Your search keyword '"Hammans S"' showing total 15 results

1. A study of mitochondrial DNA mutations in peripheral lymphocytes in an aging cohort.

Author

Zhang B, Ye S, Sayer AA, Hammans SR, Adio S, Hinks LJ, Smythe PJ, Groot D, Cooper C, and Day IN

Subjects

Aged, Cohort Studies, DNA Mutational Analysis, Databases, Nucleic Acid, England, Female, Humans, Male, Phenotype, Aging genetics, DNA, Mitochondrial genetics, Lymphocytes, Mutation

Abstract

Somatic mutation in the mitochondrial genome occurs much more rapidly than in the nuclear genome and is a feature, possibly contributory, of the aging of cells and tissues. Identifying mitochondrial sequence changes in blood DNA of elderly subjects may provide a maker for the epigenetic changes of mitochondrial DNA known to occur in tissues with lower cellular turnover, and would also have implications for immunosenescence. No large-scale epidemiological studies have been reported previously. In this study we have established long-PCR banks of the mitochondrial genome from peripheral lymphocytes for an elderly cohort of 716 individuals with a range of measured aging phenotypes, and we have established assays for three widely reported mutations: the 4977 bp and 8048 bp deletions and point mutation A3243G. No individuals were identified with detectable heteroplasmy for these changes. Implications for tissue and population prevalence are discussed. The mitochondrial long-PCR DNA banks established will be useful for a wide range of studies of somatic mutation and of germline haplotypes in relation to aging.

Published

2003

2. A mitochondrial DNA tRNA(Val) point mutation associated with adult-onset Leigh syndrome.

Author

Chalmers RM, Lamont PJ, Nelson I, Ellison DW, Thomas NH, Harding AE, and Hammans SR

Subjects

Adult, Age of Onset, Brain pathology, Female, Humans, Leigh Disease diagnosis, Leigh Disease epidemiology, Magnetic Resonance Imaging, Male, Middle Aged, Muscles pathology, Pedigree, DNA, Mitochondrial genetics, Leigh Disease genetics, Point Mutation, RNA, Transfer, Val genetics

Abstract

Subacute necrotizing encephalomyelopathy (Leigh syndrome) is associated with a number of mitochondrial DNA (mtDNA) abnormalities. We studied a family with maternally inherited encephalomyelopathy. Two siblings developed adult-onset Leigh syndrome. Muscle biopsy specimens showed enhanced succinic dehydrogenase activity and cytochrome oxidase-negative fibers. We sequenced the ATPase- and transfer RNA (tRNA)-encoding genes of mtDNA and identified a novel mtDNA valine tRNA mutation at base pair 1644. This transversion was heteroplasmic in blood and muscle in all individuals studied, and the proportion of mutant mtDNA correlated with disease severity. This is the first heteroplasmic transversion within a mtDNA tRNA gene and the second pathogenic mtDNA tRNA(Val) mutation to be associated with human disease.

Published

1997

3. The mitochondrial DNA transfer RNALeu(UUR) A-->G(3243) mutation. A clinical and genetic study.

Author

Hammans SR, Sweeney MG, Hanna MG, Brockington M, Morgan-Hughes JA, and Harding AE

Subjects

Adult, Age of Onset, Aged, Child, Codon genetics, Cytochrome-c Oxidase Deficiency, DNA Mutational Analysis, DNA, Mitochondrial blood, Electron Transport Complex IV genetics, Female, Genetic Testing, Humans, Male, Middle Aged, Mitochondrial Encephalomyopathies classification, Mitochondrial Encephalomyopathies epidemiology, Mitochondrial Encephalomyopathies metabolism, Muscle, Skeletal chemistry, Muscle, Skeletal pathology, Neurologic Examination, Pedigree, Phenotype, DNA, Mitochondrial genetics, Mitochondrial Encephalomyopathies genetics, Point Mutation, RNA, Transfer, Leu genetics

Abstract

The mitochondrial tRNALeu(UUR) A-->G(3243) mutation was identified in 22 unrelated patients. The probands and their relatives were assessed clinically and by quantitative mitochondrial DNA (mtDNA) analysis. While 10 probands had clinical features consistent with the syndrome of mitochondrial myopathy, encephalopathy, lactic acidosis and stroke-like episodes (MELAS), usually associated with this mutation, 12 probands had other phenotypes including other encephalopathies, chronic progressive external ophthalmoplegia (CPEO), myoclonic epilepsy and ragged red fibres (MERRF), myopathy alone and diabetes and deafness. Histochemical analyses of muscle biopsies showed a higher proportion of cytochrome oxidase (COX) negative fibres, but fewer strongly COX reactive fibres, in patients with CPEO compared with those with MELAS. The proportion of mutant mtDNA present in blood was significantly greater in symptomatic than asymptomatic subjects, and was correlated with age in both. This correlation was not observed in patients with the tRNALys A-->G(8344) mutation. The proportion of mutant mtDNA A-->G(3243) in muscle was always greater than that in blood. Significant correlations between proportion of mutant mtDNA in blood and both age of onset of disease and a clinical severity score were observed. However, the proportion of mutant mtDNA in blood in affected and unaffected cases overlapped, preventing use of the genetic-clinical correlation for prognostic or predictive purposes. The presence of intrafamilial clustering of phenotypes and the imperfect relationship between proportion of mutant mtDNA and the presence or absence of disease suggests that other factors may determine the phenotype. To investigate this possibility further, the tRNALeu(UUR) gene was sequenced in 23 probands and six relatives. In 28 patients the sequence was normal apart from the 3243 mutation, but in members of one family there was a homoplasmic T-->C transition at position 3290 which was not found in 140 controls or 50 other patients with mitochondrial myopathy. The family with this transition had high levels of mutant mtDNA A-->G(3243), with a unique phenotype of predominant skeletal myopathy, suggesting that this second base change in tRNALeu(UUR) may influence the clinical phenotype.

Published

1995

4. Mitochondrial DNA (mtDNA) diseases: correlation of genotype to phenotype.

Author

Morgan-Hughes JA, Sweeney MG, Cooper JM, Hammans SR, Brockington M, Schapira AH, Harding AE, and Clark JB

Subjects

Adolescent, Adult, Age of Onset, Biopsy, Child, Cytochrome b Group genetics, Electron Transport Complex III genetics, Electron Transport Complex IV genetics, Female, Genotype, Humans, Male, Middle Aged, Muscle, Skeletal metabolism, Muscle, Skeletal pathology, NAD(P)H Dehydrogenase (Quinone) genetics, Phenotype, DNA, Mitochondrial genetics, MELAS Syndrome genetics, Mitochondrial Encephalomyopathies genetics, Point Mutation, RNA, Transfer, Leu genetics

Abstract

This study examines the relationship of genotype to phenotype in 14 unselected patients who were found to harbour the A3243G transition in the mitochondrial transfer RNALeu(UUR) gene commonly associated with the syndrome of mitochondrial encephalopathy, lactic acidosis and strokes (MELAS). Only 6 of the 14 cases (43%) had seizures and recurrent strokes, the core clinical features of the MELAS phenotype. Of the remaining cases, four had an encephalomyopathy with deafness, ataxia and dementia, two had syndromes with progressive external ophthalmoplegia and two had limb weakness alone. Even within the MELAS subgroup, the majority of patients had one or more clinical manifestations considered to be atypical of the MELAS syndrome. They included developmental delay, ophthalmoparesis, pigmentary retinopathy and intestinal pseudo-obstruction. The proportion of mutant mitochondrial DNA (mtDNA) in muscle was generally higher in patients with recurrent strokes than in those without strokes, the highest levels being observed in MELAS cases with early onset disease. Studies of isolated muscle mitochondria identified a range of respiratory chain abnormalities mostly involving Complex I; immunoblots of Complex I in 3 of 10 cases showed selective loss of specific subunits encoded by nuclear genes. In the group as a whole, however, no clear correlations were observed between the severity or extent of the respiratory chain abnormality and clinical phenotype or the proportion of mutant mtDNA in biopsied skeletal muscle. These discrepancies suggest that, in patients harbouring the common MELAS3243 mutation, differences in heteroplasmy and the proportions of mutant mtDNA may not be the sole determinants of disease expression and that additional genetic mechanisms are involved in defining the range of clinical and biochemical phenotypes associated with this aberrant mitochondrial genome.

Published

1995

5. Cortical reflex myoclonus in patients with the mitochondrial DNA transfer RNA(Lys)(8344) (MERRF) mutation.

Author

Thompson PD, Hammans SR, and Harding AE

Subjects

Adult, Child, Preschool, Electromyography, Evoked Potentials, Somatosensory, Female, Humans, Male, Middle Aged, Mitochondrial Myopathies diagnosis, Mitochondrial Myopathies physiopathology, Myoclonus diagnosis, Myoclonus physiopathology, Reaction Time, Cerebral Cortex physiopathology, DNA, Mitochondrial genetics, Mitochondrial Myopathies genetics, Mutation, Myoclonus genetics, RNA, Transfer, Lys genetics, Reflex

Abstract

Five patients from three families with the syndrome of myoclonic epilepsy and ragged red fibres (MERRF), associated with the mitochondrial DNA point mutation at position 8344, were studied neurophysiologically to determine the characteristics of their myoclonus. The findings were those of cortical reflex myoclonus, with enlarged cortical somatosensory evoked potentials and late reflex responses to peripheral nerve stimulation. Electroencephalography showed paroxysmal spike and polyspike and wave discharges, with photic sensitivity. This pattern of electrophysiological abnormalities was uniform, despite considerable variation in severity of myoclonus. Although a consistent finding, cortical reflex myoclonus is not specific to MERRF amongst myoclonic syndromes.

Published

1994

6. Mitochondrial DNA mutation underlying Leigh's syndrome: clinical, pathological, biochemical, and genetic studies of a patient presenting with progressive myoclonic epilepsy.

Author

Sweeney MG, Hammans SR, Duchen LW, Cooper JM, Schapira AH, Kennedy CR, Jacobs JM, Youl BD, Morgan-Hughes JA, and Harding AE

Subjects

Adolescent, Base Sequence, Brain pathology, Humans, Leigh Disease physiopathology, Magnetic Resonance Imaging, Male, Molecular Sequence Data, DNA, Mitochondrial genetics, Epilepsies, Myoclonic complications, Leigh Disease genetics, Leigh Disease pathology, Mutation

Abstract

An 18-year-old male patient presented with clinical and radiological evidence of Leigh's syndrome (LS), having developed progressive myoclonic epilepsy and ataxia 11 years previously. Muscle biopsy showed cytochrome oxidase deficiency but no ragged red fibres. Autopsy confirmed the diagnosis of LS; there was additional degenerative change in the cerebellum and dentate and olivary nuclei, and an axonal peripheral neuropathy. Biochemical studies showed reduced activity of complexes I and IV of the respiratory chain in mitochondria from heart, liver and kidney. The mutation of mitochondrial DNA (mtDNA) at position 8344, commonly associated with the syndrome of myoclonic epilepsy and ragged red fibres, was detected in the patient's blood and was present in muscle, brain, liver, heart, and kidney in uniformly high amounts. It is clear that LS is genetically heterogeneous and represents one of the most severe phenotypes of a number of different mtDNA defects.

Published

1994

7. Mitochondrial DNA and disease.

Author

Hammans SR

Subjects

Female, Humans, Male, Mutation physiology, DNA, Mitochondrial genetics, Mitochondrial Myopathies genetics

Published

1994

8. The mitochondrial DNA transfer RNA(Lys)A-->G(8344) mutation and the syndrome of myoclonic epilepsy with ragged red fibres (MERRF). Relationship of clinical phenotype to proportion of mutant mitochondrial DNA.

Author

Hammans SR, Sweeney MG, Brockington M, Lennox GG, Lawton NF, Kennedy CR, Morgan-Hughes JA, and Harding AE

Subjects

Adult, Aged, Amino Acid Sequence, Child, DNA, Mitochondrial analysis, DNA, Mitochondrial blood, Female, Humans, Male, Middle Aged, Molecular Sequence Data, Muscles chemistry, Pedigree, Phenotype, DNA, Mitochondrial genetics, MERRF Syndrome genetics, Mutation, RNA, Transfer, Lys genetics

Abstract

The mitochondrial DNA (mtDNA) transfer RNA (tRNA)Lys A-->G(8344) mutation was identified in seven patients. These patients and their relatives were assessed clinically; in one family the mutation was deduced to be present in four generations. The phenotype in index cases was consistent with the syndrome of myoclonic epilepsy with ragged red fibres, with the core clinical features of myoclonus, ataxia and seizures. Amongst other features, progressive external ophthalmoplegia, Leigh's syndrome and stroke-like episodes were observed, well recognized in mitochondrial myopathies but novel manifestations of this genotype. Samples of blood and muscle were analysed for the proportion of mutant mtDNA using an oligonucleotide hybridization technique. The proportion of mutant mtDNA in blood was significantly greater in symptomatic than asymptomatic cases. Furthermore, the proportion of mutant mtDNA in blood correlated with age of onset of disease and clinical severity assessed by a simple scale. Study of disease associated with the tRNA(Lys) A-->G(8344) mutation provides further insight into the pathogenesis and transmission of mitochondrial diseases. Quantification of the proportion of mtDNA in tissues demonstrates that this is a major factor determining the course of disease, but other, as yet unidentified factors are also likely to play a role.

Published

1993

9. A tandem duplication in the D-loop of human mitochondrial DNA is associated with deletions in mitochondrial myopathies.

Author

Brockington M, Sweeney MG, Hammans SR, Morgan-Hughes JA, and Harding AE

Subjects

Aged, Base Sequence, Female, Humans, Kearns-Sayre Syndrome genetics, Molecular Sequence Data, Muscles chemistry, Muscles pathology, DNA, Mitochondrial genetics, Mitochondrial Myopathies genetics, Multigene Family, Sequence Deletion

Abstract

About 40 per cent of patients with mitochondrial myopathies have two populations of mitochondrial DNA (mtDNA) in muscle, one of which is deleted. All patients with single mtDNA deletions and neurological disease are sporadic cases, suggesting that deletions arise as fresh mutational events. We have detected a low abundance heteroplasmic tandem duplication involving the displacement loop of mtDNA in 18 of 58 patients with deletions and 5/5 of their mothers, but not in normal subjects. The location of the duplication to a region that controls both replication and transcription of mtDNA could explain features suggesting mild mitochondrial dysfunction in the muscle biopsies of three patients' mothers, and a predisposition to deletion.

Published

1993

10. Evidence for intramitochondrial complementation between deleted and normal mitochondrial DNA in some patients with mitochondrial myopathy.

Author

Hammans SR, Sweeney MG, Holt IJ, Cooper JM, Toscano A, Clark JB, Morgan-Hughes JA, and Harding AE

Subjects

Base Sequence, Electron Transport Complex IV metabolism, Histocytochemistry, Humans, Molecular Sequence Data, Restriction Mapping, DNA metabolism, DNA, Mitochondrial metabolism, Mitochondria, Muscle metabolism, Muscular Diseases metabolism

Abstract

Twenty-three patients with mitochondrial myopathies and mitochondrial DNA deletions in muscle were studied by means of deletion mapping and sequencing, histochemistry and polarography. Histochemistry showed significantly less focal cytochrome oxidase deficiency relative to number of ragged red fibres when the deletion did not involve reading frames for cytochrome oxidase subunits. Polarography in such patients showed defects exclusively involving complex I, in contrast to the others with larger deletions who generally had more diffuse respiratory chain defects. Analysis of other published histochemical data showed similar findings to our own. It is concluded that translation of a proportion of deleted mitochondrial DNAs occurs in at least some patients with mitochondrial DNA deletions, implying that deleted and normal mitochondrial genomes share transfer RNAs within mitochondria in such cases.

Published

1992

11. Deletions of the mitochondrial genome.

Author

Harding AE and Hammans SR

Subjects

Humans, Muscular Diseases genetics, Chromosome Deletion, DNA, Mitochondrial genetics

Abstract

Single large deletions of mitochondrial DNA are found in the muscle of about 40% of patients with mitochondrial myopathies, and are detectable in both blood and muscle in Pearson syndrome. In mitochondrial myopathies, there is a close association between the presence of deletions and involvement of extra-ocular muscles, together with other features of the Kearns-Sayre syndrome. Deletions appear to arise as fresh mutations in the vast majority of patients and are often flanked by direct repeats up to 13 nucleotides in length. They should affect translation of all mitochondrially encoded components of the respiratory chain, but there is evidence to suggest that intramitochondrial complementation occurs in some cases.

Published

1992

12. Mitochondrial disease and mitochondrial DNA.

Author

Hammans SR and Harding AE

Subjects

Humans, Mitochondria metabolism, Mitochondria, Muscle pathology, Muscular Diseases pathology, Mutation, DNA, Mitochondrial genetics, Muscular Diseases genetics, Nervous System Diseases genetics

Abstract

In the last decade there have been dramatic advances in the understanding of genetic, biochemical and clinical aspects of disorders of the mitochondrial respiratory chain. Neurological manifestations are prominent although involvement of other systems is increasingly recognized. This article reviews current understanding of mitochondrial disease and in particular its genetic basis.

Published

1991

13. Mitochondrial encephalopathies: molecular genetic diagnosis from blood samples.

Author

Hammans SR, Sweeney MG, Brockington M, Morgan-Hughes JA, and Harding AE

Subjects

Acidosis, Lactic diagnosis, Adolescent, Adult, Ataxia diagnosis, Brain Diseases blood, Cerebrovascular Disorders diagnosis, Child, Child, Preschool, DNA, Mitochondrial blood, Epilepsies, Myoclonic diagnosis, Epilepsies, Myoclonic pathology, Humans, Mitochondria, Muscle, Muscles pathology, Mutation, Syndrome, Brain Diseases diagnosis, DNA, Mitochondrial genetics

Abstract

Point mutations of mitochondrial DNA have been described in the muscle of patients with syndromes of myoclonic epilepsy and ragged red fibres (MERRF) and of mitochondrial encephalopathy with lactic acidosis and stroke-like episodes (MELAS). We have found the MERRF mutation in members of 6 British kindreds; 2 of these had unusual phenotypes but all index patients had myoclonus. The MELAS mutation was detected in 17 patients from 16 families, who had a wide range of clinical features that particularly affected the central nervous system; stroke-like episodes were observed in 10.3 patients with mitochondrial DNA mutations did not have ragged red fibres on muscle biopsy, generally considered to be the morphological hallmark of mitochondrial diseases. In all 6 patients with the MERRF mutation, and 10 of 11 with the MELAS mutation, the genetic defect was easily detected in blood cells as well as muscle (blood samples were not available in 6 patients with MELAS mutations in muscle). Molecular genetic analysis of blood samples represents an inexpensive and reliable screening test for mitochondrial encephalopathies, and use of such techniques could influence diagnosis and genetic counselling in patients with seizure disorders and young-onset stroke.

Published

1991

14. Pearson syndrome and mitochondrial encephalomyopathy in a patient with a deletion of mtDNA.

Author

McShane MA, Hammans SR, Sweeney M, Holt IJ, Beattie TJ, Brett EM, and Harding AE

Subjects

Anemia, Sideroblastic genetics, Child, Exocrine Pancreatic Insufficiency genetics, Humans, Male, Mitochondria, Muscle pathology, Syndrome, Brain Diseases genetics, Chromosome Deletion, DNA, Mitochondrial genetics, Kearns-Sayre Syndrome genetics, Muscular Diseases genetics

Abstract

A patient is described who has features of Pearson syndrome and who presented in the neonatal period with a hypoplastic anemia. He later developed hepatic, renal, and exocrine pancreatic dysfunction. At the age of 5 years he developed visual impairment, tremor, ataxia, proximal muscle weakness, external ophthalmoplegia, and a pigmentary retinopathy (Kearns-Sayre syndrome). Muscle biopsy confirmed the diagnosis of mitochondrial myopathy. Analysis of mtDNA from leukocytes and muscle showed mtDNA heteroplasmy in both tissues, with one population of mtDNA deleted by 4.9 kb. The deleted region was bridged by a 13-nucleotide sequence occurring as a direct repeat in normal mtDNA. Both Pearson syndrome and Kearns-Sayre syndrome have been noted to be associated with deletions of mtDNA; they have not previously been described in the same patient. These observations indicate that the two disorders have the same molecular basis; the different phenotypes are probably determined by the initial proportion of deleted mtDNAs and modified by selection against them in different tissues.

Published

1991

15. Pearson syndrome and mitochondrial encephalomyopathy in a patient with a deletion of mtDNA

Author

Mcshane, M. A., Hammans, S. R., Sweeney, M., ian holt, Beattie, T. J., Brett, E. M., and Harding, A. E.

Subjects

Male, Brain Diseases, Muscular Diseases, Humans, Exocrine Pancreatic Insufficiency, Kearns-Sayre Syndrome, Syndrome, Chromosome Deletion, Child, DNA, Mitochondrial, Research Article, Anemia, Sideroblastic, Mitochondria, Muscle

Abstract

A patient is described who has features of Pearson syndrome and who presented in the neonatal period with a hypoplastic anemia. He later developed hepatic, renal, and exocrine pancreatic dysfunction. At the age of 5 years he developed visual impairment, tremor, ataxia, proximal muscle weakness, external ophthalmoplegia, and a pigmentary retinopathy (Kearns-Sayre syndrome). Muscle biopsy confirmed the diagnosis of mitochondrial myopathy. Analysis of mtDNA from leukocytes and muscle showed mtDNA heteroplasmy in both tissues, with one population of mtDNA deleted by 4.9 kb. The deleted region was bridged by a 13-nucleotide sequence occurring as a direct repeat in normal mtDNA. Both Pearson syndrome and Kearns-Sayre syndrome have been noted to be associated with deletions of mtDNA; they have not previously been described in the same patient. These observations indicate that the two disorders have the same molecular basis; the different phenotypes are probably determined by the initial proportion of deleted mtDNAs and modified by selection against them in different tissues.