A severe mitochondrial protein synthesis defect in myoblasts from a patient with mitochondrial myopathy was transferred with myoblast mitochondria into two genetically unrelated mitochondrial DNA (mtDNA)-less human cell lines, pointing to an mtDNA alteration as being responsible and sufficient for causing the disease. The transfer of the defect correlated with marked deficiencies in respiration and cytochrome c oxidase activity of the transformants and the presence in their mitochondria of mtDNA carrying a tRNA^(Lys) mutation. Furthermore, apparently complete segregation of the defective genotype and phenotype was observed in the transformants derived from the heterogeneous proband myoblast population, suggesting that the mtDNA heteroplasmy...
In the present work, a large scale investigation was done regarding the capacity of cultured human c...
The segregation of mutant and wild-type mtDNA was investigated in transformants constructed by trans...
AbstractTo investigate whether protein import is defective in mitochondrial disease, we compared the...
A severe mitochondrial protein synthesis defect in myoblasts from a patient with mitochondrial myopa...
We studied the physiometabolic effects of a mitochondrial DNA (mtDNA) heteroplasmic point mutation, ...
The mitochondrial myopathies are associated with an expanding list of mitochondrial DNA (mtDNA) abno...
Mitochondria are organelles present in all nucleated cells and are the only location of extra-chromo...
The pathogenetic mechanism of the mitochondrial tRNA^(Leu)_(UUR) gene mutation responsible for the M...
AbstractMitochondrial respiratory chain deficiencies represent one of the major causes of metabolic ...
AbstractDefects of the mitochondrial protein synthesis cause a subgroup of mitochondrial diseases, w...
Mutations in several mitochondrial DNA and nuclear genes involved in mitochondrial protein synthesis...
The human mitochondrial genome (mtDNA) encodes polypeptides that are critical for coupling oxidative...
The maternally inherited mitochondrial DNA (mtDNA) A3243G point mutation, in tRNALeu(UUR) gene is as...
Mutations in several mitochondrial DNA and nuclear genes involved in mitochondrial protein synthesis...
Mitochondrial disorders have become the most common cause of inborn errors of metabolism. Impairment...
In the present work, a large scale investigation was done regarding the capacity of cultured human c...
The segregation of mutant and wild-type mtDNA was investigated in transformants constructed by trans...
AbstractTo investigate whether protein import is defective in mitochondrial disease, we compared the...
A severe mitochondrial protein synthesis defect in myoblasts from a patient with mitochondrial myopa...
We studied the physiometabolic effects of a mitochondrial DNA (mtDNA) heteroplasmic point mutation, ...
The mitochondrial myopathies are associated with an expanding list of mitochondrial DNA (mtDNA) abno...
Mitochondria are organelles present in all nucleated cells and are the only location of extra-chromo...
The pathogenetic mechanism of the mitochondrial tRNA^(Leu)_(UUR) gene mutation responsible for the M...
AbstractMitochondrial respiratory chain deficiencies represent one of the major causes of metabolic ...
AbstractDefects of the mitochondrial protein synthesis cause a subgroup of mitochondrial diseases, w...
Mutations in several mitochondrial DNA and nuclear genes involved in mitochondrial protein synthesis...
The human mitochondrial genome (mtDNA) encodes polypeptides that are critical for coupling oxidative...
The maternally inherited mitochondrial DNA (mtDNA) A3243G point mutation, in tRNALeu(UUR) gene is as...
Mutations in several mitochondrial DNA and nuclear genes involved in mitochondrial protein synthesis...
Mitochondrial disorders have become the most common cause of inborn errors of metabolism. Impairment...
In the present work, a large scale investigation was done regarding the capacity of cultured human c...
The segregation of mutant and wild-type mtDNA was investigated in transformants constructed by trans...
AbstractTo investigate whether protein import is defective in mitochondrial disease, we compared the...