Your search keyword '"Johanna, Uusimaa"' showing total 3 results

1. 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

2. Analysis of mitochondrial DNA sequences in patients with isolated or combined oxidative phosphorylation system deficiency

Author

Johanna Uusimaa, R.J.H. Smeets, Jan A.M. Smeitink, Reetta Hinttala, Jukka S. Moilanen, Kari Majamaa, and Cristina Ugalde

Subjects

Genetics, Mutation, Mitochondrial DNA, Nuclear gene, Energy and redox metabolism [NCMLS 4], Biology, medicine.disease_cause, Molecular biology, Respiratory enzyme, Nuclear DNA, Mitochondrial medicine [IGMD 8], medicine, Coding region, medicine.symptom, Cellular energy metabolism [UMCN 5.3], Myopathy, Gene, Letter to JMG, Genetics (clinical)

Abstract

Contains fulltext : 50631.pdf (Publisher’s version ) (Closed access) BACKGROUND: Enzyme deficiencies of the oxidative phosphorylation (OXPHOS) system may be caused by mutations in the mitochondrial DNA (mtDNA) or in the nuclear DNA. OBJECTIVE: To analyse the sequences of the mtDNA coding region in 25 patients with OXPHOS system deficiency to identify the underlying genetic defect. RESULTS: Three novel non-synonymous substitutions in protein-coding genes, 4681T-->C in MT-ND2, 9891T-->C in MT-CO3 and 14122A-->G in MT-ND5, and one novel substitution in the 12S rRNA gene, 686A-->G, were found. The definitely pathogenic mutation 3460G-->A was identified in an 18-year-old woman who had severe isolated complex I deficiency and progressive myopathy. CONCLUSIONS: Bioinformatic analyses suggest a pathogenic role for the novel 4681T-->C substitution found in a boy with Leigh's disease. These results show that the clinical phenotype caused by the primary Leber's hereditary optic neuropathy mutation 3460G-->A is more variable than has been thought. In the remaining 23 patients, the role of mtDNA mutations as a cause of the OXPHOS system deficiency could be excluded. The deficiency in these children probably originates from mutations in the nuclear genes coding for respiratory enzyme subunits or assembly factors.

Published

2006

3. Reversible infantile respiratory chain deficiency is a unique, genetically heterogenous mitochondrial disease

Author

Johanna Uusimaa, Gian Brown, Joanna Poulton, Imelda Hughes, Lucy Feng, Caroline Sewry, Francesco Muntoni, Massimo Zeviani, Jacqueline Birks, Carl Fratter, Mairtin McDermott, Giangiorgio Crisponi, Eileen P. Treacy, and Heinz Jungbluth

Subjects

Male, Candidate gene, Cytochrome-c Oxidase Deficiency, medicine.disease_cause, Child, Genetics (clinical), Genetics, Mutation, tRNA Methyltransferases, Lactic, Histocytochemistry, Brain, Skeletal, Magnetic Resonance Imaging, Hypotonia, Liver, Lactic acidosis, Child, Preschool, Muscle Hypotonia, Muscle, Acidosis, Lactic, Female, medicine.symptom, Acidosis, Adult, Adolescent, Mitochondrial disease, Molecular Sequence Data, Biology, Article, Electron Transport Complex IV, Mitochondrial Proteins, Genetic Heterogeneity, Intensive care, medicine, Animals, Humans, Family, Amino Acid Sequence, Myopathy, Muscle, Skeletal, Preschool, Face, Infant, Infant, Newborn, Sequence Alignment, Genetic heterogeneity, medicine.disease, Newborn, Immunology

Abstract

OBJECTIVES: Homoplasmic maternally inherited, m.14674T>C or m. 14674T>G mt-tRNA(Glu) mutations have recently been identified in reversible infantile cytochrome c oxidase deficiency (or 'benign COX deficiency'). This study sought other genetic defects that may give rise to similar presentations. PATIENTS: Eight patients from seven families with clinicopathological features of infantile reversible cytochrome c oxidase deficiency were investigated. METHODS: The study reviewed the diagnostic features and performed molecular genetic analyses of mitochondrial DNA and nuclear encoded candidate genes. RESULTS: Patients presented with subacute onset of profound hypotonia, feeding difficulties and lactic acidosis within the first months of life. Although recovery was remarkable, a mild myopathy persisted into adulthood. Histopathological findings in muscle included increased lipid and/or glycogen content, ragged-red and COX negative fibres. Biochemical studies suggested more generalised abnormalities than pure COX deficiency. Clinical improvement was reflected by normalisation of lactic acidosis and histopathological abnormalities. The m.14674T>C mt-tRNA(Glu) mutation was identified in four families, but none had the m. 14674T>G mutation. Furthermore, in two families pathogenic mutations were also found in the nuclear TRMU gene which has not previously been associated with this phenotype. In one family, the genetic aetiology still remains unknown. CONCLUSIONS: Benign COX deficiency is better described as 'reversible infantile respiratory chain deficiency'. It is genetically heterogeneous, and patients not carrying the m.14674T>C or T>G mt-tRNA(Glu) mutations may have mutations in the TRMU gene. Diagnosing this disorder at the molecular level is a significant advance for paediatric neurologists and intensive care paediatricians, enabling them to select children with an excellent prognosis for continuing respiratory support from those with severe mitochondrial presentation in infancy.

Published

2011