Title of article
Multiple hepatic mitochondrial DNA deletions suggest premature oxidative aging in alcoholic patients
Author/Authors
Abdellah Mansouri، نويسنده , , Bernard Fromenty، نويسنده , , Alain Berson، نويسنده , , Marie-Anne Robin، نويسنده , , Sylvie Grimbert، نويسنده , , Michel Beaugrand، نويسنده , , Serge Erlinger، نويسنده , , Dominique Pessayre، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 1997
Pages
7
From page
96
To page
102
Abstract
Background/Aims: A 4977-base pair deletion has been detected in the hepatic mitochondrial DNA of alcoholic patients with microvesicular steatosis, a lesion ascribed to impaired mitochondrial β-oxidation. However, only a single deletion had been looked for in this previous study, and it could not be determined whether the deletion was preexisting or acquired. Alcohol abuse increases the formation of reactive oxygen species in hepatic mitochondria. If this effect accelerates the oxidative aging of mitochondrial DNA, several other mutations would be expected.
Methods: The mtDNA region extending from nucleotide 8167 to nucleotide 14246 was screened for the presence of large mitochondrial DNA deletions in 58 alcoholic patients and 67 age-matched non-alcoholic controls. Hepatic DNA was subjected to polymerase chain reactions that amplified non-deleted and deleted mitochondrial DNA, respectively, and the boundaries of the mitochondrial DNA deletions were sequenced.
Results: Only 3% of the non-alcoholic controls carried a mitochondrial DNA deletion, whereas 24% of all alcoholic patients and 85% of the 13 alcoholic patients with microvesicular steatosis exhibited either single or multiple 4977, 5385, 5039 and 5556-base pair mitochondrial DNA deletions. No deletion(s) were observed, however, in 13 patients with microvesicular steatosis due to other causes.
Conclusions: Diverse mitochondrial DNA rearrangements are observed in alcoholic patients with microvesicular steatosis. We suggest that alcohol abuse leads to premature oxidative aging of mitochondrial DNA. Hypothetically, oxidative damage to mitochondrial constituents (DNA, proteins and lipids) may favor microvesicular fat deposition.
Keywords
aging , Alcoholism , DNA , mitochondria , Steatosis. , mutations
Journal title
Journal of Hepatology
Serial Year
1997
Journal title
Journal of Hepatology
Record number
583814
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