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Temporal bone histopathological and quantitative analysis of mitochondrial DNA in MELAS
Authors:Takahashi Katsumasa  Merchant Saumil N  Miyazawa Tetsuo  Yamaguchi Toshikazu  McKenna Michael J  Kouda Hiroko  Iino Yukiko  Someya Tsutomu  Tamagawa Yuya  Takiyama Yoshihisa  Nakano Imaharu  Saito Ken  Boyer Philip  Kitamura Ken
Affiliation:Department of Otolarynology, Gunma University, Maebashi, Japan.
Abstract:OBJECTIVES/HYPOTHESIS: Although hearing loss is common in MELAS (syndrome of mitochondrial encephalopathy, lactic acidosis and stroke-like episodes), the histopathology of the temporal bone has not been reported. The majority of cases of MELAS are linked to a mitochondrial DNA (mtDNA) mutation at nucleotide 3243. In MELAS, normal mtDNA and mutant mtDNA coexist in a heteroplasmic manner. The purpose of the study was to report the otopathological findings from two patients with MELAS and quantitative mtDNA analysis in the inner ear of one of these patients. STUDY DESIGN: Basic scientific histopathological examination and quantitative mtDNA analysis of the temporal bone. METHODS: Temporal bones were embedded in celloidin and sectioned for light microscopic study. Graphic reconstruction of the cochlea was performed using the method described by Schuknecht. For quantitative mtDNA analysis, total DNA from the membranous part of the inner ear was collected, amplified by polymerase chain reaction, and digested with the restriction enzyme. The percentage of mutant/total mtDNA was measured by the ratio of fluorescence intensity. RESULTS: Histopathological examination revealed severe degeneration of the stria vascularis and degenerative change of spiral ganglion cells in both patients. The quantitative DNA studies showed that the proportion of mutant to wild-type mtDNA was similar in both histologically affected and histologically unaffected tissues within the inner ear. CONCLUSION: Dysfunction of the stria vascularis and spiral ganglion cells causes sensorineural hearing loss in MELAS.
Keywords:Mitochondrial DNA  MELAS  hearing loss  histopathology  heteroplasmy
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