J Korean Diabetes Assoc.  2000 Apr;24(2):202-215.

Devrease of Mitochondrial DNA Content in Non-Insulin Dependent Diabetic Rats

Affiliations
  • 1Divison of Metabolic Disease.
  • 2Divison of Degenerative Disease.
  • 3Department of Biomedical Sciences, NIH, Seoul, Korea .
  • 4Department of Internal Medicine, School of Medicine, Seoul National University Tohoku University.
  • 5Department of Internal Medicine, Japan.

Abstract

BACKGROUND: Although genetic disorder in diabetes mellitus (DM) is not well understood, it has been suggested that the maternally inherited mitochondrial DNA which does not follow the Mendel's laws is a genetic factor for DM. It was reported that the mitochondrial DNA contents in DM patients were decreased compared to the normal control. Similar decrease in mitochondrial DNA content before DM development was tested in animal models. METHOD: The mitochondrial DNA (mtDNA) content in various tissues obtained from two types of non-insulin dependent diabetic rats, Goto-Kakizaki (GK) and Otsuka Long-Evans Tokushima Fatty (OLETF) rats at different ages were quantified. We also determined the quantity of hepatic COX subunit lll(COX III) mRNA, and the enzyme activities of succinate dehydrogenase (SDH) and cytochrome c oxidase (COX) in mitochondria isolated from liver and skeletal muscle were measured.
RESULTS
At 6 weeks, mtDNA content of GK rat liver was 20% decreased compared to the Wistar control, The mtDNA content of Wistar rat liver was decreased to aging from 6 weeks to 24 weeks while mtDNA in GK rat liver remains relatively constant. In case of skeletal muscle, however, mtDNA contents in GK rats were 50% decreased compared to the control at 12 and 24 week old, Similarly, OLETF and LETO control rats showed the age-dependent decrease of mtDNA content in liver and pancreas. Especially the mtDNA contents in OLETF rat tissues were reduced at the younger age than the LETO control content. That is, at 6 weeks old mtDNA contents in OLETF rat pancreas and liver were only 50% of the control. The level of mitochondrial coded hepatic CDX subunit III mRNA tends to decrease with age. Despite the decrease of mtDNA content, hepatic COX lll mRNA level and COX activities and SDH activities were not altered significantly, implying that the change of mtDNA contents did not damage the mitochondrial gene transcription and mitochondrial function dramatically.
CONCLUSIONS
This results suggest that mtDNA contents in pancreas and liver decrease age-dependently but it occurs at younger age in NIDDM. The decrease of mtDNA content at young age may be a cause of NIODM.

Keyword

Mitochondrial DNA; NIDDM; Rats; COX subunit III mRNA; COX; SDH

MeSH Terms

Aging
Animals
Diabetes Mellitus
Diabetes Mellitus, Type 2
DNA, Mitochondrial*
Electron Transport Complex IV
Genes, Mitochondrial
Humans
Jurisprudence
Liver
Mitochondria
Models, Animal
Muscle, Skeletal
Pancreas
Rats*
Rats, Inbred OLETF
RNA, Messenger
Succinate Dehydrogenase
DNA, Mitochondrial
Electron Transport Complex IV
RNA, Messenger
Succinate Dehydrogenase
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