Your search keyword '"Karin Naess"' showing total 44 results

1. Unraveling mucolipidosis type III gamma through whole genome sequencing in late-onset retinitis pigmentosa: a case report

Author

Karl De Geer, Katarzyna Mascianica, Karin Naess, Eliane Sardh, Anna Lindstrand, and Erik Björck

Subjects

Inherited retinal dystrophy, Retinitis pigmentosa, Whole genome sequencing, GNPTG, Mucolipidosis type III gamma, Lysosomal disease, Ophthalmology, RE1-994

Abstract

Abstract Background We describe the case of a 47-year-old man referred to a retinal clinic and diagnosed with late-onset retinitis pigmentosa. Surprisingly, genetic testing revealed compound heterozygous pathogenic variants in GNPTG, leading to the diagnosis of the autosomal recessive lysosomal storage disorder mucolipidosis type III gamma. Mucolipidosis type III gamma is typically diagnosed during childhood due to symptoms relating to skeletal dysplasia. Retinal dystrophy is not a common phenotypic feature. Case presentation Ophthalmologic examination was consistent with a mild form of retinitis pigmentosa and included fundus photography, measurement of best-corrected visual acuity, optical coherence tomography, electroretinogram and visual field testing. Extraocular findings included joint restriction and pains from an early age leading to bilateral hip replacement by age 30, aortic insufficiency, and hypertension. Genetic analysis was performed by whole genome sequencing filtered for a gene panel of 325 genes associated with retinal disease. Two compound heterozygous pathogenic variants were identified in GNPTG, c.347_349del and c.607dup. The diagnosis of mucolipidosis type III gamma was confirmed biochemically by measurement of increased activities of specific lysosomal enzymes in plasma. Conclusion To our knowledge this is the first description of retinitis pigmentosa caused by compound heterozygous variants in GNPTG, providing further indications that late-onset retinal dystrophy is part of the phenotypic spectrum of mucolipidosis type III gamma.

Published

2023

2. Genome sequencing with comprehensive variant calling identifies structural variants and repeat expansions in a large fraction of individuals with ataxia and/or neuromuscular disorders

Author

Marlene Ek, Daniel Nilsson, Martin Engvall, Helena Malmgren, Håkan Thonberg, Maria Pettersson, Britt-Marie Anderlid, Anna Hammarsjö, Hafdis T. Helgadottir, Snjolaug Arnardottir, Karin Naess, Inger Nennesmo, Martin Paucar, Helgi Thor Hjartarson, Rayomand Press, Göran Solders, Thomas Sejersen, Anna Lindstrand, and Malin Kvarnung

Subjects

neuromuscular disorders, genome sequencing, single nucleotide variant, structural variant, repeat expansion, ataxia, Neurology. Diseases of the nervous system, RC346-429

Abstract

IntroductionNeuromuscular disorders (NMDs) have a heterogeneous etiology. A genetic diagnosis is key to personalized healthcare and access to targeted treatment for the affected individuals.MethodsIn this study, 861 patients with NMDs were analyzed with genome sequencing and comprehensive variant calling including single nucleotide variants, small insertions/deletions (SNVs/INDELs), and structural variants (SVs) in a panel of 895 NMD genes, as well as short tandem repeat expansions (STRs) at 28 loci. In addition, for unsolved cases with an unspecific clinical presentation, the analysis of a panel with OMIM disease genes was added.ResultsIn the cohort, 27% (232/861) of the patients harbored pathogenic variants, of which STRs and SVs accounted for one-third of the patients (71/232). The variants were found in 107 different NMD genes. Furthermore, 18 pediatric patients harbored pathogenic variants in non-NMD genes.DiscussionOur results highlight that for children with unspecific hypotonia, a genome-wide analysis rather than a disease-based gene panel should be considered as a diagnostic approach. More importantly, our results clearly show that it is crucial to include STR- and SV-analyses in the diagnostics of patients with neuromuscular disorders.

Published

2023

3. Renal Phenotype in Mitochondrial Diseases: A Multicenter Study

Author

Maria Parasyri, Per Brandström, Johanna Uusimaa, Elsebet Ostergaard, Omar Hikmat, Pirjo Isohanni, Karin Naess, I.F.M. de Coo, Andrés Nascimento Osorio, Matti Nuutinen, Christopher Lindberg, Laurence A. Bindoff, Már Tulinius, Niklas Darin, and Kalliopi Sofou

Subjects

mitochondrial disease, acute kidney injury, mitochondrial dna, renal manifestations, Internal medicine, RC31-1245

Abstract

Aims: This study aimed to investigate associations between renal and extrarenal manifestations of mitochondrial diseases and their natural history as well as predictors of renal disease severity and overall disease outcome. The secondary aim was to generate a protocol of presymptomatic assessment and monitoring of renal function in patients with a defined mitochondrial disease. Methods: A multicenter, retrospective cohort study was performed by the Mitochondrial Clinical and Research Network (MCRN). Patients of any age with renal manifestations associated with a genetically verified mitochondrial disease were included from 8 expert European centers specializing in mitochondrial diseases: Gothenburg, Oulu, Copenhagen, Bergen, Helsinki, Stockholm, Rotterdam, and Barcelona. Results: Of the 36 patients included, two-thirds had mitochondrial DNA-associated disease. Renal manifestations were the first sign of mitochondrial disease in 19%, and renal involvement was first identified by laboratory tests in 57% of patients. Acute kidney injury occurred in 19% of patients and was the first sign of renal disease in the majority of these. The most common renal manifestation was chronic kidney disease (75% with stage 2 or greater), followed by tubulopathy (44.4%), the latter seen mostly among patients with single large-scale mitochondrial DNA deletions. Acute kidney injury and tubulopathy correlated with worse survival outcome. The most common findings on renal imaging were increased echogenicity and renal dysplasia/hypoplasia. Renal histology revealed focal segmental glomerulosclerosis, nephrocalcinosis, and nephronophthisis. Conclusion: Acute kidney injury is a distinct renal phenotype in patients with mitochondrial disease. Our results highlight the importance to recognize renal disease as a sign of an underlying mitochondrial disease. Acute kidney injury and tubulopathy are 2 distinct indicators of poor survival in patients with mitochondrial diseases.

Published

2022

4. Expanding the phenotypic spectrum of BCS1L‐related mitochondrial disease

Author

Omar Hikmat, Pirjo Isohanni, Nandaki Keshavan, Matteo P. Ferla, Elisa Fassone, Mary‐Alice Abbott, Marcello Bellusci, Niklas Darin, David Dimmock, Daniele Ghezzi, Henry Houlden, Federica Invernizzi, Nazreen B. Kamarus Jaman, Manju A. Kurian, Eva Morava, Karin Naess, Juan Darío Ortigoza‐Escobar, Sumit Parikh, Alessandra Pennisi, Giulia Barcia, Karin B. Tylleskär, Damien Brackman, Saskia B. Wortmann, Jenny C. Taylor, Laurence A. Bindoff, Vineta Fellman, and Shamima Rahman

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective To delineate the full phenotypic spectrum of BCS1L‐related disease, provide better understanding of the genotype–phenotype correlations and identify reliable prognostic disease markers. Methods We performed a retrospective multinational cohort study of previously unpublished patients followed in 15 centres from 10 countries. Patients with confirmed biallelic pathogenic BCS1L variants were considered eligible. Clinical, laboratory, neuroimaging and genetic data were analysed. Patients were stratified into different groups based on the age of disease onset, whether homozygous or compound heterozygous for the c.232A>G (p.Ser78Gly) variant, and those with other pathogenic BCS1L variants. Results Thirty‐three patients were included. We found that growth failure, lactic acidosis, tubulopathy, hepatopathy and early death were more frequent in those with disease onset within the first month of life. In those with onset after 1 month, neurological features including movement disorders and seizures were more frequent. Novel phenotypes, particularly involving movement disorder, were identified in this group. The presence of the c.232A>G (p.Ser78Gly) variant was associated with significantly worse survival and exclusively found in those with disease onset within the first month of life, whilst other pathogenic BCS1L variants were more frequent in those with later symptom onset. Interpretation The phenotypic spectrum of BCS1L‐related disease comprises a continuum of clinical features rather than a set of separate syndromic clinical identities. Age of onset defines BCS1L‐related disease clinically and early presentation is associated with poor prognosis. Genotype correlates with phenotype in the presence of the c.232A>G (p.Ser78Gly) variant.

Published

2021

5. Integration of whole genome sequencing into a healthcare setting: high diagnostic rates across multiple clinical entities in 3219 rare disease patients

Author

Henrik Stranneheim, Kristina Lagerstedt-Robinson, Måns Magnusson, Malin Kvarnung, Daniel Nilsson, Nicole Lesko, Martin Engvall, Britt-Marie Anderlid, Henrik Arnell, Carolina Backman Johansson, Michela Barbaro, Erik Björck, Helene Bruhn, Jesper Eisfeldt, Christoph Freyer, Giedre Grigelioniene, Peter Gustavsson, Anna Hammarsjö, Maritta Hellström-Pigg, Erik Iwarsson, Anders Jemt, Mikael Laaksonen, Sara Lind Enoksson, Helena Malmgren, Karin Naess, Magnus Nordenskjöld, Mikael Oscarson, Maria Pettersson, Chiara Rasi, Adam Rosenbaum, Ellika Sahlin, Eliane Sardh, Tommy Stödberg, Bianca Tesi, Emma Tham, Håkan Thonberg, Virpi Töhönen, Ulrika von Döbeln, Daphne Vassiliou, Sofie Vonlanthen, Ann-Charlotte Wikström, Josephine Wincent, Ola Winqvist, Anna Wredenberg, Sofia Ygberg, Rolf H. Zetterström, Per Marits, Maria Johansson Soller, Ann Nordgren, Valtteri Wirta, Anna Lindstrand, and Anna Wedell

Subjects

Whole genome sequencing, Monogenic disease, Single nucleotide variant, Clinical diagnostics, Medicine, Genetics, QH426-470

Abstract

Abstract Background We report the findings from 4437 individuals (3219 patients and 1218 relatives) who have been analyzed by whole genome sequencing (WGS) at the Genomic Medicine Center Karolinska-Rare Diseases (GMCK-RD) since mid-2015. GMCK-RD represents a long-term collaborative initiative between Karolinska University Hospital and Science for Life Laboratory to establish advanced, genomics-based diagnostics in the Stockholm healthcare setting. Methods Our analysis covers detection and interpretation of SNVs, INDELs, uniparental disomy, CNVs, balanced structural variants, and short tandem repeat expansions. Visualization of results for clinical interpretation is carried out in Scout—a custom-developed decision support system. Results from both singleton (84%) and trio/family (16%) analyses are reported. Variant interpretation is done by 15 expert teams at the hospital involving staff from three clinics. For patients with complex phenotypes, data is shared between the teams. Results Overall, 40% of the patients received a molecular diagnosis ranging from 19 to 54% for specific disease groups. There was heterogeneity regarding causative genes (n = 754) with some of the most common ones being COL2A1 (n = 12; skeletal dysplasia), SCN1A (n = 8; epilepsy), and TNFRSF13B (n = 4; inborn errors of immunity). Some causative variants were recurrent, including previously known founder mutations, some novel mutations, and recurrent de novo mutations. Overall, GMCK-RD has resulted in a large number of patients receiving specific molecular diagnoses. Furthermore, negative cases have been included in research studies that have resulted in the discovery of 17 published, novel disease-causing genes. To facilitate the discovery of new disease genes, GMCK-RD has joined international data sharing initiatives, including ClinVar, UDNI, Beacon, and MatchMaker Exchange. Conclusions Clinical WGS at GMCK-RD has provided molecular diagnoses to over 1200 individuals with a broad range of rare diseases. Consolidation and spread of this clinical-academic partnership will enable large-scale national collaboration.

Published

2021

6. The impact of gender, puberty, and pregnancy in patients with POLG disease

Author

Omar Hikmat, Karin Naess, Martin Engvall, Claus Klingenberg, Magnhild Rasmussen, Chantal M. E. Tallaksen, Christian Samsonsen, Eylert Brodtkorb, Elsebet Ostergaard, Rene de Coo, Leticia Pias‐Peleteiro, Pirjo Isohanni, Johanna Uusimaa, Niklas Darin, Shamima Rahman, and Laurence A. Bindoff

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective To study the impact of gender, puberty, and pregnancy on the expression of POLG disease, one of the most common mitochondrial diseases known. Methods Clinical, laboratory, and genetic data were collected retrospectively from 155 patients with genetically confirmed POLG disease recruited from seven European countries. We used the available data to study the impact of gender, puberty, and pregnancy on disease onset and deterioration. Results We found that disease onset early in life was common in both sexes but there was also a second peak in females around the time of puberty. Further, pregnancy had a negative impact with 10 of 14 women (71%) experiencing disease onset or deterioration during pregnancy. Interpretation Gender clearly influences the expression of POLG disease. While onset very early in life was common in both males and females, puberty in females appeared associated both with disease onset and increased disease activity. Further, both disease onset and deterioration, including seizure aggravation and status epilepticus, appeared to be associated with pregnancy. Thus, whereas disease activity appears maximal early in life with no subsequent peaks in males, both menarche and pregnancy appear associated with disease onset or worsening in females. This suggests that hormonal changes may be a modulating factor.

Published

2020

7. A Missense Variant in PDK1 Associated with Severe Neurodevelopmental Delay and Epilepsy

Author

Raquel Vaz, Josephine Wincent, Najla Elfissi, Kristina Rosengren Forsblad, Maria Pettersson, Karin Naess, Anna Wedell, Anna Wredenberg, Anna Lindstrand, and Sofia Ygberg

Subjects

pyruvate dehydrogenase kinase, epilepsy, neurodevelopmental delay, zebrafish, Biology (General), QH301-705.5

Abstract

The pyruvate dehydrogenase complex (PDC) is responsible for the conversion of pyruvate into acetyl-CoA, which is used for energy conversion in cells. PDC activity is regulated by phosphorylation via kinases and phosphatases (PDK/PDP). Variants in all subunits of the PDC and in PDK3 have been reported, with varying phenotypes including lactic acidosis, neurodevelopmental delay, peripheral neuropathy, or seizures. Here, we report a de novo heterozygous missense variant in PDK1 (c.1139G > A; p.G380D) in a girl with developmental delay and early onset severe epilepsy. To investigate the role of PDK1G380D in energy metabolism and neuronal development, we used a zebrafish model. In zebrafish embryos we show a reduced number of cells with mitochondria with membrane potential, reduced movements, and a delay in neuronal development. Furthermore, we observe a reduction in the phosphorylation of PDH-E1α by PDKG380D, which suggests a disruption in the regulation of PDC activity. Finally, in patient fibroblasts, a mild reduction in the ratio of phosphorylated PDH over total PDH-E1α was detected. In summary, our findings support the notion that this aberrant PDK1 activity is the cause of clinical symptoms in the patient.

Published

2022

8. Mutations in the mitochondrial tryptophanyl‐tRNA synthetase cause growth retardation and progressive leukoencephalopathy

Author

Camilla Maffezzini, Isabelle Laine, Cristina Dallabona, Paula Clemente, Javier Calvo‐Garrido, Rolf Wibom, Karin Naess, Michela Barbaro, Anna Falk, Claudia Donnini, Christoph Freyer, Anna Wredenberg, and Anna Wedell

Subjects

aminoacylation, mitochondria, mitochondrial tryptophanyl‐tRNA synthetase, WARS2, Genetics, QH426-470

Abstract

Abstract Background Mutations in mitochondrial aminoacyl tRNA synthetases form a subgroup of mitochondrial disorders often only perturbing brain function by affecting mitochondrial translation. Here we report two siblings with mitochondrial disease, due to compound heterozygous mutations in the mitochondrial tryptophanyl‐tRNA synthetase (WARS2) gene, presenting with severe neurological symptoms but normal mitochondrial function in skeletal muscle biopsies and cultured skin fibroblasts. Methods Whole exome sequencing on genomic DNA samples from both subjects and their parents identified two compound heterozygous variants c.833T>G (p.Val278Gly) and c.938A>T (p.Lys313Met) in the WARS2 gene as potential disease‐causing variants. We generated patient‐derived neuroepithelial stem cells and modeled the disease in yeast and Drosophila melanogaster to confirm pathogenicity. Results Biochemical analysis of patient‐derived neuroepithelial stem cells revealed a mild combined complex I and IV defect, while modeling the disease in yeast demonstrated that the reported aminoacylation defect severely affects respiration and viability. Furthermore, silencing of wild type WARS2 in Drosophila melanogaster showed that a partial defect in aminoacylation is enough to cause lethality. Conclusions Our results establish the identified WARS2 variants as disease‐causing and highlight the benefit of including human neuronal models, when investigating mutations specifically affecting the nervous system.

Published

2019

9. Expanded Screening of One Million Swedish Babies with R4S and CLIR for Post-Analytical Evaluation of Data

Author

Lene Sörensen, Ulrika von Döbeln, Henrik Åhlman, Annika Ohlsson, Martin Engvall, Karin Naess, Carolina Backman-Johansson, Yvonne Nordqvist, Anna Wedell, and Rolf H. Zetterström

Subjects

newborn screening, post-analytical evaluation, Collaborative Laboratory Integrated Reports (CLIR), tandem mass spectrometry, expanded screening, dried blood spots (DBS), Pediatrics, RJ1-570

Abstract

Sweden has one neonatal screening laboratory, receiving 115 to 120 thousand samples per year. Among the one million babies screened by tandem mass spectrometry from November 2010 until July 2019, a total of 665 babies were recalled and 311 verified as having one of the diseases screened for with this methodology, giving a positive predictive value (PPV) of 47% and an incidence of 1:3200. The PPV was high (41%) already in the first year after start of screening, thanks to the availability of the collaborative project Region 4 Stork database. The PPV is presently 58%. This improvement was achieved by the implementation of second-tier analyses in the screening for methylmalonic aciduria, propionic aciduria, isovaleric aciduria, and homocystinuria, and the employment of various post analytical tools of the Region 4 Stork, and its successor the collaborative laboratory integrated reports.

Published

2020

10. Visual outcome, ocular findings, and visual quality of life in patients with Fabry disease

Author

Mattias Nilsson, Hani Tavakoli Kolagari, David Epstein, Branka Samolov, Monica Olsson, Karin Naess, Mikael Oscarson, and Kristina Teaer Fahnehjelm

Subjects

Ophthalmology, Pediatrics, Perinatology and Child Health, Genetics (clinical)

Abstract

Fabry disease (FD) is an X-linked lysosomal disease, in which diagnosis is often established several years after onset of symptoms. Ocular manifestations can occur in childhood and be a clue to earlier diagnosis. The aim was to report ocular outcome and visual quality of life (QoL) in patients with FD.FD-patients recruited from Karolinska University Hospital underwent ophthalmological examinations including best corrected visual acuity (BCVA), refraction, biomicroscopy, optical coherence tomography, keratometry, review of medical records and QoL Inventories. A total severity score (TSS), as estimated via Fabry Stabilization Index, was calculated.Twenty-six FD-patients (16 men) mean age 36.4 years (range 5.0-63.5 years) were included. BCVA was median 1.0 (range 0.5-1.6). Conjunctival blood vessel tortuosity occurred in 15/26 patients, chemosis in 2/26 patients, cornea verticillata in 23/26 patients, lens opacities in 19/26 patients, and tortuous or dilated retinal vessels in 20/25 patients. Group-wise comparisons of adult patients showed no differences regarding age, TSS, or ocular parameters. Overall, TSS was correlated to age (r = 0.53, p = 0.02). A linear regression model showed that age and sex explained 38% of the variance in TSS. Keratometry did not reveal corneal ectasia in any of the 12 patients examined. VFQ 25 in 15 patients showed a high median composite score, 93.6 (range: 78.1-100).BCVA in FD-patients was good despite corneal and lens pathology. Ocular variables did not show an association with TSS in adult patients. Corneal or lens opacities should also lead to a suspicion of FD in children.

Published

2022

11. A Missense Variant in PDK1 Associated with Severe Neurodevelopmental Delay and Epilepsy

Author

Ygberg, Raquel Vaz, Josephine Wincent, Najla Elfissi, Kristina Rosengren Forsblad, Maria Pettersson, Karin Naess, Anna Wedell, Anna Wredenberg, Anna Lindstrand, and Sofia

Subjects

pyruvate dehydrogenase kinase, epilepsy, neurodevelopmental delay, zebrafish

Abstract

The pyruvate dehydrogenase complex (PDC) is responsible for the conversion of pyruvate into acetyl-CoA, which is used for energy conversion in cells. PDC activity is regulated by phosphorylation via kinases and phosphatases (PDK/PDP). Variants in all subunits of the PDC and in PDK3 have been reported, with varying phenotypes including lactic acidosis, neurodevelopmental delay, peripheral neuropathy, or seizures. Here, we report a de novo heterozygous missense variant in PDK1 (c.1139G > A; p.G380D) in a girl with developmental delay and early onset severe epilepsy. To investigate the role of PDK1G380D in energy metabolism and neuronal development, we used a zebrafish model. In zebrafish embryos we show a reduced number of cells with mitochondria with membrane potential, reduced movements, and a delay in neuronal development. Furthermore, we observe a reduction in the phosphorylation of PDH-E1α by PDKG380D, which suggests a disruption in the regulation of PDC activity. Finally, in patient fibroblasts, a mild reduction in the ratio of phosphorylated PDH over total PDH-E1α was detected. In summary, our findings support the notion that this aberrant PDK1 activity is the cause of clinical symptoms in the patient.

Published

2022

12. The impact of gender, puberty, and pregnancy in patients with POLG disease

Author

Karin Naess, Shamima Rahman, Elsebet Ostergaard, Martin Engvall, Johanna Uusimaa, Claus Klingenberg, Laurence A. Bindoff, Niklas Darin, Chantal M. E. Tallaksen, Leticia Pias-Peleteiro, René I. de Coo, Christian Samsonsen, Magnhild Rasmussen, Eylert Brodtkorb, Omar Hikmat, Pirjo Isohanni, HUS Children and Adolescents, Research Programs Unit, Anu Wartiovaara / Principal Investigator, Clinicum, Children's Hospital, STEMM - Stem Cells and Metabolism Research Program, Faculty of Medicine, University of Helsinki, Lastenneurologian yksikkö, RS: MHeNs - R3 - Neuroscience, and Klinische Genetica

Subjects

0301 basic medicine, Mitochondrial Diseases, Physiology, Disease, DNA-POLYMERASE-GAMMA, MITOCHONDRIAL, 3124 Neurology and psychiatry, Epilepsy, 0302 clinical medicine, Pregnancy, NEUROSTEROIDS, LACTIC-ACIDOSIS, EPILEPSY, Research Articles, General Neuroscience, ENCEPHALOPATHY, VDP::Medical disciplines: 700::Basic medical, dental and veterinary science disciplines: 710, 3. Good health, DNA Polymerase gamma, Europe, Menarche, Female, medicine.symptom, RC321-571, Research Article, DISORDERS, Encephalopathy, Neurosciences. Biological psychiatry. Neuropsychiatry, Status epilepticus, 03 medical and health sciences, medicine, Humans, RC346-429, Retrospective Studies, business.industry, MUTATIONS, Puberty, STROKE-LIKE EPISODES, 3112 Neurosciences, Retrospective cohort study, VDP::Medisinske Fag: 700::Basale medisinske, odontologiske og veterinærmedisinske fag: 710, medicine.disease, 030104 developmental biology, MODULATORS, Neurology (clinical), Neurology. Diseases of the nervous system, business, 030217 neurology & neurosurgery

Abstract

Objective To study the impact of gender, puberty, and pregnancy on the expression of POLG disease, one of the most common mitochondrial diseases known. Methods Clinical, laboratory, and genetic data were collected retrospectively from 155 patients with genetically confirmed POLG disease recruited from seven European countries. We used the available data to study the impact of gender, puberty, and pregnancy on disease onset and deterioration. Results We found that disease onset early in life was common in both sexes but there was also a second peak in females around the time of puberty. Further, pregnancy had a negative impact with 10 of 14 women (71%) experiencing disease onset or deterioration during pregnancy. Interpretation Gender clearly influences the expression of POLG disease. While onset very early in life was common in both males and females, puberty in females appeared associated both with disease onset and increased disease activity. Further, both disease onset and deterioration, including seizure aggravation and status epilepticus, appeared to be associated with pregnancy. Thus, whereas disease activity appears maximal early in life with no subsequent peaks in males, both menarche and pregnancy appear associated with disease onset or worsening in females. This suggests that hormonal changes may be a modulating factor. © 2020 The Authors. Annals of Clinical and Translational Neurology published by Wiley Periodicals LLC on behalf of American Neurological Association This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

Published

2020

13. Novel imaging findings in pyruvate dehydrogenase complex (PDHc) deficiency-Results from a nationwide population-based study

Author

Antri Savvidou, Liz Ivarsson, Karin Naess, Erik A. Eklund, Johan Lundgren, Maria Dahlin, Deborah Frithiof, Kalliopi Sofou, and Niklas Darin

Subjects

Male, leukoencephalopathy, Leigh-like lesions, Neurologi, Brain, Pyruvate Dehydrogenase Complex, pyruvate dehydrogenase complex deficiency, Magnetic Resonance Imaging, Stroke, Neurology, Leukoencephalopathies, Pregnancy, stroke-like lesions, Genetics, magnetic resonance imaging, Humans, Female, Pyruvate Dehydrogenase (Lipoamide), Pyruvate Dehydrogenase Complex Deficiency Disease, Genetics (clinical)

Abstract

The vast clinical and radiological spectrum of pyruvate dehydrogenase complex (PDHc) deficiency continues to pose challenges both in diagnostics and disease monitoring. Prompt diagnosis is important to enable early initiation of ketogenic diet. The patients were recruited from an ongoing population-based study in Sweden. All patients with a genetically confirmed diagnosis who had been investigated with an MRI of the brain were included. Repeated investigations were assessed to study the evolution of the MRI changes. Sixty-two MRI investigations had been performed in 34 patients (23 females). The genetic cause was mutations in PDHA1 in 29, PDHX and DLAT in 2 each, and PDHB in 1. The lesions were prenatal developmental in 16, prenatal clastic in 18, and postnatal clastic in 15 individuals. Leigh-like lesions with predominant involvement of globus pallidus were present in 12, while leukoencephalopathy was present in 6 and stroke-like lesions in 3 individuals. A combination of prenatal developmental and clastic lesions was present in 15 individuals. In addition, one male with PDHA1 also had postnatal clastic lesions. The most common lesions found in our study were agenesis or hypoplasia of corpus callosum, ventriculomegaly, or Leigh-like lesions. Furthermore, we describe a broad spectrum of other MRI changes that include leukoencephalopathy and stroke-like lesions. We argue that a novel important clue, suggesting the possibility of PDHc deficiency on MRI scans, is the simultaneous presence of multiple lesions on MRI that have occurred during different phases of brain development.

Published

2021

14. Segmental and total uniparental isodisomy (UPiD) as a disease mechanism in autosomal recessive lysosomal disorders

Author

Clara Sá Miranda, Lies H. Hoefsloot, Karin Naess, Galhana M. Somers-Bolman, Ineke Labrijn-Marks, Irene Mavridou, Trijnie Dijkhuizen, Jasper J. Saris, Marianne Hoogeveen-Westerveld, Ans T. van der Ploeg, Frans W. Verheijen, Olga Amaral, Sirpa Ala-Mello, Hannerieke J. M. P. van den Hout, Dicky J. Halley, Helen Michelakakis, Stijn L.M. in 't Groen, W.W.M. Pim Pijnappel, Marloes Benjamins, M. A. Kroos, Department of Medical and Clinical Genetics, Medicum, Helsinki University Hospital Area, Clinical Genetics, and Pediatrics

Subjects

Male, Genetic testing, Mucopolysaccharidosis I, Genotype, Medicine, DISOMY, HOMOZYGOSITY, Child, 10. No inequality, Genetics (clinical), Genetics, 0303 health sciences, Disease genetics, Glycogen Storage Disease Type II, Medical genetics, 030305 genetics & heredity, 1184 Genetics, developmental biology, physiology, Uniparental disomy, 3. Good health, SNP genotyping, Chromosome 17 (human), Child, Preschool, Female, Adolescent, Genetic Diagnosis, Genética Humana, MOSAICISM, Polymorphism, Single Nucleotide, PATIENT, Article, 03 medical and health sciences, Mucopolysaccharidosis type I, Humans, SNP, CYSTIC-FIBROSIS, business.industry, DELETION, Laboratory techniques and procedures, Infant, Human Genetics, Uniparental Disomy, medicine.disease, GENE, Human genetics, Doenças Genéticas, Uniparental Isodisomy, Lysiosomal Diseases, 1182 Biochemistry, cell and molecular biology, 3111 Biomedicine, business

Abstract

Collaboration from previous work institution. Free PMC article: https://www.ncbi.nlm.nih.gov/pmc/articles/pmid/30737479/ Analyses in our diagnostic DNA laboratory include genes involved in autosomal recessive (AR) lysosomal storage disorders such as glycogenosis type II (Pompe disease) and mucopolysaccharidosis type I (MPSI, Hurler disease). We encountered 4 cases with apparent homozygosity for a disease-causing sequence variant that could be traced to one parent only. In addition, in a young child with cardiomyopathy, in the absence of other symptoms, a diagnosis of Pompe disease was considered. Remarkably, he presented with different enzymatic and genotypic features between leukocytes and skin fibroblasts. All cases were examined with microsatellite markers and SNP genotyping arrays. We identified one case of total uniparental disomy (UPD) of chromosome 17 leading to Pompe disease and three cases of segmental uniparental isodisomy (UPiD) causing Hurler-(4p) or Pompe disease (17q). One Pompe patient with unusual combinations of features was shown to have a mosaic segmental UPiD of chromosome 17q. The chromosome 17 UPD cases amount to 11% of our diagnostic cohort of homozygous Pompe patients (plus one case of pseudoheterozygosity) where segregation analysis was possible. We conclude that inclusion of parental DNA is mandatory for reliable DNA diagnostics. Mild or unusual phenotypes of AR diseases should alert physicians to the possibility of mosaic segmental UPiD. SNP genotyping arrays are used in diagnostic workup of patients with developmental delay. Our results show that even small Regions of Homozygosity that include telomeric areas are worth reporting, regardless of the imprinting status of the chromosome, as they might indicate segmental UPiD. info:eu-repo/semantics/publishedVersion

Published

2019

15. Integration of whole genome sequencing into a healthcare setting: high diagnostic rates across multiple clinical entities in 3219 rare disease patients

Author

Tommy Stödberg, Magnus Nordenskjöld, Emma Tham, Virpi Töhönen, Karin Naess, Bianca Tesi, Eliane Sardh, Erik Björck, Martin Engvall, Helena Malmgren, Josephine Wincent, Adam Rosenbaum, Peter Gustavsson, Sofie Vonlanthen, Anders Jemt, Måns Magnusson, Helene Bruhn, Anna Wredenberg, Mikael Oscarson, Sofia Ygberg, Kristina Lagerstedt-Robinson, Erik Iwarsson, Carolina Backman Johansson, Christoph Freyer, Michela Barbaro, Ellika Sahlin, Henrik Stranneheim, Anna Lindstrand, Anna Wedell, Ann Nordgren, Ulrika von Döbeln, Britt-Marie Anderlid, Mikael Laaksonen, Maria Pettersson, Henrik Arnell, Nicole Lesko, Rolf Zetterström, Chiara Rasi, Ann-Charlotte Wikström, Malin Kvarnung, Valtteri Wirta, Sara Lind Enoksson, Giedre Grigelioniene, Maria Johansson Soller, Anna Hammarsjö, Ola Winqvist, Daphne Vassiliou, Håkan Thonberg, Per Marits, Jesper Eisfeldt, Daniel Nilsson, and Maritta Hellström-Pigg

Subjects

medicine.medical_specialty, lcsh:QH426-470, DNA Copy Number Variations, Inheritance Patterns, lcsh:Medicine, Genomics, Disease, Cohort Studies, Genetic Heterogeneity, Rare Diseases, Internal medicine, Genetics, medicine, Humans, Medical diagnosis, Indel, Monogenic disease, Molecular Biology, Genetics (clinical), Whole genome sequencing, Sweden, Whole Genome Sequencing, business.industry, Information Dissemination, Research, lcsh:R, High-Throughput Nucleotide Sequencing, Uniparental Disomy, medicine.disease, Human genetics, Uniparental disomy, Single nucleotide variant, lcsh:Genetics, Clinical diagnostics, Mutation, Molecular Medicine, business, Delivery of Health Care, Rare disease, Microsatellite Repeats

Abstract

Background We report the findings from 4437 individuals (3219 patients and 1218 relatives) who have been analyzed by whole genome sequencing (WGS) at the Genomic Medicine Center Karolinska-Rare Diseases (GMCK-RD) since mid-2015. GMCK-RD represents a long-term collaborative initiative between Karolinska University Hospital and Science for Life Laboratory to establish advanced, genomics-based diagnostics in the Stockholm healthcare setting. Methods Our analysis covers detection and interpretation of SNVs, INDELs, uniparental disomy, CNVs, balanced structural variants, and short tandem repeat expansions. Visualization of results for clinical interpretation is carried out in Scout—a custom-developed decision support system. Results from both singleton (84%) and trio/family (16%) analyses are reported. Variant interpretation is done by 15 expert teams at the hospital involving staff from three clinics. For patients with complex phenotypes, data is shared between the teams. Results Overall, 40% of the patients received a molecular diagnosis ranging from 19 to 54% for specific disease groups. There was heterogeneity regarding causative genes (n = 754) with some of the most common ones being COL2A1 (n = 12; skeletal dysplasia), SCN1A (n = 8; epilepsy), and TNFRSF13B (n = 4; inborn errors of immunity). Some causative variants were recurrent, including previously known founder mutations, some novel mutations, and recurrent de novo mutations. Overall, GMCK-RD has resulted in a large number of patients receiving specific molecular diagnoses. Furthermore, negative cases have been included in research studies that have resulted in the discovery of 17 published, novel disease-causing genes. To facilitate the discovery of new disease genes, GMCK-RD has joined international data sharing initiatives, including ClinVar, UDNI, Beacon, and MatchMaker Exchange. Conclusions Clinical WGS at GMCK-RD has provided molecular diagnoses to over 1200 individuals with a broad range of rare diseases. Consolidation and spread of this clinical-academic partnership will enable large-scale national collaboration.

Published

2021

16. An international classification of inherited metabolic disorders (ICIMD)

Author

Ferreira C. R., Rahman S., Keller M., Zschocke J., ICIMD Advisory Group: Jose Abdenur, Houda Ali, Rafael Artuch, Andrea Ballabio, Bruce Barshop, Matthias Baumgartner, Enrico Silvio Bertini, Nenad Blau, Valerio Carelli, Christopher Carroll, Patrick F Chinnery, John Christodoulou, Veronica Cornejo, Niklas Darin, Terry Derks, Daria Diodato, Carlo Dionisi-Vici, John A Duley, Toshi Fukao, Ángeles García-Cazorla, Roberto Giugliani, Amy Goldstein, Georg Hoffmann, Rita Horvath, Isabel Ibarra, Anita Inwood, Jaak Jaeken, Cecilia Jimenez-Mallebrera, Amel Karaa, Thomas Klopstock, Stefan Kölker, Cornelia Kornblum, Viktor Kožich, Costanza Lamperti, Nils-Göran Larsson, Aida Lemes, Barry Lewis, Michelangelo Mancuso, Robert McFarland, Fanny Mochel, Julio Montoya, Eva Morava, Karin Naess, Torayuki Okuyama, Annie Olry, Veronique Paquis-Flucklinger, Sumit Parikh, Marc Patterson, Ceila Pérez de Ferrán, Verena Peters, Holger Prokisch, Ann Saada, Gajja S Salomons, Jean-Marie Saudubray, Maurizio Scarpa, Ulrike Schara-Schmidt, Manuel Schiff, Serenella Servidei, Jan Smeitink, Anu Suomalainen, Trine Tangeraas, Robert W Taylor, Ines Thiele, David Thorburn, Johan Van Hove, Ans T Van der Ploeg, Clara Van Karnebeek, Gepke Visser, Jerry Vockley, Ronald Wanders, Dianne Webster, Anna Wedell, Veronica Wiley, Anna Wredenberg, Massimo Zeviani, C. R., Ferreira, S., Rahman, M., Keller, J., Zschocke, Advisory Group: Jose Abdenur, Icimd, Ali, Houda, Artuch, Rafael, Ballabio, Andrea, Barshop, Bruce, Baumgartner, Matthia, Silvio Bertini, Enrico, Blau, Nenad, Carelli, Valerio, Carroll, Christopher, F Chinnery, Patrick, Christodoulou, John, Cornejo, Veronica, Darin, Nikla, Derks, Terry, Diodato, Daria, Dionisi-Vici, Carlo, A Duley, John, Fukao, Toshi, García-Cazorla, Ángele, Giugliani, Roberto, Goldstein, Amy, Hoffmann, Georg, Horvath, Rita, Ibarra, Isabel, Inwood, Anita, Jaeken, Jaak, Jimenez-Mallebrera, Cecilia, Karaa, Amel, Klopstock, Thoma, Kölker, Stefan, Kornblum, Cornelia, Kožich, Viktor, Lamperti, Costanza, Larsson, Nils-Göran, Lemes, Aida, Lewis, Barry, Mancuso, Michelangelo, Mcfarland, Robert, Mochel, Fanny, Montoya, Julio, Morava, Eva, Naess, Karin, Okuyama, Torayuki, Olry, Annie, Paquis-Flucklinger, Veronique, Parikh, Sumit, Patterson, Marc, Pérez de Ferrán, Ceila, Peters, Verena, Prokisch, Holger, Saada, Ann, S Salomons, Gajja, Saudubray, Jean-Marie, Scarpa, Maurizio, Schara-Schmidt, Ulrike, Schiff, Manuel, Servidei, Serenella, Smeitink, Jan, Suomalainen, Anu, Tangeraas, Trine, W Taylor, Robert, Thiele, Ine, Thorburn, David, Van Hove, Johan, T Van der Ploeg, An, Van Karnebeek, Clara, Visser, Gepke, Vockley, Jerry, Wanders, Ronald, Webster, Dianne, Wedell, Anna, Wiley, Veronica, Wredenberg, Anna, Zeviani, Massimo, University of Zurich, Ferreira C.R., Rahman S., Keller M., Zschocke J., ICIMD Advisory Group, and Carelli V.

Subjects

Nosology, medicine.medical_specialty, 2716 Genetics (clinical), Expert advice, 610 Medicine & health, Genetic Condition, Article, ICIMD, 03 medical and health sciences, 1311 Genetics, International Classification of Diseases, Genetics, Humans, Relevance (law), Medicine, ontology, Intensive care medicine, Genetics (clinical), 030304 developmental biology, 0303 health sciences, Mechanism (biology), business.industry, 030305 genetics & heredity, inherited metabolic disorder, classification, inherited metabolic disorders, 10036 Medical Clinic, Metabolism, Inborn Error, business, Metabolism, Inborn Errors, Human

Abstract

Several initiatives at establishing a classification of inherited metabolic disorders have been published previously, some focusing on pathomechanisms, others on clinical manifestations, while yet another attempted a simplified approach of a comprehensive nosology. Some of these classifications suffered from shortcomings, such as lack of a mechanism for continuous update in light of a rapidly evolving field, or lack of widespread input from the metabolic community at large. Our classification-the International Classification of Inherited Metabolic Disorders, or International Classification of Inborn Metabolic Disorders (ICIMD)-includes 1450 disorders, and differs from prior approaches in that it benefited from input by a large number of experts in the field, and was endorsed by major metabolic societies around the globe. Several criteria such as pathway involvement and pathomechanisms were considered. The main purpose of the hierarchical, group-based approach of the ICIMD is an improved understanding of the interconnections between many individual conditions that may share functional, clinical, and diagnostic features. The ICIMD aims to include any primary genetic condition in which alteration of a biochemical pathway is intrinsic to specific biochemical, clinical, and/or pathophysiological features. As new disorders are discovered, we will seek the opinion of experts in the advisory board prior to inclusion in the appropriate group of the ICIMD, thus guaranteeing the continuing relevance of this classification via regular curation and expert advice.

Published

2021

17. Expanded Screening of One Million Swedish Babies with R4S and CLIR for Post-Analytical Evaluation of Data

Author

Carolina Backman-Johansson, Rolf Zetterström, Martin Engvall, Anna Wedell, Henrik Åhlman, Yvonne Nordqvist, Annika Ohlsson, Ulrika von Döbeln, Lene Sörensen, and Karin Naess

Subjects

0301 basic medicine, Pediatrics, medicine.medical_specialty, 030105 genetics & heredity, Article, post-analytical evaluation, 03 medical and health sciences, Immunology and Microbiology (miscellaneous), tandem mass spectrometry, Medicine, dried blood spots (DBS), Newborn screening, biology, business.industry, newborn screening, Incidence (epidemiology), positive predictive value (PPV), lcsh:RJ1-570, Obstetrics and Gynecology, lcsh:Pediatrics, Stork, Collaborative Laboratory Integrated Reports (CLIR), biology.organism_classification, Predictive value, 030104 developmental biology, Methylmalonic aciduria, Pediatrics, Perinatology and Child Health, business, expanded screening

Abstract

Sweden has one neonatal screening laboratory, receiving 115 to 120 thousand samples per year. Among the one million babies screened by tandem mass spectrometry from November 2010 until July 2019, a total of 665 babies were recalled and 311 verified as having one of the diseases screened for with this methodology, giving a positive predictive value (PPV) of 47% and an incidence of 1:3200. The PPV was high (41%) already in the first year after start of screening, thanks to the availability of the collaborative project Region 4 Stork database. The PPV is presently 58%. This improvement was achieved by the implementation of second-tier analyses in the screening for methylmalonic aciduria, propionic aciduria, isovaleric aciduria, and homocystinuria, and the employment of various post analytical tools of the Region 4 Stork, and its successor the collaborative laboratory integrated reports.

Published

2020

18. Clinical Presentation, Genetic Etiology, and Coenzyme Q10 Levels in 55 Children with Combined Enzyme Deficiencies of the Mitochondrial Respiratory Chain

Author

Henrik Stranneheim, Arnaud Mourier, Rolf Wibom, Anna Wredenberg, Karin Naess, Anna Wedell, Nicole Lesko, Ulrika von Döbeln, Martin Engvall, Helene Bruhn, Inger Nennesmo, Christoph Freyer, Institut de biochimie et génétique cellulaires (IBGC), and Université Bordeaux Segalen - Bordeaux 2-Centre National de la Recherche Scientifique (CNRS)

Subjects

Adult, Mitochondrial DNA, Mitochondrial Diseases, Adolescent, Ubiquinone, DNA Mutational Analysis, Respiratory chain, Disease, [SDV.BC.BC]Life Sciences [q-bio]/Cellular Biology/Subcellular Processes [q-bio.SC], Bioinformatics, DNA, Mitochondrial, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Metabolic Diseases, 030225 pediatrics, Exome Sequencing, Medicine, Humans, 030212 general & internal medicine, Child, Exome sequencing, ComputingMilieux_MISCELLANEOUS, Whole genome sequencing, Massive parallel sequencing, business.industry, Infant, Newborn, Infant, Hypotonia, [SDV.BBM.BC]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biomolecules [q-bio.BM], [SDV.GEN.GA]Life Sciences [q-bio]/Genetics/Animal genetics, Mitochondrial respiratory chain, Child, Preschool, Pediatrics, Perinatology and Child Health, Mutation, medicine.symptom, business

Abstract

Objectives To evaluate the clinical symptoms and biochemical findings and establish the genetic etiology in a cohort of pediatric patients with combined deficiencies of the mitochondrial respiratory chain complexes. Study design Clinical and biochemical data were collected from 55 children. All patients were subjected to sequence analysis of the entire mitochondrial genome, except when the causative mutations had been identified based on the clinical picture. Whole exome sequencing/whole genome sequencing (WES/WGS) was performed in 32 patients. Results Onset of disease was generally early in life (median age, 6 weeks). The most common symptoms were muscle weakness, hypotonia, and developmental delay/intellectual disability. Nonneurologic symptoms were frequent. Disease causing mutations were found in 20 different nuclear genes, and 7 patients had mutations in mitochondrial DNA. Causative variants were found in 18 of the 32 patients subjected to WES/WGS. Interestingly, many patients had low levels of coenzyme Q10 in muscle, irrespective of genetic cause. Conclusions Children with combined enzyme defects display a diversity of clinical symptoms with varying age of presentation. We established the genetic diagnosis in 35 of the 55 patients (64%). The high diagnostic yield was achieved by the introduction of massive parallel sequencing, which also revealed novel genes and enabled elucidation of new disease mechanisms.

Published

2020

19. Simplifying the clinical classification of polymerase gamma (POLG) disease based on age of onset; studies using a cohort of 155 cases

Author

Irenaeus F.M. de Coo, Chantal M. E. Tallaksen, Claus Klingenberg, Omar Hikmat, Eylert Brodtkorb, Shamima Rahman, Leticia Pias-Peleteiro, Niklas Darin, Johanna Uusimaa, Laurence A. Bindoff, Karin Naess, Magnhild Rasmussen, Martin Engvall, Elsebet Ostergaard, Pirjo Isohanni, HUS Children and Adolescents, Research Programs Unit, Anu Wartiovaara / Principal Investigator, Clinicum, Children's Hospital, Lastenneurologian yksikkö, University of Helsinki, Helsinki University Hospital Area, STEMM - Stem Cells and Metabolism Research Program, Faculty of Medicine, RS: MHeNs - R3 - Neuroscience, and Toxicogenomics

Subjects

Male, Pediatrics, Mitochondrial Diseases, Disease, Compound heterozygosity, Epilepsy, 0302 clinical medicine, Medicine, Age of Onset, Child, Genetics (clinical), Aged, 80 and over, 0303 health sciences, 1184 Genetics, developmental biology, physiology, Middle Aged, DNA Polymerase gamma, 3. Good health, Europe, mitochondrial disease, POLG, Child, Preschool, Cohort, Female, medicine.symptom, Adult, medicine.medical_specialty, Ataxia, Adolescent, Young Adult, 03 medical and health sciences, Genetics, Humans, Genetic Predisposition to Disease, VDP::Medisinske Fag: 700, stroke-like episodes, Aged, Retrospective Studies, 030304 developmental biology, SPECTRUM, business.industry, MUTATIONS, 3112 Neurosciences, Infant, Retrospective cohort study, medicine.disease, Survival Analysis, Alpers syndrome, VDP::Medical disciplines: 700, Peripheral neuropathy, 3121 General medicine, internal medicine and other clinical medicine, Mutation, epilepsy, Age of onset, business, 030217 neurology & neurosurgery, PARKINSONISM

Abstract

Background Variants in POLG are one of the most common causes of inherited mitochondrial disease. Phenotypic classification of POLG disease has evolved haphazardly making it complicated and difficult to implement in everyday clinical practise. The aim of our study was to simplify the classification and facilitate better clinical recognition. Methods A multinational, retrospective study using data from 155 patients with POLG variants recruited from seven European countries. Results We describe the spectrum of clinical features associated with POLG variants in the largest known cohort of patients. While clinical features clearly form a continuum, stratifying patients simply according to age of onset—onset prior to age 12 years; onset between 12 and 40 years and onset after the age of 40 years, permitted us to identify clear phenotypic and prognostic differences. Prior to 12 years of age, liver involvement (87%), seizures (84%), and feeding difficulties (84%) were the major features. For those with onset between 12 and 40 years, ataxia (90%), peripheral neuropathy (84%), and seizures (71%) predominated, while for those with onset over 40 years, ptosis (95%), progressive external ophthalmoplegia (89%), and ataxia (58%) were the major clinical features. The earlier the onset the worse the prognosis. Patients with epilepsy and those with compound heterozygous variants carried significantly worse prognosis. Conclusion Based on our data, we propose a simplified POLG disease classification, which can be used to guide diagnostic investigations and predict disease course. This is an open access article under the terms of the Creative Commons Attribution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

Published

2020

20. Children with mucopolysaccharidosis risk progressive visual dysfunction despite haematopoietic stem cell transplants

Author

Monica Olsson, Jacek Winiarski, Kristina Teär Fahnehjelm, Jürg Hengstler, Karin Naess, and Enping Chen

Subjects

Male, Retinal degeneration, medicine.medical_specialty, Visual acuity, Adolescent, genetic structures, Photophobia, Mucopolysaccharidosis, Vision Disorders, Visual Acuity, Refraction, Ocular, Retina, Cornea, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Ophthalmology, medicine, Humans, Prospective Studies, Child, Hurler syndrome, Prospective cohort study, medicine.diagnostic_test, business.industry, Hematopoietic Stem Cell Transplantation, Infant, General Medicine, Mucopolysaccharidoses, medicine.disease, eye diseases, Strabismus, Haematopoiesis, Eye examination, Child, Preschool, Pediatrics, Perinatology and Child Health, 030221 ophthalmology & optometry, Female, medicine.symptom, business, 030217 neurology & neurosurgery, Follow-Up Studies

Abstract

AIM This prospective study assessed the long-term ocular and visual outcomes of children with mucopolysaccharidoses type I Hurler syndrome (MPS IH) who were treated with haematopoietic stem cell transplants (HSCT). METHODS Clinical ophthalmological assessments were performed on eight patients at the St Erik Eye Hospital, Huddinge, Stockholm, Sweden, from 2001-2018: The median age at diagnosis and HSCT were 12.2 (range 5.0-16.4) and 16.7 (8.0-20.4) months. The last eye examination was at a median of 13.4 (6.3-19.0) years and follow-up lasted a median of 12.0 (5.0-17.4) years. RESULTS Poor visual acuity, poor night vision and, or, photophobia were reported by six children. The best corrected visual acuity at the last visit was a median of 0.4 and 0.5 in the right and left eye and had declined significantly in two patients. Corneal opacities had increased despite HSCT in five patients. High hyperopia, at a median of +6 Dioptres, occurred in all patients and stiff corneas in all four patients that were measured. The patients' corrected intraocular pressures were normal. Retinal degeneration was identified in two patients. CONCLUSION Despite HSCT, the long-term follow-up of patients with MPS IH showed reduced visual acuity due to corneal opacities or retinal degeneration.

Published

2018

21. Phenotype-genotype correlations in Leigh syndrome: new insights from a multicentre study of 96 patients

Author

Mar Tulinius, Niklas Darin, Kalliopi Sofou, Linda De Meirleir, Johanna Uusimaa, Charalampos Tzoulis, Pirjo Isohanni, Karin Naess, Elsebet Ostergaard, Irenaeus F.M. de Coo, Tuula Lönnqvist, Laurence A. Bindoff, Neurology, Reproduction and Genetics, Neurogenetics, Clinical sciences, Research Programme for Molecular Neurology, Research Programs Unit, Anu Wartiovaara / Principal Investigator, Clinicum, Children's Hospital, University of Helsinki, Lastenneurologian yksikkö, and HUS Children and Adolescents

Subjects

0301 basic medicine, Male, Cardiomyopathy, CHILDHOOD, CHILDREN, DNA, Mitochondrial/genetics, 0302 clinical medicine, ENCEPHALOMYOPATHY, 3123 Gynaecology and paediatrics, Leigh Disease/genetics, Genetics (clinical), Genetics, 1184 Genetics, developmental biology, physiology, Phenotype, Cohort, Female, medicine.symptom, Leigh Disease, medicine.medical_specialty, Mitochondrial DNA, Ataxia, DNA ABNORMALITIES, Mutation/genetics, Mitochondrial disease, Biology, DNA/genetics, MITOCHONDRIAL DISEASE, DNA, Mitochondrial, Central nervous system disease, 03 medical and health sciences, Internal medicine, medicine, Humans, Leigh disease, Genetic Association Studies, Cell Nucleus, CARDIOMYOPATHY, Genetic heterogeneity, CLINICAL-FEATURES, 3112 Neurosciences, Infant, DNA, medicine.disease, 030104 developmental biology, NDUFS4 GENE, Mutation, Cell Nucleus/metabolism, COMPLEX-I DEFICIENCY, 030217 neurology & neurosurgery, SURF1 GENE-MUTATIONS, Follow-Up Studies

Abstract

BackgroundLeigh syndrome is a phenotypically and genetically heterogeneous mitochondrial disorder. While some genetic defects are associated with well-described phenotypes, phenotype-genotype correlations in Leigh syndrome are not fully explored.ObjectiveWe aimed to identify phenotype-genotype correlations in Leigh syndrome in a large cohort of systematically evaluated patients.MethodsWe studied 96 patients with genetically confirmed Leigh syndrome diagnosed and followed in eight European centres specialising in mitochondrial diseases.ResultsWe found that ataxia, ophthalmoplegia and cardiomyopathy were more prevalent among patients with mitochondrial DNA defects. Patients with mutations in MT-ND and NDUF genes with complex I deficiency shared common phenotypic features, such as early development of central nervous system disease, followed by high occurrence of cardiac and ocular manifestations. The cerebral cortex was affected in patients with NDUF mutations significantly more often than the rest of the cohort. Patients with the m.8993T>G mutation in MT-ATP6 gene had more severe clinical and radiological manifestations and poorer disease outcome compared with patients with the m.8993T>C mutation.ConclusionOur study provides new insights into phenotype-genotype correlations in Leigh syndrome and particularly in patients with complex I deficiency and with defects in the mitochondrial ATP synthase.

Published

2018

22. Allelic Expression Imbalance Promoting a Mutant PEX6 Allele Causes Zellweger Spectrum Disorder

Author

Aurora Pujol, Karin Naess, Francjan J. van Spronsen, Nancy Braverman, Hans R. Waterham, Ronald J.A. Wanders, Irene M. L. W. Korver-Keularts, Steven J. Steinberg, Kim D. Falkenberg, Martin Engvall, Femke C. C. Klouwer, Montserrat Ruiz, Sacha Ferdinandusse, M. Estela Rubio-Gozalbo, Agatha Schlüter, Ann B. Moser, MUMC+: DA KG Lab Centraal Lab (9), MUMC+: DA CDL Algemeen (9), RS: CARIM - R2.02 - Cardiomyopathy, Afdeling Onderwijs FHML, MUMC+: MA Medische Staf Kindergeneeskunde (9), RS: GROW - R4 - Reproductive and Perinatal Medicine, Kindergeneeskunde, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Graduate School, ARD - Amsterdam Reproduction and Development, Paediatric Neurology, Laboratory Genetic Metabolic Diseases, and Center for Liver, Digestive and Metabolic Diseases (CLDM)

Subjects

Male, 0301 basic medicine, Untranslated region, FIBROBLASTS, Mutant, Allelic Imbalance, Biology, METABOLISM, VARIANTS, Article, Loss of heterozygosity, 03 medical and health sciences, POLYADENYLATION, Transcription (biology), Exome Sequencing, Peroxisomal disorder, Peroxisomes, Genetics, medicine, Humans, Genetic Predisposition to Disease, TRANSCRIPTION, Allele, Zellweger Syndrome, AAA, 3' Untranslated Regions, Alleles, Cells, Cultured, Genetics (clinical), GENE-EXPRESSION, ALTERNATIVE CLEAVAGE, PEROXISOME BIOGENESIS DISORDERS, MUTATIONS, medicine.disease, 030104 developmental biology, Gene Expression Regulation, ATPases Associated with Diverse Cellular Activities, Female, PEX1, PEX6

Abstract

Zellweger spectrum disorders (ZSDs) are autosomal-recessive disorders that are caused by defects in peroxisome biogenesis due to bi-allelic mutations in any of 13 different PEX genes. Here, we identified seven unrelated individuals affected with an apparent dominant ZSD in whom a heterozygous mutant PEX6 allele (c.2578C>T [p.Arg860Trp]) was overrepresented due to allelic expression imbalance (AEI). We demonstrated that AEI of PEX6 is a common phenomenon and is correlated with heterozygosity for a frequent variant in the 3' untranslated region (UTR) of the mutant allele, which disrupts the most distal of two polyadenylation sites. Asymptomatic parents, who were heterozygous for PEX c.2578C>T, did not show AEI and were homozygous for the 3' UTR variant. Overexpression models confirmed that the overrepresentation of the pathogenic PEX6 c.2578T variant compared to wild-type PEX6 c.2578C results in a peroxisome biogenesis defect and thus constitutes the cause of disease in the affected individuals. AEI promoting the overrepresentation of a mutant allele might also play a role in other autosomal-recessive disorders, in which only one heterozygous pathogenic variant is identified.

Published

2017

23. Rescue of primary ubiquinone deficiency due to a novelCOQ7defect using 2,4–dihydroxybensoic acid

Author

Rolf Wibom, Camilla Maffezzini, Måns Magnusson, Helene Bruhn, Nicole Lesko, Arnaud Mourier, Ulrika von Döbeln, Andrea Felser, Henrik Stranneheim, Christoph Freyer, Michela Barbaro, Yvonne Hinze, Robin Andeer, Rolf Zetterström, Martin Engvall, Anna Wedell, Karin Naess, and Anna Wredenberg

Subjects

Male, Mitochondrial Diseases, Ubiquinone, DNA Mutational Analysis, Molecular Sequence Data, Mutation, Missense, Metabolic disorders, Therapeutics, Mitochondrion, medicine.disease_cause, Cofactor, Tandem Mass Spectrometry, Hydroxybenzoates, Genetics, medicine, COQ7, Humans, Missense mutation, Exome, Amino Acid Sequence, Molecular genetics, Child, Genetics (clinical), Exome sequencing, Mutation, Muscle Weakness, biology, Homozygote, Infant, Newborn, Molecular biology, Mitochondria, Biochemistry, Child, Preschool, Coenzyme Q – cytochrome c reductase, biology.protein, Ataxia, Sequence Alignment, Chromatography, Liquid

Abstract

BACKGROUND: Coenzyme Q is an essential mitochondrial electron carrier, redox cofactor and a potent antioxidant in the majority of cellular membranes. Coenzyme Q deficiency has been associated with a range of metabolic diseases, as well as with some drug treatments and ageing. METHODS: We used whole exome sequencing (WES) to investigate patients with inherited metabolic diseases and applied a novel ultra-pressure liquid chromatography-mass spectrometry approach to measure coenzyme Q in patient samples. RESULTS: We identified a homozygous missense mutation in the COQ7 gene in a patient with complex mitochondrial deficiency, resulting in severely reduced coenzyme Q levels We demonstrate that the coenzyme Q analogue 2,4-dihydroxybensoic acid (2,4DHB) was able to specifically bypass the COQ7 deficiency, increase cellular coenzyme Q levels and rescue the biochemical defect in patient fibroblasts. CONCLUSION: We report the first patient with primary coenzyme Q deficiency due to a homozygous COQ7 mutation and a potentially beneficial treatment using 2,4DHB.

Published

2015

24. Eyes on MEGDEL: Distinctive Basal Ganglia Involvement in Dystonia Deafness Syndrome

Author

Manuel Schiff, Nicole I. Wolf, Ron A. Wevers, Lock Hock Ngu, Gilian Riordan, Michèl A.A.P. Willemsen, Ewa Pronicka, Zita Krumina, Ivo Barić, René Santer, Eva Morava, Saskia B. Wortmann, Karin Naess, Linda De Meirleir, Sema Kalkan Uçar, Mahmut Çoker, Friederike Hörster, Tamas Kozicz, Johannes Zschocke, Jan A.M. Smeitink, Peter M. van Hasselt, Alberto Burlina, Mohammed Al-Owain, Evangeline Wassmer, Niklas Darin, Pediatric surgery, NCA - Brain mechanisms in health and disease, Clinical sciences, Reproduction and Genetics, and Neurogenetics

Subjects

Pathology, medicine.medical_specialty, Mitochondrial Diseases, Movement disorders, Encephalopathy, Stress-related disorders Donders Center for Medical Neuroscience [Radboudumc 13], Caudate nucleus, Deafness, Basal Ganglia, Pathognomonic, Basal ganglia, medicine, Humans, business.industry, Putamen, Infant, Metabolic Disorders Radboud Institute for Molecular Life Sciences [Radboudumc 6], Syndrome, General Medicine, 3-Methylglutaconic Aciduria, Disorders of movement Donders Center for Medical Neuroscience [Radboudumc 3], medicine.disease, Magnetic Resonance Imaging, Dystonic Disorders, Child, Preschool, Pediatrics, Perinatology and Child Health, Disease Progression, Neurology (clinical), medicine.symptom, business, Dystonic disorder

Abstract

Contains fulltext : 155252.pdf (Publisher’s version ) (Closed access) Pediatric movement disorders are still a diagnostic challenge, as many patients remain without a (genetic) diagnosis. Magnetic resonance imaging (MRI) pattern recognition can lead to the diagnosis. MEGDEL syndrome (3-MethylGlutaconic aciduria, Deafness, Encephalopathy, Leigh-like syndrome MIM #614739) is a clinically and biochemically highly distinctive dystonia deafness syndrome accompanied by 3-methylglutaconic aciduria, severe developmental delay, and progressive spasticity. Mutations are found in SERAC1, encoding a phosphatidylglycerol remodeling enzyme essential for both mitochondrial function and intracellular cholesterol trafficking. Based on the homogenous phenotype, we hypothesized an accordingly characteristic MRI pattern. A total of 43 complete MRI studies of 30 patients were systematically reevaluated. All patients presented a distinctive brain MRI pattern with five characteristic disease stages affecting the basal ganglia, especially the putamen. In stage 1, T2 signal changes of the pallidum are present. In stage 2, swelling of the putamen and caudate nucleus is seen. The dorsal putamen contains an "eye" that shows no signal alteration and (thus) seems to be spared during this stage of the disease. It later increases, reflecting progressive putaminal involvement. This "eye" was found in all patients with MEGDEL syndrome during a specific age range, and has not been reported in other disorders, making it pathognomonic for MEDGEL and allowing diagnosis based on MRI findings.

Published

2015

25. Partial tetrasomy 14 associated with multiple malformations

Author

Kristina Lagerstedt Robinson, Nicole Lesko, Karin Naess, Agneta Nordenskjöld, Caroline Graff, Agne Liedén, Peter Gustavsson, Johanna Winberg, Ann Nordgren, Britt-Marie Anderlid, and Rolf Wibom

Subjects

Pathology, medicine.medical_specialty, Mitochondrial Diseases, Gastrointestinal Diseases, Cleft Lip, Marker chromosome, In situ hybridization, Biology, Craniosynostoses, Seizures, Intellectual Disability, Genetics, medicine, Humans, Abnormalities, Multiple, Child, Muscle, Skeletal, In Situ Hybridization, Fluorescence, Genetics (clinical), Chromosomes, Human, Pair 14, Sweden, Comparative Genomic Hybridization, Coloboma, Electron Transport Complex I, Muscle biopsy, Models, Genetic, medicine.diagnostic_test, Karyotype, medicine.disease, Mitochondrial respiratory chain, Karyotyping, Tetrasomy, Female, Microsatellite Repeats, Comparative genomic hybridization

Abstract

We report on an 8-year-old female patient with multiple malformations including bilateral cleft lip and palate, coloboma, and craniosynostosis. She presented with severe intellectual disability, seizures, and gastrointestinal dysfunction. Mitochondrial investigations in a muscle biopsy revealed reduced activity in complex I of the mitochondrial respiratory chain. Chromosome analysis and fluorescent in situ hybridization (FISH) studies showed an isodicentric marker chromosome 14 that was identified in all cells analyzed in peripheral blood lymphocytes and cultured fibroblasts. Parental chromosome studies were normal. To further characterize the marker chromosome and determine its origin, we performed array-based comparative genomic hybridization (CGH) and polymorphic marker analysis with quantitative fluorescent PCR (QF-PCR). The combined results from cytogenetic and array-CGH analyses showed tetrasomy 14p13q13.1 and results from the QF-PCR point to formation of the marker chromosome in the maternal meiosis. Isodicentric chromosomes involving partial 14q have previously been reported in four cases; however, this is the first patient with tetrasomy 14p13q13.1 in non-mosaic form surviving beyond infancy.

Published

2013

26. Succinate-CoA ligase deficiency due to mutations in SUCLA2 and SUCLG1: phenotype and genotype correlations in 71 patients

Author

Elisabeth Holme, Rosalba Carrozzo, Andrés Nascimento Osorio, Robert W. Taylor, Carlo Dionisi-Vici, Kirstine Ravn, Hernan Amartino, Duccio Maria Cordelli, Alberto Burlina, Karin Naess, Filippo M. Santorelli, René de Coo, Niklas Darin, Berit Woldseth, Alfred Peter Born, Päivi Vieira, Morten Duno, Flemming Wibrand, Fróði Joensen, Enrico Bertini, Magnhild Rasmussen, Robert McFarland, Daniela Buhas, Gabriela Stangoni, Elsebet Ostergaard, Samir Mesli, Johanna Uusimaa, Marzia Bianchi, Paolo Prontera, Mustafa Batbayli, Isabelle Redonnet-Vernhet, Mar Tulinius, Daniela Verrigni, Philippe Jouvencel, Neurology, Carrozzo, Rosalba, Verrigni, Daniela, Rasmussen, Magnhild, de Coo, Rene, Amartino, Hernan, Bianchi, Marzia, Buhas, Daniela, Mesli, Samir, Naess, Karin, Born, Alfred Peter, Woldseth, Berit, Prontera, Paolo, Batbayli, Mustafa, Ravn, Kirstine, Joensen, Fróði, Cordelli, Duccio M., Santorelli, Filippo Maria, Tulinius, Mar, Darin, Nikla, Duno, Morten, Jouvencel, Philippe, Burlina, Alberto, Stangoni, Gabriela, Bertini, Enrico, Redonnet-Vernhet, Isabelle, Wibrand, Flemming, Dionisi-Vici, Carlo, Uusimaa, Johanna, Vieira, Paivi, Osorio, Andrés Nascimento, McFarland, Robert, Taylor, Robert W., Holme, Elisabeth, and Ostergaard, Elsebet

Subjects

Male, 0301 basic medicine, Mitochondrial Diseases, SUCLA2, DNA Mutational Analysis, Methylmalonic acid, Bioinformatics, Gastroenterology, Mitochondrial Encephalomyopathie, chemistry.chemical_compound, Succinate-CoA Ligases, Gene duplication, Genotype, Mitochondrial Disease, Missense mutation, Child, Genetics (clinical), education.field_of_study, Amino Acid Metabolism, Inborn Error, Phenotype, Codon, Nonsense, Child, Preschool, Female, Human, Adult, medicine.medical_specialty, Adolescent, Nonsense mutation, Population, Mutation, Missense, DNA, Mitochondrial, DNA Mutational Analysi, Young Adult, 03 medical and health sciences, Genetic, Mitochondrial Encephalomyopathies, Internal medicine, Genetics, medicine, Humans, Amino Acid Sequence, education, Amino Acid Metabolism, Inborn Errors, Succinate-CoA Ligase, business.industry, Infant, Newborn, Infant, 030104 developmental biology, Methylmalonic aciduria, chemistry, business, Methylmalonic Acid

Abstract

Background: The encephalomyopathic mtDNA depletion syndrome with methylmalonic aciduria is associated with deficiency of succinate-CoA ligase, caused by mutations in SUCLA2 or SUCLG1. We report here 25 new patients with succinate-CoA ligase deficiency, and review the clinical and molecular findings in these and 46 previously reported patients. Patients and results: Of the 71 patients, 50 had SUCLA2 mutations and 21 had SUCLG1 mutations. In the newly-reported 20 SUCLA2 patients we found 16 different mutations, of which nine were novel: two large gene deletions, a 1 bp duplication, two 1 bp deletions, a 3 bp insertion, a nonsense mutation and two missense mutations. In the newly-reported SUCLG1 patients, five missense mutations were identified, of which two were novel. The median onset of symptoms was two months for patients with SUCLA2 mutations and at birth for SUCLG1 patients. Median survival was 20 years for SUCLA2 and 20 months for SUCLG1. Notable clinical differences between the two groups were hepatopathy, found in 38 % of SUCLG1 cases but not in SUCLA2 cases, and hypertrophic cardiomyopathy which was not reported in SUCLA2 patients, but documented in 14 % of cases with SUCLG1 mutations. Long survival, to age 20 years or older, was reported in 12 % of SUCLA2 and in 10 % of SUCLG1 patients. The most frequent abnormality on neuroimaging was basal ganglia involvement, found in 69 % of SUCLA2 and 80 % of SUCLG1 patients. Analysis of respiratory chain enzyme activities in muscle generally showed a combined deficiency of complexes I and IV, but normal histological and biochemical findings in muscle did not preclude a diagnosis of succinate-CoA ligase deficiency. In five patients, the urinary excretion of methylmalonic acid was only marginally elevated, whereas elevated plasma methylmalonic acid was consistently found. Conclusions: To our knowledge, this is the largest study of patients with SUCLA2 and SUCLG1 deficiency. The most important findings were a significantly longer survival in patients with SUCLA2 mutations compared to SUCLG1 mutations and a trend towards longer survival in patients with missense mutations compared to loss-of-function mutations. Hypertrophic cardiomyopathy and liver involvement was exclusively found in patients with SUCLG1 mutations, whereas epilepsy was much more frequent in patients with SUCLA2 mutations compared to patients with SUCLG1 mutations. The mutation analysis revealed a number of novel mutations, including a homozygous deletion of the entire SUCLA2 gene, and we found evidence of two founder mutations in the Scandinavian population, in addition to the known SUCLA2 founder mutation in the Faroe Islands.

Published

2016

27. MtDNA mutations are a common cause of severe disease phenotypes in children with Leigh syndrome

Author

Karin Naess, Inger Nennesmo, Rolf Wibom, Gunilla Malm, Nils-Göran Larsson, Christoph Freyer, Helene Bruhn, and Ulrika von Döbeln

Subjects

Male, Mitochondrial DNA, Mitochondrial Diseases, Paediatric disease, Mitochondrial disease, Genetic counseling, Biophysics, Respiratory chain, Neurologic disease/disorder, DNA-Directed DNA Polymerase, Encephalopathy, Biology, DNA, Mitochondrial, Polymorphism, Single Nucleotide, Severity of Illness Index, Biochemistry, Genetic analysis, Mitochondrial Proteins, Adenosine Triphosphate, Glutamate Dehydrogenase, medicine, Humans, SURF1, Child, Gene, Genetics, Infant, Newborn, Infant, Membrane Proteins, Cell Biology, medicine.disease, Survival Analysis, Leigh syndrome, DNA Polymerase gamma, Mitochondrial disorder, Kinetics, Phenotype, Child, Preschool, Female, Leigh Disease, Age of onset, Polymorphism, Restriction Fragment Length

Abstract

Leigh syndrome is a common clinical manifestation in children with mitochondrial disease and other types of inborn errors of metabolism. We characterised clinical symptoms, prognosis, respiratory chain function and performed extensive genetic analysis of 25 Swedish children suffering from Leigh syndrome with the aim to obtain insights into the molecular pathophysiology and to provide a rationale for genetic counselling. We reviewed the clinical history of all patients and used muscle biopsies in order to perform molecular, biochemical and genetic investigations, including sequencing the entire mitochondrial DNA (mtDNA), the mitochondrial DNA polymerase (POLGA) gene and the surfeit locus protein 1 (SURF1) gene. Respiratory chain enzyme activity measurements identified five patients with isolated complex I deficiency and five with combined enzyme deficiencies. No patient presented with isolated complex IV deficiency. Seven patients had a decreased ATP production rate. Extensive sequence analysis identified eight patients with pathogenic mtDNA mutations and one patient with mutations in POLGA. Mutations of mtDNA are a common cause of LS and mtDNA analysis should always be included in the diagnosis of LS patients, whereas SURF1 mutations are not a common cause of LS in Sweden. Unexpectedly, age of onset, clinical symptoms and prognosis did not reveal any clear differences in LS patients with mtDNA or nuclear DNA mutations.

Published

2009

28. Outcome in six children with mucopolysaccharidosis type IH, hurler syndrome, after haematopoietic stem cell transplantation (HSCT)

Author

Gunilla Malm, Britt Gustafsson, Birgit Borgström, Gunilla Berglund, Karin Naess, Olle Ringdén, Maria Lindström, and Ulrika von Döbeln

Subjects

Male, medicine.medical_specialty, Pediatrics, Time Factors, Genotype, Mucopolysaccharidosis I, Mucopolysaccharidosis, Chimerism, Mucopolysaccharidosis type I, Humans, Point Mutation, Medicine, Child, Hurler syndrome, Sweden, business.industry, Hematopoietic Stem Cell Transplantation, Infant, General Medicine, Enzyme replacement therapy, medicine.disease, Surgery, Transplantation, Haematopoiesis, Early Diagnosis, Hyperopia, medicine.anatomical_structure, Child, Preschool, Pediatrics, Perinatology and Child Health, Female, Bone marrow, Stem cell, Cognition Disorders, business

Abstract

Aim: To follow-up six children with severe mucopolysaccharidosis type IH, Hurler syndrome, who were treated before 24 months of age with haematopoietic stem cell transplantation. Methods: In Sweden, during the last 10-year period, six consecutive children born with severe mucopolysaccharidoses type IH have been successfully transplanted using matched unrelated donors between the ages of 11 and 24 months (mean age 18 months). Three children received intravenous enzyme replacement therapy once a week, from diagnosis until engraftment of their bone marrow. Result: Two children developed chimerism and a progressive increase in recipient cells and later received a successful re-transplantation. One to two years after transplantation the children demonstrated some developmental delays in cognitive function. Latterly this was followed by normalization. Orthopaedic operations on the spine and hips and carpal tunnel syndrome were still required following transplantation. Cardiac valve involvement remained progressive in the children. Conclusion: The outcome of six children in this study confirms that early haematopoietic stem cell transplantation in mucopolysaccharidosis type I, Hurler syndrome, preserves an affected child's mental ability. Consequently, it is essential that clinical recognition and early diagnosis take place, providing an additional challenge to paediatricians treating this condition.

Published

2008

29. Cyclophilin D, a target for counteracting skeletal muscle dysfunction in mitochondrial myopathy

Author

Anna Wedell, Daniel C. Andersson, Mattias Carlström, Andrés Hernández, Arthur J. Cheng, Nicole Lesko, Anna Wredenberg, Shi-Jin Zhang, Christoph Freyer, Charlotte Gineste, Niklas Ivarsson, Johanna T. Lanner, Karin Naess, Håkan Westerblad, Joseph D. Bruton, Helene Bruhn, and Rolf Wibom

Subjects

medicine.medical_specialty, Mitochondrial disease, Biology, Mitochondrion, DNA, Mitochondrial, Cyclophilins, Mice, Mitochondrial myopathy, Internal medicine, Genetics, medicine, Animals, Humans, Myopathy, Muscle, Skeletal, Molecular Biology, Genetics (clinical), Peptidylprolyl isomerase, Mice, Knockout, Skeletal muscle, Muscle weakness, Mitochondrial Myopathies, General Medicine, Articles, TFAM, medicine.disease, Mitochondria, Disease Models, Animal, medicine.anatomical_structure, Endocrinology, Biochemistry, Gene Expression Regulation, Mutation, Cyclosporine, Calcium, medicine.symptom, Cyclophilin D

Abstract

Muscle weakness and exercise intolerance are hallmark symptoms in mitochondrial disorders. Little is known about the mechanisms leading to impaired skeletal muscle function and ultimately muscle weakness in these patients. In a mouse model of lethal mitochondrial myopathy, the muscle-specific Tfam knock-out (KO) mouse, we previously demonstrated an excessive mitochondrial Ca(2+) uptake in isolated muscle fibers that could be inhibited by the cyclophilin D (CypD) inhibitor, cyclosporine A (CsA). Here we show that the Tfam KO mice have increased CypD levels, and we demonstrate that this increase is a common feature in patients with mitochondrial myopathy. We tested the effect of CsA treatment on Tfam KO mice during the transition from a mild to terminal myopathy. CsA treatment counteracted the development of muscle weakness and improved muscle fiber Ca(2+) handling. Importantly, CsA treatment prolonged the lifespan of these muscle-specific Tfam KO mice. These results demonstrate that CsA treatment is an efficient therapeutic strategy to slow the development of severe mitochondrial myopathy.

Published

2015

30. Biotin and Thiamine Responsive Basal Ganglia Disease--A vital differential diagnosis in infants with severe encephalopathy

Author

Chen Wang, Henrik Stranneheim, Karin Naess, Sofia Ygberg, Mats Eriksson, Rolf Wibom, Nicole Lesko, Ronny Wickström, Anna Wedell, and Michela Barbaro

Subjects

0301 basic medicine, Male, Pediatrics, medicine.medical_specialty, Heterozygote, Encephalopathy, Physiology, Biotin, Compound heterozygosity, White People, Diagnosis, Differential, 03 medical and health sciences, 0302 clinical medicine, Basal Ganglia Diseases, Basal ganglia, medicine, Humans, Thiamine, Sibling, Basal ganglia disease, biology, business.industry, Siblings, Infant, Newborn, Infant, Membrane Transport Proteins, General Medicine, medicine.disease, Magnetic Resonance Imaging, 030104 developmental biology, Pediatrics, Perinatology and Child Health, SLC19A3, Mutation, Vitamin B Complex, biology.protein, Neurology (clinical), Differential diagnosis, business, 030217 neurology & neurosurgery

Abstract

We report two siblings of Swedish origin with infantile Biotin and Thiamine Responsive Basal Ganglia Disease (BTRBG). Case report Initial symptoms were in both cases lethargia, with reduced contact and poor feeding from the age of 5 weeks. Magnetic resonance imaging showed altered signal in the basal ganglia, along with grey and white matter abnormalities. The diagnosis BTRBG was not recognized in the first sibling who died at the age of 8 weeks. The second sibling was started on biotin and thiamine immediately upon development of symptoms, leading to clinical improvement and partial reversion of the magnetic resonance imaging findings. Genetic analysis of the SLC19A3 gene identified two mutations, c.74dupT and c.1403delA, carried in compound heterozygous form in both boys, each inherited from one parent. Comments The first mutation has previously been described in children with BTRBG, and the second mutation is novel. Although the clinical picture in BTRGB is very severe it is also rather unspecific and the diagnosis may be missed. Conclusion This report highlights the importance of considering biotin and thiamine treatment also in a European infant born to non-consanguineous parents, who presents with symptoms of acute/subacute encephalopathy.

Published

2015

31. Intra-mitochondrial Methylation Deficiency Due to Mutations in SLC25A26

Author

Paul Govaert, Yoshihito Kishita, Lut Van Laer, Kei Murayama, Akira Ohtake, Carlo M.T. Marobbio, Helene Bruhn, Aleksandra Pajak, Karin Naess, Arnaud Mourier, Masakazu Kohda, Christoph Freyer, Ferdinando Palmieri, Henrik Stranneheim, Magnus Monné, Anna Wedell, Anna Wredenberg, Nikhita Ajit Bolar, Camilla Maffezzini, Rolf Wibom, Bart Loeys, Daniela Valeria Miniero, Ann Jespers, Yasushi Okazaki, Inger Nennesmo, and Nicole Lesko

Subjects

Male, S-Adenosylmethionine, Mitochondrial Diseases, Amino Acid Transport Systems, Mitochondrial translation, Ubiquinone, RNA Stability, Molecular Sequence Data, Other Research Radboud Institute for Molecular Life Sciences [Radboudumc 0], Mitochondrion, Biology, medicine.disease_cause, chemistry.chemical_compound, Report, mitochondrial dysfunction, Genetics, medicine, Humans, Genetics(clinical), Amino Acid Sequence, SLC25A26, Gene, Genetics (clinical), Mutation, Methionine, Muscle Weakness, Sequence Homology, Amino Acid, Thioctic Acid, Calcium-Binding Proteins, Methylation, DNA Methylation, Prognosis, Molecular biology, Pedigree, mitochondria, SAM, chemistry, Methionine Adenosyltransferase, Child, Preschool, DNA methylation, Female, methylation, Human medicine

Abstract

Contains fulltext : 152388.pdf (Publisher’s version ) (Open Access) S-adenosylmethionine (SAM) is the predominant methyl group donor and has a large spectrum of target substrates. As such, it is essential for nearly all biological methylation reactions. SAM is synthesized by methionine adenosyltransferase from methionine and ATP in the cytoplasm and subsequently distributed throughout the different cellular compartments, including mitochondria, where methylation is mostly required for nucleic-acid modifications and respiratory-chain function. We report a syndrome in three families affected by reduced intra-mitochondrial methylation caused by recessive mutations in the gene encoding the only known mitochondrial SAM transporter, SLC25A26. Clinical findings ranged from neonatal mortality resulting from respiratory insufficiency and hydrops to childhood acute episodes of cardiopulmonary failure and slowly progressive muscle weakness. We show that SLC25A26 mutations cause various mitochondrial defects, including those affecting RNA stability, protein modification, mitochondrial translation, and the biosynthesis of CoQ10 and lipoic acid.

Published

2015

32. Secondary metabolic effects in complex I deficiency

Author

Nils-Göran Larsson, Reetta Hinttala, Karin Naess, Kari Majamaa, Rolf Wibom, Nicole Hance, Nayla Esteitie, Kristina Teär-Fahnehjelm, Helene Nilsson, and Ulrika von Döbeln

Subjects

Adult, Male, Threonine, medicine.medical_specialty, Mitochondrial DNA, Adolescent, Blotting, Western, DNA Mutational Analysis, Respiratory chain, medicine.disease_cause, DNA, Mitochondrial, Models, Biological, chemistry.chemical_compound, Adenosine Triphosphate, Internal medicine, medicine, Humans, Child, Gene, Mutation, Electron Transport Complex I, biology, Succinate dehydrogenase, NADH dehydrogenase, Infant, NADH Dehydrogenase, Citric acid cycle, Endocrinology, Neurology, chemistry, Child, Preschool, biology.protein, Female, Neurology (clinical), Adenosine triphosphate, Metabolism, Inborn Errors

Abstract

The objective of this study was to investigate clinical, biochemical, and genetic features in 7 probands (a total of 11 patients) with nicotine-amide adenine dinucleotide (NADH) dehydrogenase (complex I) deficiency. We screened the mitochondrial DNA for mutations and found pathogenic mutations in complex I genes (mitochondrial NADH dehydrogenase subunit (MTND) genes) in three probands. The 10191T〉C mutation in MTND3 and the 14487T〉C mutation in MTND6 were present in two probands with Leigh's-like and Leigh's syndrome, respectively. Four siblings with a syndrome consisting of encephalomyopathy with hearing impairment, optic nerve atrophy, and cardiac involvement had the 11778G〉A mutation in MTND4, previously associated with Leber hereditary optic neuropathy. These findings demonstrate that mutations in MTND genes are relatively frequent in patients with complex I deficiency. Biochemical measurements of respiratory chain function in muscle mitochondria showed that all patients had a moderate decrease of the mitochondrial adenosine triphosphate production rate. Interestingly, the complex I deficiency caused secondary metabolic alterations with decreased oxaloacetate-induced inhibition of succinate dehydrogenase (complex II) and excretion of Krebs cycle intermediates in the urine. Our results thus suggest that altered regulation of metabolism may play an important role in the pathogenesis of complex I deficiency. Ann Neurol 2005

Published

2005

33. A multicenter study on Leigh syndrome: disease course and predictors of survival

Author

Charalampos Tzoulis, Pirjo Isohanni, Isabell B De Angst, Johanna Uusimaa, Tuula Lönnqvist, Katariina Mankinen, Kalliopi Sofou, Helena Pihko, Karin Naess, Mar Tulinius, Linda De Meirleir, Niklas Darin, Irenaeus F.M. de Coo, Elsebet Ostergaard, Laurence A. Bindoff, Reproduction and Genetics, Pediatrics, Clinical sciences, Neurogenetics, Research Programme for Molecular Neurology, Research Programs Unit, Clinicum, Children's Hospital, Lastenneurologian yksikkö, Lastentautien yksikkö, HUS Children and Adolescents, Neurology, and Urology

Subjects

Male, Pediatrics, Diagnostic criteria, Survival, CHILDHOOD, CHILDREN, 3124 Neurology and psychiatry, 0302 clinical medicine, 3123 Gynaecology and paediatrics, Genotype, Missense mutation, Genetics(clinical), Pharmacology (medical), Relapse, Young adult, Child, MITOCHONDRIAL DISORDERS, Genetics (clinical), Medicine(all), 0303 health sciences, General Medicine, Prognosis, 3. Good health, DEFICIENCY, Natural history, Child, Preschool, Failure to thrive, Female, Leigh Disease, medicine.symptom, Adult, medicine.medical_specialty, DNA ABNORMALITIES, Adolescent, Mitochondrial disease, education, BILATERAL STRIATAL NECROSIS, CASE SERIES, Young Adult, 03 medical and health sciences, MISSENSE MUTATION, progressive neurodegenerative disorder, medicine, Humans, Pathological, Retrospective Studies, 030304 developmental biology, business.industry, Research, CLINICAL-FEATURES, Retrospective cohort study, medicine.disease, Leigh syndrome, mitochondrial oxidative phosphorylation, FOLLOW-UP, business, 030217 neurology & neurosurgery, Survival, Relapse

Abstract

Background: Leigh syndrome is a progressive neurodegenerative disorder, associated with primary or secondary dysfunction of the mitochondrial oxidative phosphorylation. Despite the fact that Leigh syndrome is the most common phenotype of mitochondrial disorders in children, longitudinal natural history data is missing. This study was undertaken to assess the phenotypic and genotypic spectrum of patients with Leigh syndrome, characterise the clinical course and identify predictors of survival in a large cohort of patients. Methods: This is a retrospective study of patients with Leigh syndrome that have been followed at eight centers specialising in mitochondrial diseases in Europe; Gothenburg, Rotterdam, Helsinki, Copenhagen, Stockholm, Brussels, Bergen and Oulu. Results: A total of 130 patients were included (78 males; 52 females), of whom 77 patients had identified pathogenic mutations. The median age of disease onset was 7 months, with 80.8% of patients presenting by the age of 2 years. The most common clinical features were abnormal motor findings, followed by abnormal ocular findings. Epileptic seizures were reported in 40% of patients. Approximately 44% of patients experienced acute exacerbations requiring hospitalisation during the previous year, mainly due to infections. The presence of pathological signs at birth and a history of epileptic seizures were associated with higher occurrence of acute exacerbations and/or relapses. Increased lactate in the cerebrospinal fluid was significantly correlated to a more severe disease course, characterised by early onset before 6 months of age, acute exacerbations and/or relapses, as well as brainstem involvement. 39% of patients had died by the age of 21 years, at a median age of 2.4 years. Disease onset before 6 months of age, failure to thrive, brainstem lesions on neuroimaging and intensive care treatment were significantly associated with poorer survival. Conclusions: This is a multicenter study performed in a large cohort of patients with Leigh syndrome. Our data help define the natural history of Leigh syndrome and identify novel predictors of disease severity and long-term prognosis. publishedVersion

Published

2014

34. Mutations in the phospholipid remodeling gene SERAC1 impair mitochondrial function and intracellular cholesterol trafficking and cause dystonia and deafness

Author

G. Herma Renkema, Sema Kalkan Uçar, Saskia B. Wortmann, Hans van Bokhoven, Jan A.M. Smeitink, Wigard P. Kloosterman, Joachim M. Gerhold, Wim Kulik, Frédéric M. Vaz, Leo A. J. Kluijtmans, Richard J. Rodenburg, Ewa Pronicka, Kapil K Singhal, Johannes N. Spelbrink, Ron A. Wevers, Leo G.J. Nijtmans, Dirk Lefeber, Christian Gilissen, Christine Klein, Joris A. Veltman, Martin Lammens, Anne Grünewald, Peter M. van Hasselt, Tamas Kozicz, Janneke H M Schuurs-Hoeijmakers, Karin Naess, Christin Christin, Thatjana Gardeitchik, Arjan P.M. de Brouwer, Lisenka E.L.M. Vissers, Zita Krumina, Magdalena Harakalova, Eva Morava, Ivo Barić, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, and Laboratory Genetic Metabolic Diseases

Subjects

Mitochondrion, Deafness, medicine.disease_cause, Oxidative Phosphorylation, chemistry.chemical_compound, 0302 clinical medicine, Cardiolipin, Exome, Phospholipids, Cell Line, Transformed, 0303 health sciences, Mutation, Mitochondrial medicine Energy and redox metabolism [IGMD 8], Phosphatidylglycerols, 3-Methylglutaconic Aciduria, Mitochondria, Complementation, Dystonia, Cholesterol, Mitochondrial medicine [IGMD 8], lipids (amino acids, peptides, and proteins), Intracellular, medicine.medical_specialty, Cardiolipins, Molecular Sequence Data, Biology, Filipin, 03 medical and health sciences, exome sequencing, SERAC1 gene, mitochondrial function, dystonia, deafness, Internal medicine, Cell Line, Tumor, Genetics, medicine, Humans, Renal disorder [DCN MP - Plasticity and memory IGMD 9], Amino Acid Sequence, Glycostation disorders [DCN PAC - Perception action and control IGMD 4], DCN NN - Brain networks and neuronal communication, 030304 developmental biology, Endoplasmic reticulum, Fibroblasts, Glycostation disorders [IGMD 4], Molecular biology, Genetics and epigenetic pathways of disease DCN MP - Plasticity and memory [NCMLS 6], Mitochondrial medicine Membrane transport and intracellular motility [IGMD 8], Endocrinology, HEK293 Cells, chemistry, Genetics and epigenetic pathways of disease Genomic disorders and inherited multi-system disorders [NCMLS 6], Carboxylic Ester Hydrolases, Sequence Alignment, 030217 neurology & neurosurgery, HeLa Cells

Abstract

Contains fulltext : 108785.pdf (Publisher’s version ) (Closed access) Using exome sequencing, we identify SERAC1 mutations as the cause of MEGDEL syndrome, a recessive disorder of dystonia and deafness with Leigh-like syndrome, impaired oxidative phosphorylation and 3-methylglutaconic aciduria. We localized SERAC1 at the interface between the mitochondria and the endoplasmic reticulum in the mitochondria-associated membrane fraction that is essential for phospholipid exchange. A phospholipid analysis in patient fibroblasts showed elevated concentrations of phosphatidylglycerol-34:1 (where the species nomenclature denotes the number of carbon atoms in the two acyl chains:number of double bonds in the two acyl groups) and decreased concentrations of phosphatidylglycerol-36:1 species, resulting in an altered cardiolipin subspecies composition. We also detected low concentrations of bis(monoacyl-glycerol)-phosphate, leading to the accumulation of free cholesterol, as shown by abnormal filipin staining. Complementation of patient fibroblasts with wild-type human SERAC1 by lentiviral infection led to a decrease and partial normalization of the mean ratio of phosphatidylglycerol-34:1 to phosphatidylglycerol-36:1. Our data identify SERAC1 as a key player in the phosphatidylglycerol remodeling that is essential for both mitochondrial function and intracellular cholesterol trafficking. 01 juli 2012

Published

2012

35. Complete Deletion of a POLG1 Allele in a Patient with Alpers Syndrome

Author

Michela Barbaro, Ulrika von Döbeln, Karin Naess, Nils-Göran Larsson, Antal Nemeth, Inger Nennesmo, Nicole Lesko, Rolf Wibom, and Helene Bruhn

Subjects

Genetics, Valproic Acid, Mutation, business.industry, Mitochondrial disease, Point mutation, Disease, medicine.disease, Bioinformatics, medicine.disease_cause, Gene dosage, Article, medicine, Multiplex ligation-dependent probe amplification, Allele, business, medicine.drug

Abstract

Mutations in the gene encoding the catalytic subunit of polymerase γ (POLG1) are a major cause of human mitochondrial disease. More than 150 different point mutations in the gene have been reported to be disease causing, resulting in a large range of clinical symptoms. Depending on the mutation or combination of mutations, disease onset can occur in early infancy or late in adult life. Here, we describe the use of multiplex ligation-dependent probe amplification (MLPA) analysis to detect deletions within POLG1, which could otherwise go undetected by solely sequencing of the gene. We present a case where an entire POLG1 allele is deleted, with a known pathogenic mutation (W748S) on the remaining allele. The deletion was found in a boy with Alpers syndrome, presenting at 18 months of age with slightly retarded motor development, balance problems, and seizures. Administration of valproic acid (VPA) led to rapidly progressive fatal liver failure in our patient, and we would like to highlight the need to carry out complete POLG1 gene analysis before administration of VPA in cases of pediatric seizure disorders of unknown origin. Debut and severity of the disease in this patient was unique when compared to homozygous or heterozygous patients with the W748S mutation, leading to the conclusion that gene dosage plays a role in the clinical phenotype of this disease.

Published

2011

36. Visual function, ocular motility and ocular characteristics in patients with mitochondrial complex I deficiency

Author

Karin Naess, Lene Martin, Monica Olsson, Kristina Teär Fahnehjelm, Jan Ygge, Ulrika von Döbeln, and Maria Kristoffersen Wiberg

Subjects

Male, medicine.medical_specialty, Pathology, Visual acuity, Mitochondrial Diseases, genetic structures, Adolescent, Vision Disorders, Visual Acuity, Biology, Ocular Motility Disorders, Young Adult, Ophthalmology, medicine, Prevalence, Humans, In patient, Prospective Studies, Young adult, Child, Electron Transport Complex I, Ocular motility, General Medicine, Magnetic Resonance Imaging, eye diseases, MITOCHONDRIAL COMPLEX I DEFICIENCY, Optic Atrophy, Complex i deficiency, Visual function, Child, Preschool, Female, sense organs, medicine.symptom, Visual Fields, Follow-Up Studies

Abstract

The aims of the present study were to investigate visual function, ocular motility and ocular characteristics in children and young adults with complex I deficiency.In a prospective study with longitudinal follow-up, the visual and ocular outcome in 13 patients with deficiency in complex I [nicotine-amide adenine dinucleotide (NADH) dehydrogenase] in the mitochondrial respiratory chain is presented. The patients were diagnosed during 1995-2007 and assessed during 1997-2009 at a median age of 12.8 years (range 3.1-23.4).Twelve of 13 patients had visual impairment and/or ocular pathology. Four of 10 patients who co-operated in visual assessment had a best corrected decimal visual acuity of ≤ 0.5 in one or both eyes. Cataract surgery was performed in one patient and another patient showed retinal pigmentations and ptosis. Eleven patients demonstrated ocular motility problems, mainly saccade deficiencies. Five patients had optic atrophy (OA), which was bilateral in four patients. In four siblings, the OA showed a similarity to Leber's Hereditary Optic Neuropathy. These patients also had the 11778 G → A mutation in mitochondrial DNA. Only one patient had normal visual acuity and ocular outcome including refraction and visual fields. Follow-up time was median 3.0 years (range 0-11).Visual impairment, ocular motility problems and OA are common in children and young adults with complex I deficiency and should prompt the paediatric ophthalmologist to consider mitochondrial disorders.

Published

2010

37. Two novel mutations in thymidine kinase-2 cause early onset fatal encephalomyopathy and severe mtDNA depletion

Author

Rolf Wibom, Inger Nennesmo, Anna Karlsson, Karin Naess, Ulrika von Döbeln, Nicola Solaroli, Nicole Lesko, and Nils-Göran Larsson

Subjects

Male, Mitochondrial DNA, Mitochondrial Diseases, DNA Mutational Analysis, Biology, medicine.disease_cause, Arginine, DNA, Mitochondrial, Thymidine Kinase, chemistry.chemical_compound, Adenosine Triphosphate, Mitochondrial Encephalomyopathies, medicine, Humans, Genetic Predisposition to Disease, Child, Muscle, Skeletal, Genetics (clinical), Mutation, Kinase, Infant, Newborn, Tryptophan, Infant, Molecular biology, Stop codon, Mitochondria, Mitochondria, Muscle, Deoxyribonucleoside, Neurology, chemistry, Child, Preschool, Pediatrics, Perinatology and Child Health, Cancer research, Mutagenesis, Site-Directed, Phosphorylation, Deoxycytidine, Female, Neurology (clinical), Thymidine

Abstract

Deficiency of thymidine kinase-2 (TK2) has been described in children with early onset fatal skeletal myopathy. TK2 is a mitochondrial deoxyribonucleoside kinase required for the phosphorylation of deoxycytidine and deoxythymidine and hence is vital for the maintenance of a balanced mitochondrial dNTP pool in post-mitotic tissues. We describe a patient with two novel TK2 mutations, which caused disease onset shortly after birth and death at the age of three months. One mutation (219insCG) generated an early stop codon, thus preventing the synthesis of a functional protein. The second mutation (R130W) resulted in an amino acid substitution, which caused a severe reduction (

Published

2009

38. [Progress on lysosomal diseases yields hope for cure and improvement]

Author

Gunilla, Malm, Ulrika, von Döbeln, Karin, Naess, and Olle, Ringdén

Subjects

Enzyme Activation, Lysosomal Storage Diseases, Early Diagnosis, Disease Progression, Humans, Child, Prognosis, Stem Cell Transplantation

Published

2009

39. O20 – 1660 Leigh syndrome: a multicenter study of natural history

Author

IB de Angst, M. Tulinius, Niklas Darin, Johanna Uusimaa, L. De Meirleir, Charalampos Tzoulis, Karin Naess, Katariina Mankinen, Kalliopi Sofou, Helena Pihko, Pirjo Isohanni, I.F.M. de Coo, Elsebet Ostergaard, and Laurence A. Bindoff

Subjects

Natural history, Pediatrics, medicine.medical_specialty, Multicenter study, business.industry, Pediatrics, Perinatology and Child Health, Medicine, Neurology (clinical), General Medicine, business

Published

2013

40. Cerebrospinal Fluid Brain Injury Biomarkers in Children: A Multicenter Study

Author

Johan Lundgren, Elizabeth Jennions, Henrik Zetterberg, Pashtun Shahim, Karin Naess, Jan-Eric Månsson, Carl-Johan Törnhage, Niklas Mattsson, Niklas Darin, Kaj Blennow, and Ulf Andreasson

Subjects

Male, Pathology, medicine.medical_specialty, Adolescent, Tau protein, tau Proteins, Status epilepticus, Cohort Studies, Cerebrospinal fluid, Developmental Neuroscience, Neurofilament Proteins, Glial Fibrillary Acidic Protein, medicine, Humans, Child, Retrospective Studies, biology, Glial fibrillary acidic protein, business.industry, Infant, Retrospective cohort study, medicine.disease, Hydrocephalus, Neurology, Brain Injuries, Child, Preschool, Pediatrics, Perinatology and Child Health, biology.protein, Biomarker (medicine), Female, Neurology (clinical), medicine.symptom, business, Meningitis, Biomarkers

Abstract

Cerebrospinal fluid (CSF) biomarkers reflecting neuronal and astroglial injury, such as total tau (T-tau), glial fibrillary acidic protein (GFAP), and neurofilament light (NFL), have been extensively investigated in neurologic diseases in adults, but no large study has investigated these biomarkers in children.This study presents a detailed evaluation of CFS T-tau, GFAP, NFL, and CSF:albumin ratio in a large cohort of pediatric patients. This is a retrospective multicenter study on pediatric patients aged16 years (n = 607), where neuronal injury biomarkers T-tau, GFAP, NFL, and CSF albumin ratio were analyzed during 2000-2010 at the Clinical Neurochemistry Laboratory, Sahlgrenska University Hospital, Sweden. The patients were grouped into eight categories: epilepsy, infectious and inflammatory central nervous system disorders, progressive encephalopathy, static encephalopathy, tumors, movement disorders, miscellaneous disorders, and a control group.T-tau, GFAP, and NFL were increased in progressive encephalopathy (P0.001), epilepsy (P0.001), and infectious and inflammatory central nervous system disorders (P0.001) compared with controls. T-tau was the biomarker with the highest diagnostic accuracy with the area under the curve of 0.83 (95% confidence interval (CI), 0.77-0.90; P0.0001) for progressive encephalopathy followed by epilepsy 0.80 (95% CI, 0.75-0.87; P0.0001). The combination of all four biomarkers further improved the area under the curve for the progressive encephalopathy 0.87 (95% CI, 0.77-0.89; P0.0001), followed by epilepsy 0.81 (95% CI, 0.74-0.80; P = 0.030). The combination of the biomarkers also separated progressive from static encephalopathy 0.88 (95% CI, 0.83-0.93; P0.0001).CSF T-tau, GFAP, and NFL are differently altered across different neurologic diseases in children. Importantly, the biomarker pattern distinguishes between progressive and static neurologic disorders.

Published

2013

41. Erratum: Mutations in the mitochondrial tRNASer(AGY) gene are associated with deafness, retinal degeneration, myopathy and epilepsy

Author

Rolf Wibom, Robert W. Taylor, John W. Yarham, Nicole Lesko, Helen A. L. Tuppen, Richard G. Weleber, Robert McFarland, Karin Naess, Inger Nennesmo, Emma L. Blakely, Helene Bruhn, Mazhor Al-Dosary, and Nancy G. Kennaway

Subjects

Adult, Retinal degeneration, Mitochondrial DNA, Mitochondrial Diseases, Adolescent, RNA, Mitochondrial, Mitochondrial disease, Molecular Sequence Data, Deafness, Biology, medicine.disease_cause, Article, Electron Transport, Young Adult, Epilepsy, Adenosine Triphosphate, Muscular Diseases, Retinitis pigmentosa, Genetics, medicine, Humans, Child, Muscle, Skeletal, Myopathy, Gene, Cells, Cultured, RNA, Transfer, Ser, Genetics (clinical), Mutation, Base Sequence, Retinal Degeneration, medicine.disease, Heteroplasmy, Human genetics, Mitochondria, Mitochondrial respiratory chain, Child, Preschool, RNA, Female, medicine.symptom, Corrigendum

Abstract

Although over 200 pathogenic mitochondrial DNA (mtDNA) mutations have been reported to date, determining the genetic aetiology of many cases of mitochondrial disease is still not straightforward. Here, we describe the investigations undertaken to uncover the underlying molecular defect(s) in two unrelated Caucasian patients with suspected mtDNA disease, who presented with similar symptoms of myopathy, deafness, neurodevelopmental delay, epilepsy, marked fatigue and, in one case, retinal degeneration. Histochemical and biochemical evidence of mitochondrial respiratory chain deficiency was observed in the patient muscle biopsies and both patients were discovered to harbour a novel heteroplasmic mitochondrial tRNA (mt-tRNA)(Ser(AGY)) (MTTS2) mutation (m.12264CT and m.12261TC, respectively). Clear segregation of the m.12261TC mutation with the biochemical defect, as demonstrated by single-fibre radioactive RFLP, confirmed the pathogenicity of this novel variant in patient 2. However, unusually high levels of m.12264CT mutation within both COX-positive (98.4 ± 1.5%) and COX-deficient (98.2 ± 2.1%) fibres in patient 1 necessitated further functional investigations to prove its pathogenicity. Northern blot analysis demonstrated the detrimental effect of the m.12264CT mutation on mt-tRNA(Ser(AGY)) stability, ultimately resulting in decreased steady-state levels of fully assembled complexes I and IV, as shown by blue-native polyacrylamide gel electrophoresis. Our findings expand the spectrum of pathogenic mutations associated with the MTTS2 gene and highlight MTTS2 mutations as an important cause of retinal and syndromic auditory impairment.

Published

2012

42. A multi-systemic mitochondrial disorder due to a dominant p.Y955H disease variant in DNA polymerase gamma

Author

Triinu Siibak, Paula Clemente, Ana Bratic, Helene Bruhn, Timo E.S. Kauppila, Bertil Macao, Florian A. Schober, Nicole Lesko, Rolf Wibom, Karin Naess, Inger Nennesmo, Anna Wedell, Bradley Peter, Christoph Freyer, Maria Falkenberg, and Anna Wredenberg

Subjects

Adult, DNA Replication, Ophthalmoplegia, Chronic Progressive External, Infant, Articles, DNA-Directed DNA Polymerase, DNA, Mitochondrial, DNA Polymerase gamma, Mitochondria, Pedigree, Disease Models, Animal, Drosophila melanogaster, Phenotype, Mutation, Animals, Humans, Female, Amino Acid Sequence

Abstract

Mutations in the mitochondrial DNA polymerase, POLG, are associated with a variety of clinical presentations, ranging from early onset fatal brain disease in Alpers syndrome to chronic progressive external ophthalmoplegia. The majority of mutations are linked with disturbances of mitochondrial DNA (mtDNA) integrity and maintenance. On a molecular level, depending on their location within the enzyme, mutations either lead to mtDNA depletion or the accumulation of multiple mtDNA deletions, and in some cases these molecular changes can be correlated to the clinical presentation. We identified a patient with a dominant p.Y955H mutation in POLG, presenting with a severe, early-onset multi-systemic mitochondrial disease with bilateral sensorineural hearing loss, cataract, myopathy, and liver failure. Using a combination of disease models of Drosophila melanogaster and in vitro biochemistry analysis, we compare the molecular consequences of the p.Y955H mutation to the well-documented p.Y955C mutation. We demonstrate that both mutations affect mtDNA replication and display a dominant negative effect, with the p.Y955H allele resulting in a more severe polymerase dysfunction.

43. Rapid pulsed whole genome sequencing for comprehensive acute diagnostics of inborn errors of metabolism

Author

Måns Magnusson, Helene Bruhn, Mats Dahlberg, Valtteri Wirta, Martin Engvall, Robin Andeer, Michela Barbaro, Anna Wredenberg, Nicole Lesko, Chris Freyer, Anna Wedell, Pontus Larsson, Rolf Zetterström, Rolf Wibom, Ulrika von Döbeln, Tesfail Emahazion, Henrik Stranneheim, and Karin Naess

Subjects

MPS, Bioinformatics, Genetic counseling, MEDLINE, Biology, Genome, DNA sequencing, Databases, Genetic, Genetics, Humans, Pyruvate Dehydrogenase (Lipoamide), In patient, Whole genome sequencing, Genome, Human, Methodology Article, Inborn Errors of Metabolism, Computational Biology, High-Throughput Nucleotide Sequencing, Sequence Analysis, DNA, Clinical diagnosis, Human genome, Mendelian disease, DNA microarray, Metabolism, Inborn Errors, WGS, Biotechnology

Abstract

Background Massively parallel DNA sequencing (MPS) has the potential to revolutionize diagnostics, in particular for monogenic disorders. Inborn errors of metabolism (IEM) constitute a large group of monogenic disorders with highly variable clinical presentation, often with acute, nonspecific initial symptoms. In many cases irreversible damage can be reduced by initiation of specific treatment, provided that a correct molecular diagnosis can be rapidly obtained. MPS thus has the potential to significantly improve both diagnostics and outcome for affected patients in this highly specialized area of medicine. Results We have developed a conceptually novel approach for acute MPS, by analysing pulsed whole genome sequence data in real time, using automated analysis combined with data reduction and parallelization. We applied this novel methodology to an in-house developed customized work flow enabling clinical-grade analysis of all IEM with a known genetic basis, represented by a database containing 474 disease genes which is continuously updated. As proof-of-concept, two patients were retrospectively analysed in whom diagnostics had previously been performed by conventional methods. The correct disease-causing mutations were identified and presented to the clinical team after 15 and 18 hours from start of sequencing, respectively. With this information available, correct treatment would have been possible significantly sooner, likely improving outcome. Conclusions We have adapted MPS to fit into the dynamic, multidisciplinary work-flow of acute metabolic medicine. As the extent of irreversible damage in patients with IEM often correlates with timing and accuracy of management in early, critical disease stages, our novel methodology is predicted to improve patient outcome. All procedures have been designed such that they can be implemented in any technical setting and to any genetic disease area. The strategy conforms to international guidelines for clinical MPS, as only validated disease genes are investigated and as clinical specialists take responsibility for translation of results. As follow-up in patients without any known IEM, filters can be lifted and the full genome investigated, after genetic counselling and informed consent. Electronic supplementary material The online version of this article (doi:10.1186/1471-2164-15-1090) contains supplementary material, which is available to authorized users.

44. Secondary metabolic effects in complex I deficiency.

Author

Nayla Esteitie, Reetta Hinttala, Rolf Wibom, Helene Nilsson, Nicole Hance, Karin Naess, Kristina Teär‐Fahnehjelm, Ulrika Von Döbeln, Kari Majamaa, and Nils‐Göran Larsson

Published

2005