclusion: The treatment effect of lenadogene nolparvovec on BCVA and vision-related quality of life observed 96 weeks (2 years) after treatment in RESCUE and REVERSE was sustained at 3 years in RESTORE, with a maximum follow-up of 52 months (4.3 years) after the onset of vision loss.

Published

2020

6. DNAJC30 defect: A frequent cause of recessive Leber hereditary optic neuropathy and Leigh syndrome

Author

Sarah L. Stenton, Marketa Tesarova, Natalia L. Sheremet, Claudia B. Catarino, Valerio Carelli, Elżbieta Ciara, Kathryn Curry, Martin Engvall, Leah R. Fleming, Peter Freisinger, Katarzyna Iwanicka-Pronicka, Elżbieta Jurkiewicz, Thomas Klopstock, Mary K. Koenig, Hana Kolářová, Bohdan Kousal, Tatiana Krylova, Chiara La Morgia, Lenka Nosková, Dorota Piekutowska-Abramczuk, Sam N. Russo, Viktor Stránecký, Iveta Tóthová, Frank Träisk, and Holger Prokisch

Subjects

Adult, Male, genetic structures, genetics [Mutation], Optic Atrophy, Hereditary, Leber, Dnajc30, Lhon, Leigh Syndrome, Mitochondrial Disease, genetics [DNA, Mitochondrial], Leigh syndrome, DNA, Mitochondrial, DNAJC30, eye diseases, LHON, mitochondrial disease, genetics [Optic Atrophy, Hereditary, Leber], Optic Atrophies, Hereditary, Mutation, genetics [Leigh Disease], Humans, Female, ddc:610, Neurology (clinical), Leigh Disease, Child

Abstract

The recent description of biallelic DNAJC30 variants in Leber hereditary optic neuropathy (LHON) and Leigh syndrome challenged the longstanding assumption for LHON to be exclusively maternally inherited and broadened the genetic spectrum of Leigh syndrome, the most frequent paediatric mitochondrial disease. Herein, we characterize 28 so far unreported individuals from 26 families carrying a homozygous DNAJC30 p.Tyr51Cys founder variant, 24 manifesting with LHON, two manifesting with Leigh syndrome, and two remaining asymptomatic. This collection of unreported variant carriers confirms sex-dependent incomplete penetrance of the homozygous variant given a significant male predominance of disease and the report of asymptomatic homozygous variant carriers. The autosomal recessive LHON patients demonstrate an earlier age of disease onset and a higher rate of idebenone-treated and spontaneous recovery of vision in comparison to reported figures for maternally inherited disease. Moreover, the report of two additional patients with childhood- or adult-onset Leigh syndrome further evidences the association of DNAJC30 with Leigh syndrome, previously only reported in a single childhood-onset case.

Published

2022

7. Vitamin B12 in Leber hereditary optic neuropathy mutation carriers: a prospective cohort study

Author

Julia Zibold, Bettina von Livonius, Hana Kolarova, Günter Rudolph, Claudia S. Priglinger, Thomas Klopstock, and Claudia B. Catarino

Subjects

Adult, Male, Adolescent, genetics [Mutation], Optic Atrophy, Hereditary, Leber, DNA, Mitochondrial, Young Adult, LHON, Humans, Leber optic atrophy, Pharmacology (medical), ddc:610, Prospective Studies, Child, Genetics (clinical), Hereditary optic atrophy, Aged, Aged, 80 and over, genetics [Vitamin B 12 Deficiency], Vitamin B12, epidemiology [Optic Atrophy, Hereditary, Leber], epidemiology [Vitamin B 12 Deficiency], Vitamin B 12 Deficiency, General Medicine, Middle Aged, genetics [DNA, Mitochondrial], Cobalamin, Mitochondrial disease, Vitamin B 12, genetics [Optic Atrophy, Hereditary, Leber], Child, Preschool, Mutation, Female

Abstract

Background Leber hereditary optic neuropathy (LHON) is the most common mitochondrial disorder, frequently resulting in acute or subacute severe bilateral central vision loss. Vitamin B12 deficiency is also a known cause of optic neuropathy through mitochondrial dysfunction. Here we evaluated the prevalence and clinical significance of vitamin B12 deficiency in a large cohort of LHON patients and asymptomatic mutation carriers from a tertiary referral center. Methods From the Munich LHON prospective cohort study, participants included all LHON patients and asymptomatic LHON mutation carriers, who were recruited between February 2014 and March 2020 and consented to participate. Neurological, general, and ophthalmological examinations were regularly performed, as were laboratory tests. Vitamin B12 deficiency was diagnosed if serum vitamin B12 was below 201 pg/mL, or if 201–339 pg/mL plus low serum holotranscobalamin or elevated serum methylmalonic acid or elevated total plasma homocysteine. Results We analyzed 244 subjects, including 147 symptomatic LHON patients (74% males) and 97 asymptomatic mutation carriers (31% males). Median age at study baseline was 34 years (range 5–82 years). The prevalence of vitamin B12 deficiency was higher for LHON mutation carriers than for the general population in all age categories. This was statistically significant for the LHON mutation carriers under 65 years (21% vs. 5–7%, p = 0.002). While vitamin B12 deficiency prevalence was not statistically different between LHON patients and asymptomatic mutation carriers, its clinical correlates, e.g., macrocytosis and polyneuropathy, were more frequent in the subgroup of LHON patients. Excessive alcohol consumption was a significant predictor of vitamin B12 deficiency (p Conclusions The high prevalence of vitamin B12 deficiency in LHON mutation carriers, both asymptomatic mutation carriers and LHON patients, highlights the need for regular vitamin B12 screening in this population, in order to ensure early treatment, aiming for better outcomes. Our study is not conclusive regarding vitamin B12 deficiency as determinant for disease conversion in LHON, and further research is warranted to disentangle the role of vitamin B12 in the pathophysiology and prognosis of LHON.

Published

2022

8. Multi-Omics Approach to Mitochondrial DNA Damage in Human Muscle Fibers

Author

Konrad Olszewski, Thomas Klopstock, Matthias Elstner, Holger Prokisch, Marta Murgia, University of Zurich, and Murgia, Marta

Subjects

Male, Ophthalmoplegia, Chronic Progressive External, skeletal muscle, mtDNA deletions, transcriptomics, proteomics, myopathy, disease models, Muscle Fibers, Skeletal, Respiratory chain, 1607 Spectroscopy, Proteomics, Transcriptome, genetics [Ophthalmoplegia, Chronic Progressive External], Gene Regulatory Networks, Biology (General), Spectroscopy, Laser capture microdissection, General Medicine, genetics [DNA, Mitochondrial], Computer Science Applications, Cell biology, ddc, Succinate Dehydrogenase, Chemistry, Proteome, ddc:540, Female, 1606 Physical and Theoretical Chemistry, Mitochondrial DNA, genetics [Mitochondria, Muscle], 1503 Catalysis, QH301-705.5, pathology [Mitochondria, Muscle], 610 Medicine & health, Laser Capture Microdissection, Biology, genetics [NADPH Dehydrogenase], DNA, Mitochondrial, Catalysis, Article, Inorganic Chemistry, Electron Transport Complex IV, metabolism [Succinate Dehydrogenase], medicine, 1312 Molecular Biology, 1706 Computer Science Applications, Humans, Physical and Theoretical Chemistry, Molecular Biology, QD1-999, metabolism [NADPH Dehydrogenase], 1604 Inorganic Chemistry, metabolism [Electron Transport Complex IV], Gene Expression Profiling, Organic Chemistry, NADPH Dehydrogenase, pathology [Ophthalmoplegia, Chronic Progressive External], medicine.disease, Mitochondria, Muscle, Disease Models, Mtdna Deletions, Myopathy, Skeletal Muscle, Transcriptomics, 10054 Clinic for Psychiatry, Psychotherapy, and Psychosomatics, Translational elongation, pathology [Muscle Fibers, Skeletal], methods [Proteomics], Chronic progressive external ophthalmoplegia, 1605 Organic Chemistry

Abstract

Mitochondrial DNA deletions affect energy metabolism at tissue-specific and cell-specific threshold levels, but the pathophysiological mechanisms determining cell fate remain poorly understood. Chronic progressive external ophthalmoplegia (CPEO) is caused by mtDNA deletions and characterized by a mosaic distribution of muscle fibers with defective cytochrome oxidase (COX) activity, interspersed among fibers with retained functional respiratory chain. We used diagnostic histochemistry to distinguish COX-negative from COX-positive fibers in nine muscle biopsies from CPEO patients and performed laser capture microdissection (LCM) coupled to genome-wide gene expression analysis. To gain molecular insight into the pathogenesis, we applied network and pathway analysis to highlight molecular differences of the COX-positive and COX-negative fiber transcriptome. We then integrated our results with proteomics data that we previously obtained comparing COX-positive and COX-negative fiber sections from three other patients. By virtue of the combination of LCM and a multi-omics approach, we here provide a comprehensive resource to tackle the pathogenic changes leading to progressive respiratory chain deficiency and disease in mitochondrial deletion syndromes. Our data show that COX-negative fibers upregulate transcripts involved in translational elongation and protein synthesis. Furthermore, based on functional annotation analysis, we find that mitochondrial transcripts are the most enriched among those with significantly different expression between COX-positive and COX-negative fibers, indicating that our unbiased large-scale approach resolves the core of the pathogenic changes. Further enrichments include transcripts encoding LIM domain proteins, ubiquitin ligases, proteins involved in RNA turnover, and, interestingly, cell cycle arrest and cell death. These pathways may thus have a functional association to the molecular pathogenesis of the disease. Overall, the transcriptome and proteome show a low degree of correlation in CPEO patients, suggesting a relevant contribution of post-transcriptional mechanisms in shaping this disease phenotype.

Published

2021

9. Efficacy and Safety of Intravitreal Gene Therapy for Leber Hereditary Optic Neuropathy Treated within 6 Months of Disease Onset

Author

Irena Tsui, Claudia B. Catarino, Piero Barboni, Günther Rudolph, Nancy J. Newman, Sara Silvestri, Alfredo A. Sadun, Michael Dattilo, Neringa Jurkute, Jean-François Girmens, Cosima Schertler, Magali Taiel, Rustum Karanjia, Claudia Priglinger, Maria K Gemenetzi, Armin Wolf, Manuela Contin, Jasmina Al-Tamami, Thomas Klopstock, James Acheson, Robert C. Sergott, Deborah Gibbs, Rabih Hage, Stephan R. Thurau, Adam A. DeBusk, Lidia Di Vito, Mark L. Moster, Valérie Biousse, Med Lindreth DuBois, Valerio Carelli, Gad Heilweil, Chiara La Morgia, Michele Carbonelli, Andrew Hendrick, Patrick Yu-Wai-Man, Jason H. Peragallo, Gerard Smits, Angelika Pressler, Martin Hildebrandt, Alcides Fernandes Filho, Michael Neuenhahn, Bettina von Livonius, Barrett Katz, Daniel R Muth, Siegfried G. Priglinger, Lauren Leitch-Devlin, Susan Mohamed, William R. Tucker, Maria Massini, Maria Eleftheriadou, Laure Blouin, Catherine Vignal-Clermont, Eman Hawy, Simona Degli Esposti, Heather Tollis, G. Baker Hubbard, Jannah Rutter Dobbs, José-Alain Sahel, Catherine Vignal, Melissa SantaMaria, Julie A. Haller, Emory University School of Medicine, Emory University [Atlanta, GA], Addenbrooke's Hospital, Cambridge University NHS Trust, Istituti di Ricovero e Cura a Carattere Scientifico (IRCCS), University of Bologna, Jefferson (Philadelphia University + Thomas Jefferson University), Fondation Ophtalmologique Adolphe de Rothschild [Paris], Centre Hospitalier National d'Ophtalmologie des Quinze-Vingts (CHNO), Ludwig-Maximilians-Universität München (LMU), University of California [Los Angeles] (UCLA), University of California, Ludwig Maximilian University [Munich] (LMU), Institut de la Vision, Centre National de la Recherche Scientifique (CNRS)-Sorbonne Université (SU)-Institut National de la Santé et de la Recherche Médicale (INSERM), University of Pittsburgh School of Medicine, Pennsylvania Commonwealth System of Higher Education (PCSHE), Institut Hospitalo-Universitaire FOReSIGHT, Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre Hospitalier National d'Ophtalmologie des Quinze-Vingts (CHNO)-Sorbonne Université (SU), Newman, NJ, Yu-Wai-Man, P, Carelli, V, Moster, ML, Biousse, V, Vignal-Clermont, C, Sergott, RC, Klopstock, T, Sadun, AA, Barboni, P, DeBusk, AA, Girmens, JF, Rudolph, G, Karanjia, R, Taiel, M, Blouin, L, Smits, G, Katz, B, Sahel, J-A, Vignal, C, Hage, R, Catarino, CB, Priglinger, C, Priglinger, S, Thurau, S, von Livonius, B, Muth, D, Wolf, A, Al-Tamami, J, Pressler, A, Schertler, C, Hildebrandt, M, Neuenhahn, M, Heilweil, G, Tsui, I, Hubbard, GB, Hendrick, A, Dattilo, M, Peragallo, J, Hawy, E, DuBois, Med L, Gibbs, D, Filho, AF, Dobbs, J, Carbonelli, M, Di Vito, L, Contin, M, Mohamed, S, La Morgia, C, Silvestri, S, Acheson, J, Eleftheriadou, M, Esposti, S, Gemenetzi, M, Leitch-Devlin, L, Tucker, WR, Jurkute, N, SantaMaria, M, Tollis, H, Haller, JA, and Massini, M.

Subjects

Male, Time Factors, Visual acuity, genetic structures, physiology [Visual Fields], [SDV]Life Sciences [q-bio], efficacy, Visual Acuity, Phases of clinical research, genetics [Dependovirus], chemistry.chemical_compound, 0302 clinical medicine, Visual Field Test, Quality of life, Clinical endpoint, Contrast (vision), intravitreal gene therapy, media_common, 0303 health sciences, physiology [Visual Acuity], Diabetic retinopathy, Dependovirus, Middle Aged, Dependoviru, genetics [DNA, Mitochondrial], Phase 3 randomized double-masked clinical trial, Treatment Outcome, Intravitreal Injections, diagnosis [Optic Atrophy, Hereditary, Leber], Female, Genetic Vector, medicine.symptom, Human, Adult, safety, LEBER HEREDITARY OPTIC NEUROPATHY, medicine.medical_specialty, retinal anatomic measures, Time Factor, Adolescent, media_common.quotation_subject, psychology [Optic Atrophy, Hereditary, Leber], Genetic Vectors, Visual Field, Humphrey visual field perimetry, Optic Atrophy, Hereditary, Leber, therapy [Optic Atrophy, Hereditary, Leber], DNA, Mitochondrial, bilateral visual improvement, Follow-Up Studie, Leber Hereditary Optic Neuropathy, Young Adult, 03 medical and health sciences, Double-Blind Method, Ophthalmology, psychology [Quality of Life], Electroretinography, medicine, Humans, ddc:610, Aged, 030304 developmental biology, contrast sensitivity, business.industry, Intravitreal Injection, Retinal, Genetic Therapy, retinal anatomic measure, medicine.disease, eye diseases, genetics [Optic Atrophy, Hereditary, Leber], chemistry, Mutation, 030221 ophthalmology & optometry, Visual Field Tests, sense organs, Visual Fields, business, Follow-Up Studies, best-corrected visual acuity

Abstract

International audience; Purpose: To evaluate the efficacy of a single intravitreal injection of rAAV2/2-ND4 in subjects with visual loss from Leber hereditary optic neuropathy (LHON).Design: RESCUE is a multicenter, randomized, double-masked, sham-controlled, phase 3 clinical trial.Participants: Subjects with the m.11778G>A mitochondrial DNA mutation and vision loss ≤6 months from onset in 1 or both eyes were included.Methods: Each subject's right eye was randomly assigned (1:1) to treatment with rAAV2/2-ND4 (single injection of 9 × 1010 viral genomes in 90 μl) or to sham injection. The left eye received the treatment not allocated to the right eye.Main outcome measures: The primary end point was the difference of the change from baseline in best-corrected visual acuity (BCVA) between rAAV2/2-ND4-treated and sham-treated eyes at week 48. Other outcome measures included contrast sensitivity, Humphrey visual field perimetry, retinal anatomic measures, and quality of life. Follow-up extended to week 96.Results: Efficacy analysis included 38 subjects. Mean age was 36.8 years, and 82% were male. Mean duration of vision loss at time of treatment was 3.6 months and 3.9 months in the rAAV2/2-ND4-treated eyes and sham-treated eyes, respectively. Mean baseline logarithm of the minimum angle of resolution (logMAR) BCVA (standard deviation) was 1.31 (0.52) in rAAV2/2-ND4-treated eyes and 1.26 (0.62) in sham-treated eyes, with a range from -0.20 to 2.51. At week 48, the difference of the change in BCVA from baseline between rAAV2/2-ND4-treated and sham-treated eyes was -0.01 logMAR (P = 0.89); the primary end point of a -0.3 logMAR (15-letter) difference was not met. The mean BCVA for both groups deteriorated over the initial weeks, reaching the worst levels at week 24, followed by a plateau phase until week 48, and then an improvement of +10 and +9 Early Treatment Diabetic Retinopathy Study letters equivalent from the plateau level in the rAAV2/2-ND4-treated and sham-treated eyes, respectively.Conclusions: At 96 weeks after unilateral injection of rAAV2/2-ND4, LHON subjects carrying the m.11778G>A mutation treated within 6 months after vision loss achieved comparable visual outcomes in the injected and uninjected eyes.

Published

2021

10. Smoking and alcohol, health-related quality of life and psychiatric comorbidities in Leber's Hereditary Optic Neuropathy mutation carriers: a prospective cohort study

Author

Rabenstein, Andrea, Catarino, Claudia B., Rampeltshammer, Verena, Schindler, David, Gallenmüller, Constanze, Priglinger, Claudia, Pogarell, Oliver, Rüther, Tobias, and Klopstock, Thomas

Subjects

Adult, Male, Quality of life, congenital, hereditary, and neonatal diseases and abnormalities, Leber’s hereditary optic atrophy, genetic structures, Adolescent, lcsh:Medicine, Optic Atrophy, Hereditary, Leber, DNA, Mitochondrial, Young Adult, LHON, Humans, ddc:610, Prospective Studies, Aged, Depression, Research, lcsh:R, epidemiology [Optic Atrophy, Hereditary, Leber], Smoking, nutritional and metabolic diseases, genetics [Smoking], Middle Aged, genetics [DNA, Mitochondrial], eye diseases, Mitochondrial disorder, Cross-Sectional Studies, genetics [Optic Atrophy, Hereditary, Leber], Mutation, Female, Mental health (< 10), Alcohol

Abstract

Background Leber’s hereditary optic neuropathy (LHON) is a rare mitochondrial disorder, characterized by acute or subacute bilateral vision loss, frequently leading to significant chronic disability, mainly in young people. The causal LHON mutations of the mitochondrial DNA have incomplete penetrance, with the highest risk of disease manifestation for male mutation carriers in the second and third decades of life. Here we evaluated smoking, alcohol drinking habits, health-related quality of life (QOL) and psychiatric comorbidities in a cohort of LHON patients and asymptomatic mutation carriers from a tertiary referral centre. Methods Cross-sectional analysis of the ongoing Munich LHON prospective cohort study. Participants included all LHON patients and asymptomatic LHON mutation carriers older than 16 years at baseline, who were recruited between February 2014 and June 2015 and consented to participate. General, neurological and ophthalmological investigations were performed, including validated questionnaires on smoking, alcohol drinking habits, depressive symptoms and health-related QOL. Results Seventy-one participants were included, 34 LHON patients (82% male) and 37 asymptomatic mutation carriers (19% male). Median age at baseline was 36 years (range 18–75 years). For LHON patients, median age at visual loss onset was 27 years (9 to 72 years). Smoking is more frequent in LHON patients than asymptomatic LHON mutation carriers, and significantly more frequent in both groups than in the general population. Sixty percent of LHON patients, who smoked at disease onset, stopped or significantly reduced smoking after visual loss onset, yet 40% of LHON patients continued to smoke at study baseline. Excessive alcohol consumption is more frequent in male LHON patients than in LHON asymptomatic and more frequent than in the male general population. Further, female asymptomatic LHON mutation carriers are at risk for depression and worse mental QOL scores. Conclusions Given the high prevalence of smoking and excessive drinking in LHON mutation carriers, implementing effective measures to reduce these risk factors may have a significant impact in reducing LHON disease conversion risk. The underrecognized prevalence of mental health issues in this population of LHON mutation carriers highlights the need for awareness and more timely diagnosis, which may lead to improved outcomes. Supplementary Information The online version contains supplementary material available at 10.1186/s13023-021-01724-5.

Published

2021

11. Mitochondrial Disorders

Author

Klopstock, Thomas, Priglinger, Claudia, Yilmaz, Ali, Kornblum, Cornelia, Distelmaier, Felix, and Prokisch, Holger

Subjects

Adult, Mitochondrial Diseases, genetics [Mitochondrial Diseases], Quality of Life, Humans, therapy [Mitochondrial Diseases], ddc:610, General Medicine, Optic Atrophy, Hereditary, Leber, diagnosis [Mitochondrial Diseases], genetics [DNA, Mitochondrial], DNA, Mitochondrial

Abstract

Mitochondrial disorders are among the most common heritable diseases, with an overall lifetime risk of approximately one in 1500. Nonetheless, their diagnosis is often missed because of their extreme phenotypic and genotypic heterogeneity.This review is based on publications retrieved by a selective literature search on the clinical features, genetics, pathogenesis, diagnosis, and treatment of mitochondrial diseases.Pathogenic defects of energy metabolism have been described to date in over 400 genes. Only a small number of these genes lie in the mitochondrial DNA; the corresponding diseases are either maternally inherited or of sporadic distribution. The remaining disease-associated genes are coded in nuclear DNA and cause diseases that are inherited according to Mendelian rules, mostly autosomal recessive. The most severely involved organs are generally those with the highest energy requirements, including the brain, the sensory epithelia, and the extraocular, cardiac, and skeletal musculature. Typical manifestations include epileptic seizures, stroke-like episodes, hearing loss, retinopathy, external ophthalmoparesis, exercise intolerance, and diabetes mellitus. More than two manifestations of these types should arouse suspicion of a disease of energy metabolism. The severity of mitochondrial disorders ranges from very severe disease, already evident in childhood, to relatively mild disease arising in late adulthood. The diagnosis is usually confirmed with molecular-genetic methods. Symptomatic treatment can improve patients' quality of life. The only disease-modifying treatment that has been approved to date is idebenone for the treatment of Leber hereditary optic neuropathy. Intravitreal gene therapy has also been developed for the treatment of this disease; its approval by the European Medicines Agency is pending.Patients with mitochondrial diseases have highly varied manifestations and can thus present to physicians in practically any branch of medicine. A correct diagnosis is the prerequisite for genetic counseling and for the initiation of personalized treatment.

Published

2020

12. Cerebrospinal Fluid Mitochondrial DNA in Rapid and Slow Progressive Forms of Alzheimer’s Disease

Author

Margalida Puigròs, Ramon Trullas, Christian Schmidt, Petar Podlesniy, Franc Llorens, Diego Sepulveda-Falla, Nuria Serra, Inga Zerr, Peter Hermann, Ministerio de Ciencia, Innovación y Universidades (España), Agencia Estatal de Investigación (España), Instituto de Salud Carlos III, Centro Investigación Biomédica en Red Enfermedades Neurodegenerativas (España), Competence Network for Neurodegenerative Dementia (Germany), Federal Ministry of Education and Research (Germany), Llorens, Franc [0000-0002-9756-7497], Schmidt, Christian [0000-0003-2210-4153], Zerr, Inga [0000-0002-6722-2463], Trullas, Ramón [0000-0001-7951-9881], Llorens, Franc, Schmidt, Christian, Zerr, Inga, and Trullas, Ramón

Subjects

0301 basic medicine, Male, Disease, mitochondrial DNA, ADN mitocondrial, Gastroenterology, lcsh:Chemistry, Cohort Studies, pathology [Alzheimer Disease], 0302 clinical medicine, Cerebrospinal fluid, lcsh:QH301-705.5, Spectroscopy, Aged, 80 and over, digital PCR, General Medicine, Alzheimer's disease, Middle Aged, genetics [DNA, Mitochondrial], Mitochondrial DNA, 3. Good health, Computer Science Applications, cerebrospinal fluid [Alzheimer Disease], cerebrospinal fluid [Biomarkers], ddc:540, Cohort, Disease Progression, cerebrospinal fluid [DNA, Mitochondrial], Biomarker (medicine), biomarker, Female, Alzheimer’s disease, classification [Alzheimer Disease], medicine.medical_specialty, DNA, Mitochondrial, Catalysis, Article, cerebrospinal fluid, Inorganic Chemistry, 03 medical and health sciences, Alzheimer Disease, Internal medicine, medicine, Dementia, Humans, Physical and Theoretical Chemistry, Molecular Biology, Pathological, Aged, business.industry, Organic Chemistry, Líquid cefalorraquidi, medicine.disease, 030104 developmental biology, Malaltia d'Alzheimer, lcsh:Biology (General), lcsh:QD1-999, Case-Control Studies, Csf biomarkers, business, Digital PCR, 030217 neurology & neurosurgery, Biomarkers

Abstract

Alzheimer&rsquo, s type dementia (AD) exhibits clinical heterogeneity, as well as differences in disease progression, as a subset of patients with a clinical diagnosis of AD progresses more rapidly (rpAD) than the typical AD of slow progression (spAD). Previous findings indicate that low cerebrospinal fluid (CSF) content of cell-free mitochondrial DNA (cf-mtDNA) precedes clinical signs of AD. We have now investigated the relationship between cf-mtDNA and other biomarkers of AD to determine whether a particular biomarker profile underlies the different rates of AD progression. We measured the content of cf-mtDNA, beta-amyloid peptide 1&ndash, 42 (A&beta, ), total tau protein (t-tau) and phosphorylated tau (p-tau) in the CSF from a cohort of 95 subjects consisting of 49 controls with a neurologic disorder without dementia, 30 patients with a clinical diagnosis of spAD and 16 patients with rpAD. We found that 37% of controls met at least one AD biomarker criteria, while 53% and 44% of subjects with spAD and rpAD, respectively, did not fulfill the two core AD biomarker criteria: high t-tau and low A&beta, in CSF. In the whole cohort, patients with spAD, but not with rpAD, showed a statistically significant 44% decrease of cf-mtDNA in CSF compared to control. When the cohort included only subjects selected by A&beta, and t-tau biomarker criteria, the spAD group showed a larger decrease of cf-mtDNA (69%), whereas in the rpAD group cf-mtDNA levels remained unaltered. In the whole cohort, the CSF levels of cf-mtDNA correlated positively with A&beta, and negatively with p-tau. Moreover, the ratio between cf-mtDNA and p-tau increased the sensitivity and specificity of spAD diagnosis up to 93% and 94%, respectively, in the biomarker-selected cohort. These results show that the content of cf-mtDNA in CSF correlates with the earliest pathological markers of the disease, A&beta, and p-tau, but not with the marker of neuronal damage t-tau. Moreover, these findings confirm that low CSF content of cf-mtDNA is a biomarker for the early detection of AD and support the hypothesis that low cf-mtDNA, together with low A&beta, and high p-tau, constitute a distinctive CSF biomarker profile that differentiates spAD from other neurological disorders.

Published

2020

13. Characterization of a Leber's hereditary optic neuropathy (LHON) family harboring two primary LHON mutations m.11778G > A and m.14484T > C of the mitochondrial DNA

Author

Bettina von Livonius, Katrin Peters, Birgit Repp, Arcangela Iuso, Thomas Klopstock, Holger Prokisch, Claudia B. Catarino, Uwe Ahting, Saskia Biskup, and Mirjana Gusic

Subjects

Adult, Male, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Mitochondrial DNA, genetic structures, Mitochondrial disease, Respiratory chain, Late onset, Optic Atrophy, Hereditary, Leber, medicine.disease_cause, DNA, Mitochondrial, Optic neuropathy, 03 medical and health sciences, 0302 clinical medicine, medicine, Humans, Point Mutation, Sex Ratio, Molecular Biology, Aged, Family Health, Genetics, Mutation, business.industry, Age Factors, Leber's hereditary optic neuropathy, nutritional and metabolic diseases, Cell Biology, Middle Aged, medicine.disease, genetics [DNA, Mitochondrial], eye diseases, Heteroplasmy, pathology [Optic Atrophy, Hereditary, Leber], 030104 developmental biology, genetics [Optic Atrophy, Hereditary, Leber], ddc:540, Molecular Medicine, Female, business, 030217 neurology & neurosurgery

Abstract

Leber's hereditary optic neuropathy (LHON) is an inherited mitochondrial disease that usually leads to acute or subacute bilateral central vision loss. In 95% of cases, LHON is caused by one of three primary mutations of the mitochondrial DNA (mtDNA), m.11778G>A in the MT-ND4 gene, m.14484T>C in the MT-ND6 gene, or m.3460G>A in the MT-ND1 gene. Here we characterize clinically, genetically, and biochemically a LHON family with multiple patients harboring two of these primary LHON mutations, m.11778G>A homoplasmic and m.14484T>C heteroplasmic. The unusually low male-to-female ratio of affected family members is also seen among the other patients previously reported with two primary LHON mutations m.11778G>A and m.14484T>C. While the index patient had very late onset of symptoms at 75years and severe visual loss, her two daughters had both onset in childhood (6 and 9years), with moderate to mild visual loss. A higher degree of heteroplasmy of the m.14484T>C mutation was found to correlate with an earlier age at onset in this family. Ours is the first LHON family harboring two primary LHON mutations where functional studies were performed in several affected family members. A more pronounced bioenergetic defect was found to correlate with an earlier age at onset. The patient with the earliest age at onset had a more significant complex I dysfunction than all controls, including the LHON patient with only the m.11778G>A mutation, suggesting a synergistic effect of the two primary LHON mutations in this patient.

Published

2017

14. Mitochondrial DNA Variation and Heteroplasmy in Monozygotic Twins Clinically Discordant for Multiple Sclerosis

Author

Jörn Walter, N Y Souren, Lisa Ann Gerdes, Tania Kümpfel, Thomas Klopstock, Reinhard Hohlfeld, and Pavlo Lutsik

Subjects

Adult, Male, 0301 basic medicine, Mitochondrial DNA, LEBER HEREDITARY OPTIC NEUROPATHY, MtDNA deletions, Multiple Sclerosis, Clinical manifestation, Biology, DNA, Mitochondrial, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Diseases in Twins, Genetics, medicine, Humans, Genetic Predisposition to Disease, ddc:610, Genetics (clinical), Aged, Subclinical infection, Multiple sclerosis, genetics [Multiple Sclerosis], Genetic Variation, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Twins, Monozygotic, Middle Aged, medicine.disease, genetics [DNA, Mitochondrial], Heteroplasmy, genetics [Diseases in Twins], 030104 developmental biology, genetics [Twins, Monozygotic], Female, 030217 neurology & neurosurgery

Abstract

We examined the debated link between mitochondrial DNA (mtDNA) variation and multiple sclerosis (MS) using 49 monozygotic (MZ) twin pairs clinically discordant for MS, which enables to associate de novo mtDNA variants, skewed heteroplasmy, and mtDNA copy number with MS manifestation. Ultra-deep sequencing of blood-derived mtDNA revealed 25 heteroplasmic variants with potentially pathogenic features in 18 pairs. All variants were pair-specific and had low and/or similar heteroplasmy levels in both cotwins. In one pair, a confirmed pathogenic variant (m.11778G>A, heteroplasmy ∼50%) associated with Leber hereditary optic neuropathy was detected. Detailed diagnostic investigation revealed subclinical MS signs in the prior nondiseased cotwin. Moreover, neither mtDNA deletions nor copy-number variations were involved. Furthermore, the majority of heteroplasmic variants were shared among MZ twins and exhibited more similar heteroplasmy levels in the same tissue of MZ twins as compared with different tissues of the same individual. Heteroplasmy levels were also more similar within MZ twins compared with nonidentical siblings. Our analysis excludes mtDNA variation as a major driver of the discordant clinical manifestation of MS in MZ twins, and provides valuable insights into the occurrence and distribution of heteroplasmic variants within MZ twins and nonidentical siblings, and across different tissues.

Published

2016

15. Mitochondrial replacement approaches: challenges for clinical implementation

Author

Barbara Klopstock, Holger Prokisch, and Thomas Klopstock

Subjects

0301 basic medicine, Male, Mitochondrial Diseases, genetics [Mitochondrial Diseases], Mitochondrial replacement therapy, Inheritance Patterns, lcsh:Medicine, ethics [Fertilization in Vitro], Bioinformatics, prevention & control [Mitochondrial Diseases], Good Quality Blastocyst, Mice, 0302 clinical medicine, ethics [Mitochondrial Replacement Therapy], Medicine, Genetics(clinical), Genetics (clinical), metabolism [Spermatozoa], Enucleated Oocyte, Haplorhini, Donor Mother, Spermatozoa, genetics [DNA, Mitochondrial], Carrier Mother, Mitochondrial Replacement Therapy, Mitochondria, Genes, Mitochondrial, Molecular Medicine, Preimplantation Genetic Diagnosis, Female, methods [Mitochondrial Replacement Therapy], pathology [Oocytes], lcsh:QH426-470, Systems biology, cytology [Spermatozoa], education, genetics [Spindle Apparatus], Fertilization in Vitro, Spindle Apparatus, Preimplantation genetic diagnosis, DNA, Mitochondrial, 03 medical and health sciences, metabolism [Oocytes], Genetics, Animals, Humans, ddc:610, transplantation [Spindle Apparatus], Molecular Biology, business.industry, transplantation [Mitochondria], lcsh:R, Comment, Human genetics, lcsh:Genetics, pathology [Mitochondrial Diseases], 030104 developmental biology, Oocytes, genetics [Mitochondria], business, 030217 neurology & neurosurgery

Abstract

Editorial summary The advent of mitochondrial replacement techniques poses many scientific, regulatory, and ethical questions. Previous studies suggest good safety and efficacy profiles of these techniques, but challenges remain for clinical implementation and international consensus is needed on the regulation of these approaches.

Published

2016

16. Loss of thymidine kinase 2 alters neuronal bioenergetics and leads to neurodegeneration

Author

David Dinsdale, Joanne Betts-Henderson, Kelvin Cain, Paolo Salomoni, Stefano Bartesaghi, Xiaoshan Zhou, Pierluigi Nicotera, and Anna Karlsson

Subjects

Mitochondrial Diseases, enzymology [Ataxia], genetics [Mitochondrial Diseases], genetics [Thymidine Kinase], Mitochondrion, medicine.disease_cause, Mice, Genetics (clinical), Neurons, Mice, Knockout, etiology [Ataxia], Mutation, deficiency [Thymidine Kinase], Neurodegeneration, Brain, Articles, General Medicine, genetics [DNA, Mitochondrial], Immunohistochemistry, Cell biology, metabolism [Neurons], Knockout mouse, medicine.symptom, Mitochondrial DNA, Ataxia, DNA Copy Number Variations, Genetic Vectors, Immunoblotting, Molecular Sequence Data, genetics [Mutation], Biology, DNA, Mitochondrial, Thymidine Kinase, ddc:570, Genetics, medicine, Animals, Myopathy, Molecular Biology, Analysis of Variance, Base Sequence, Lentivirus, medicine.disease, complications [Mitochondrial Diseases], Molecular biology, thymidine kinase 2, metabolism [Brain], Thymidine kinase, cytology [Neurons], Energy Metabolism

Abstract

Mutations of thymidine kinase 2 (TK2), an essential component of the mitochondrial nucleotide salvage pathway, can give rise to mitochondrial DNA (mtDNA) depletion syndromes (MDS). These clinically heterogeneous disorders are characterized by severe reduction in mtDNA copy number in affected tissues and are associated with progressive myopathy, hepatopathy and/or encephalopathy, depending in part on the underlying nuclear genetic defect. Mutations of TK2 have previously been associated with an isolated myopathic form of MDS (OMIM 609560). However, more recently, neurological phenotypes have been demonstrated in patients carrying TK2 mutations, thus suggesting that loss of TK2 results in neuronal dysfunction. Here, we directly address the role of TK2 in neuronal homeostasis using a knockout mouse model. We demonstrate that in vivo loss of TK2 activity leads to a severe ataxic phenotype, accompanied by reduced mtDNA copy number and decreased steady-state levels of electron transport chain proteins in the brain. In TK2-deficient cerebellar neurons, these abnormalities are associated with impaired mitochondrial bioenergetic function, aberrant mitochondrial ultrastructure and degeneration of selected neuronal types. Overall, our findings demonstrate that TK2 deficiency leads to neuronal dysfunction in vivo, and have important implications for understanding the mechanisms of neurological impairment in MDS.

Published

2010

17. Mitochondrial cardiomyopathies: how to identify candidate pathogenic mutations by mitochondrial DNA sequencing, MITOMASTER and phylogeny

Author

Douglas C. Wallace, Michael V. Zaragoza, Marta Diegoli, Eloisa Arbustini, and Martin Brandon

Subjects

Male, Nonsynonymous substitution, Mutation rate, Mitochondrial Diseases, methods [Sequence Analysis, DNA], 030204 cardiovascular system & hematology, phylogeny, medicine.disease_cause, Haplogroup, 0302 clinical medicine, Databases, Genetic, Medicine and Health Sciences, genetic databases, Child, Phylogeny, Genetics (clinical), Genetics, 0303 health sciences, Mutation, Middle Aged, genetics [DNA, Mitochondrial], Heteroplasmy, Mitochondria, Pedigree, 3. Good health, Genes, Mitochondrial, Italy, Echocardiography, Female, cardiomyopathies, Adult, Mitochondrial DNA, Adolescent, Biology, DNA, Mitochondrial, Article, 03 medical and health sciences, Genetic variation, medicine, Humans, genetics, pathology [Cardiomyopathies], Allele frequency, 030304 developmental biology, pathology [Mitochondrial Diseases], Genetic Variation, Infant, Sequence Analysis, DNA, genetics [Mitochondria]

Abstract

Pathogenic mitochondrial DNA (mtDNA) mutations leading to mitochondrial dysfunction can cause cardiomyopathy and heart failure. Owing to a high mutation rate, mtDNA defects may occur at any nucleotide in its 16 569 bp sequence. Complete mtDNA sequencing may detect pathogenic mutations, which can be difficult to interpret because of normal ethnic/geographic-associated haplogroup variation. Our goal is to show how to identify candidate mtDNA mutations by sorting out polymorphisms using readily available online tools. The purpose of this approach is to help investigators in prioritizing mtDNA variants for functional analysis to establish pathogenicity. We analyzed complete mtDNA sequences from 29 Italian patients with mitochondrial cardiomyopathy or suspected disease. Using MITOMASTER and PhyloTree, we characterized 593 substitution variants by haplogroup and allele frequencies to identify all novel, non-haplogroup-associated variants. MITOMASTER permitted determination of each variant's location, amino acid change and evolutionary conservation. We found that 98% of variants were common or rare, haplogroup-associated variants, and thus unlikely to be primary cause in 80% of cases. Six variants were novel, non-haplogroup variants and thus possible contributors to disease etiology. Two with the greatest pathogenic potential were heteroplasmic, nonsynonymous variants: m.15132T>C in MT-CYB for a patient with hypertrophic dilated cardiomyopathy and m.6570GT in MT-CO1 for a patient with myopathy. In summary, we have used our automated information system, MITOMASTER, to make a preliminary distinction between normal mtDNA variation and pathogenic mutations in patient samples; this fast and easy approach allowed us to select the variants for traditional analysis to establish pathogenicity. © 2011 Macmillan Publishers Limited All rights reserved.

Published

2010

18. A distinct clinical phenotype in a German kindred with motor neuron disease carrying a CHCHD10 mutation

Author

Michael T. Heneka, Saskia Biskup, Stefanie Krüger, and Delia Kurzwelly

Subjects

Male, Mitochondrial DNA, Candidate gene, Mitochondrial Diseases, Biology, medicine.disease_cause, DNA, Mitochondrial, pathology [Mitochondria], Mitochondrial Proteins, Exon, C9orf72, medicine, Humans, ddc:610, Amyotrophic lateral sclerosis, Letters to the Editor, etiology [Frontotemporal Dementia], Genetics, Mutation, Amyotrophic Lateral Sclerosis, medicine.disease, genetics [DNA, Mitochondrial], complications [Mitochondrial Diseases], Mitochondria, etiology [Amyotrophic Lateral Sclerosis], Frontotemporal Dementia, genetics [Mitochondrial Proteins], Female, Neurology (clinical), Trinucleotide repeat expansion, Frontotemporal dementia

Abstract

Sir, Emerging data provide evidence for CHCHD10 as a new candidate gene in familial amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) (Bannwarth et al. , 2014; Johnson et al. , 2014; Muller et al. , 2014). This gene encodes a mitochondrial protein located in the intermembrane space (Bannwarth et al. , 2014). Mutant CHCHD10 may lead to altered mitochondrial genome stability and maintenance of cristae junctions (Bannwarth et al. , 2014; Chaussenot et al. , 2014). So far, three different mutations located either in the non-structured N-terminal region or in the α-helix of the CHCHD10 gene have been attributed to cause both ALS and ALS-FTD phenotypes. Here we report another large German family with a history suggestive of autosomal-dominant motor neuron disorder (Fig. 1). After excluding a repeat expansion in C9orf72 and mutations in 25 other known ALS genes in parallel by next-generation sequencing we performed whole-exome sequencing of three affected individuals (Patients III.1, III.2 and III.9). This identified a heterozygous c.44G>T variant (p.Arg15Leu) in exon 2 of the CHCHD10 gene which has recently been reported by Muller et al. (2014) as the likely cause of pure ALS in two German families and was also identified in three families with familial motor neuron disease in the USA (Johnson et al. , 2014). The mutation segregated with disease in another cousin (Patient III.5) of our index patient (Patient III.1) and could not be identified in his 41-year-old son (Patient IV.1) and an 85-year-old aunt (Patient II.7), who are both unaffected. No DNA samples were available from the …

Published

2015

19. MTO1-Deficient Mouse Model Mirrors the Human Phenotype Showing Complex I Defect and Cardiomyopathy

Author

Ilona Mossbrugger, Frauke Neff, Ilka Wittig, Evelyn Schiller, Wolfgang Wurst, Valentina Strecker, Andreas Bender, Anja Schrewe, Thomas Floss, Sabine M. Hölter, Valerie Gailus-Durner, Helmut Fuchs, Julia Calzada-Wack, Thomas Meitinger, Thomas Klopstock, Raffi Bekeredjian, Martin Hrabě de Angelis, Michaela Aichler, Tina Wenz, Holger Prokisch, Ramona Zeh, Lore Becker, Dirk Janik, Iulia Dumitru, Leticia Quintanilla-Fend, Eva Kling, and Axel Walch

Subjects

Male, pathology [Myocardium], Pathology, Heredity, Mitochondrial Diseases, Mitochondrial Myopathy, Mitochondrial translation, Physiology, Respiratory chain, Cardiomyopathy, Gene Dosage, Gene Expression, pathology [Cardiomyopathies], Mitochondrion, genetics [Carrier Proteins], Mto1 protein, mouse, Biochemistry, pathology [Mitochondria], Oxidative Phosphorylation, Mice, Molecular Cell Biology, Medicine and Health Sciences, genetics [Electron Transport Complex I], Energy-Producing Organelles, genetics [Cardiomyopathies], Mice, Knockout, Multidisciplinary, Respiration, Hypertrophic cardiomyopathy, RNA-Binding Proteins, Heart, Animal Models, genetics [DNA, Mitochondrial], Mitochondria, Phenotypes, Genes, Mitochondrial, Cardiovascular Diseases, Lactic acidosis, Gene Knockdown Techniques, Medicine, Female, Cardiomyopathies, Arrhythmia, Research Article, medicine.medical_specialty, Science, Cardiology, Mutagenesis (molecular biology technique), Mouse Models, Bioenergetics, Research and Analysis Methods, Gene dosage, DNA, Mitochondrial, Mitochondrial Proteins, Oxygen Consumption, Model Organisms, medicine, Genetics, Animals, Humans, ddc:610, Clinical Genetics, physiopathology [Heart], Electron Transport Complex I, business.industry, Myocardium, Biology and Life Sciences, Human Genetics, Cell Biology, physiopathology [Cardiomyopathies], medicine.disease, metabolism [Mitochondria], Mice, Inbred C57BL, Disease Models, Animal, Protein Translation, business, Physiological Processes, Carrier Proteins

Abstract

Recently, mutations in the mitochondrial translation optimization factor 1 gene (MTO1) were identified as causative in children with hypertrophic cardiomyopathy, lactic acidosis and respiratory chain defect. Here, we describe an MTO1-deficient mouse model generated by gene trap mutagenesis that mirrors the human phenotype remarkably well. As in patients, the most prominent signs and symptoms were cardiovascular and included bradycardia and cardiomyopathy. In addition, the mutant mice showed a marked worsening of arrhythmias during induction and reversal of anaesthesia. The detailed morphological and biochemical workup of murine hearts indicated that the myocardial damage was due to complex I deficiency and mitochondrial dysfunction. In contrast, neurological examination was largely normal in Mto1-deficient mice. A translational consequence of this mouse model may be to caution against anaesthesia-related cardiac arrhythmias which may be fatal in patients.

Published

2014

20. Human iPSC-Derived Neural Progenitors Are an Effective Drug Discovery Model for Neurological mtDNA Disorders

Author

Josef Priller, Manvendra K. Singh, Nancy Mah, Carmen Lorenz, Pierre Lesimple, Anne Lombès, Gizem Inak, Zsuzsanna Izsvák, Ekaterini-Maria Lyras, Erich E. Wanker, Marcus Semtner, James Adjaye, Raul Bukowiecki, Megan Leong, Barbara Mlody, Karine Auré, Norbert Huebner, Jochen C. Meier, David Meierhofer, Thorsten Mielke, Jenny Eichhorst, Annika Zink, Alessandro Prigione, Markus Schuelke, Frédéric Bouillaud, Vanessa Pfiffer, Beatrix Fauler, Burkhard Wiesner, and Oleksandr Zabiegalov

Subjects

0301 basic medicine, Mitochondrial DNA, Mitochondrial disease, methods [Drug Discovery], metabolism [Neural Stem Cells], Mitochondrion, Biology, medicine.disease_cause, DNA, Mitochondrial, Cell Line, 03 medical and health sciences, 0302 clinical medicine, ddc:570, Genetics, medicine, Humans, metabolism [Calcium], cytology [Neural Stem Cells], Progenitor cell, Induced pluripotent stem cell, Mutation, cytology [Induced Pluripotent Stem Cells], Cell Biology, medicine.disease, genetics [DNA, Mitochondrial], Phenotype, Molecular biology, Neural stem cell, Cell biology, metabolism [Induced Pluripotent Stem Cells], 030104 developmental biology, Cardiovascular and Metabolic Diseases, Molecular Medicine, Calcium, genetics [Mitochondria], Function and Dysfunction of the Nervous System, 030217 neurology & neurosurgery

Abstract

Mitochondrial DNA (mtDNA) mutations frequently cause neurological diseases. Modeling of these defects has been difficult because of the challenges associated with engineering mtDNA. We show here that neural progenitor cells (NPCs) derived from human induced pluripotent stem cells (iPSCs) retain the parental mtDNA profile and exhibit a metabolic switch toward oxidative phosphorylation. NPCs derived in this way from patients carrying a deleterious homoplasmic mutation in the mitochondrial gene MT-ATP6 (m.9185T>C) showed defective ATP production and abnormally high mitochondrial membrane potential (MMP), plus altered calcium homeostasis, which represents a potential cause of neural impairment. High-content screening of FDA-approved drugs using the MMP phenotype highlighted avanafil, which we found was able to partially rescue the calcium defect in patient NPCs and differentiated neurons. Overall, our results show that iPSC-derived NPCs provide an effective model for drug screening to target mtDNA disorders that affect the nervous system.

Published

2017

21. Lewy body pathology is associated with mitochondrial DNA damage in Parkinson's disease

Author

Sarina K. Müller, Thomas Klopstock, Andreas Bender, Falk Schlaudraff, Birgit Liss, Tobias Högen, Christoph Laub, and Matthias Elstner

Subjects

Male, Aging, Pathology, Parkinson's disease, genetics [Lewy Bodies], Protein aggregation, physiology [Oxidative Stress], chemistry.chemical_compound, Mesencephalon, genetics [Parkinson Disease], genetics [Oxidative Stress], metabolism [Reactive Oxygen Species], metabolism [alpha-Synuclein], Neurons, Aged, 80 and over, biology, General Neuroscience, Parkinson Disease, genetics [DNA, Mitochondrial], metabolism [Neurons], alpha-Synuclein, Female, medicine.medical_specialty, Mitochondrial DNA, Tau protein, Substantia nigra, DNA, Mitochondrial, medicine, Humans, ddc:610, SNCA protein, human, Aged, Alpha-synuclein, cytology [Mesencephalon], pathology [Lewy Bodies], Lewy body, medicine.disease, pathology [Parkinson Disease], Oxidative Stress, nervous system, chemistry, cytology [Neurons], biology.protein, Synuclein, Lewy Bodies, Neurology (clinical), Geriatrics and Gerontology, Reactive Oxygen Species, Developmental Biology, DNA Damage

Abstract

Mitochondrial dysfunction has been strongly implicated in the pathogenesis of Parkinson's disease (PD) and Alzheimer's disease (AD), but its relation to protein aggregation is unclear. PD is characterized by synuclein aggregation (i.e., Lewy body (LB) formation). In AD, the abnormal accumulation of tau protein forms neurofibrillary tangles. In this study, we laser-dissected LB-positive and -negative neurons from the substantia nigra of postmortem PD brains, and tau-positive and -negative hippocampal neurons from AD brains. We quantified mitochondrial DNA deletions in relation to the cellular phenotype and in comparison with age-matched controls. Deletion levels were highest in LB-positive neurons of PD brains (40.5 � 16.8%), followed by LB-negative neurons of PD cases (31.8 � 14.4%) and control subjects (25.6 � 17.5%; analysis of variance p < 0.005). In hippocampal neurons, deletion levels were 25%e30%, inde- pendent of disease status and neurofibrillary tangles. The presented findings imply increased mito- chondrial DNA damage in LB-positive midbrain neurons, but do not support a direct causative link of respiratory chain dysfunction and protein aggregation.

Published

2013

22. Mitochondrial DNA polymorphisms specifically modify cerebral β-amyloid proteostasis

Author

Hans-Jochen Heinze, Lary C. Walker, Jörg Gsponer, Saleh M. Ibrahim, Katja Scheffler, Bruno Miroux, Jens Pahnke, Jan Stenzel, Oliver von Bohlen und Halbach, Tina Dunkelmann, and Markus Krohn

Subjects

Male, Mitochondrial DNA, Amyloid beta, metabolism [Amyloid beta-Peptides], genetics [Alzheimer Disease], Mice, Inbred Strains, Mice, Transgenic, Oxidative phosphorylation, metabolism [Microglia], Mitochondrion, Biology, medicine.disease_cause, Human mitochondrial genetics, DNA, Mitochondrial, Article, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, Mice, Inbred strain, Alzheimer Disease, genetics [Oxidative Stress], medicine, genetics [Amyloid beta-Peptides], Animals, ddc:610, Amyloid beta-Peptides, Polymorphism, Genetic, Brain, metabolism [Mitochondria], genetics [DNA, Mitochondrial], Molecular biology, Mitochondria, Oxidative Stress, Proteostasis, metabolism [Brain], biology.protein, Female, genetics [Mitochondria], Neurology (clinical), Microglia, metabolism [DNA, Mitochondrial], metabolism [Alzheimer Disease], Oxidative stress

Abstract

Several lines of evidence link mutations and deletions in mitochondrial DNA (mtDNA) and its maternal inheritance to neurodegenerative diseases in the elderly. Age-related mutations of mtDNA modulate the tricarboxylic cycle enzyme activity, mitochondrial oxidative phosphorylation capacity and oxidative stress response. To investigate the functional relevance of specific mtDNA polymorphisms of inbred mouse strains in the proteostasis regulation of the brain, we established novel mitochondrial congenic mouse lines of Alzheimer's disease (AD). We crossed females from inbred strains (FVB/N, AKR/J, NOD/LtJ) with C57BL/6 males for at least ten generations to gain specific mitochondrial conplastic strains with pure C57BL/6 nuclear backgrounds. We show that specific mtDNA polymorphisms originating from the inbred strains differentially influence mitochondrial energy metabolism, ATP production and ATP-driven microglial activity, resulting in alterations of cerebral β-amyloid (Aβ) accumulation. Our findings demonstrate that mtDNA-related increases in ATP levels and subsequently in microglial activity are directly linked to decreased Aβ accumulation in vivo, implicating reduced mitochondrial function in microglia as a causative factor in the development of age-related cerebral proteopathies such as AD.

Published

2012