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Mutation in mitochondrial tRNA(Leu(UUR)) gene associated with progressive kidney disease.
Author(s) -
Janna J. Jansen,
J. A. Maassen,
Fokko J. van der Woude,
H A Lemmink,
J M van den Ouweland,
Leen M. ‘t Hart,
H.J.M. Smeets,
Jan A. Bruijn,
H.H.P.J. Lemkes
Publication year - 1997
Publication title -
journal of the american society of nephrology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 4.451
H-Index - 279
eISSN - 1533-3450
pISSN - 1046-6673
DOI - 10.1681/asn.v871118
Subject(s) - heteroplasmy , alport syndrome , mitochondrial dna , melas syndrome , sensorineural hearing loss , genetics , mutation , mitochondrial disease , diabetes mellitus , hearing loss , medicine , biology , mitochondrial myopathy , endocrinology , kidney , glomerulonephritis , gene , audiology
Several studies show an association of a guanine for adenine substitution (A-->G) at position 3243 in mitochondrial DNA (mtDNA) with a recently recognized diabetic subtype designated maternally inherited diabetes and deafness (MIDD). This mutation shows heterogeneity in its phenotypic expression as is apparent from its association with several other syndromes. Screening for the 3243A-->G mutation in mtDNA was performed in those diabetic patients attending the Leiden University Hospital diabetics clinic who had a history of maternally inherited diabetes, sensorineural hearing loss, or both. Four individuals from three unrelated families were identified who suffered from progressive nondiabetic kidney disease in association with diabetes mellitus and hearing loss. The mode of inheritance suggested maternal transmission. The combination of renal failure and hearing loss had been misdiagnosed as Alport syndrome in three of the four individuals. Therefore, in addition to these three families, another 63 unrelated patients with possible Alport syndrome were selected at random. DNA from peripheral blood and other tissues from members of the three families and from the 63 additional Alport syndrome patients was examined for the presence of the 3243A-->G mutation in mtDNA. The mutation was detected in heteroplasmic form in the four patients and their maternal relatives. Also, one of the 63 suspected Alport syndrome patients showed heteroplasmy for the 3243 mutation. These data show the existence of a kidney disease that is characterized by the presence of the A-->G mutation at position 3243 in the mtDNA.

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