Tadasu Ikeda scite author profile

Organic cation transporters (OCTs) are responsible for the hepatic and renal transport of metformin. In this study we analyzed variants of OCT1 and OCT2 genes in 33 patients (24 responders and nine non-responders) based on the hypothesis that polymorphisms in both genes contribute to large interpatient variability in the clinical efficacy of metformin. The sequences of the 5¢-flanking and coding regions of the two genes of interest were screened by singlestrand conformation polymorphism (SSCP) analysis. To compare the causative factors between responders and non-responders, we performed stepwise discriminant functional analysis. Age, body mass index (BMI) and treatment with lipid-lowering agents were demonstrated as positive predictors, and two mutations in the OCT1 gene, -43T > G in intron 1 and 408Met > Val (1222A > G) in exon 7, were negative and positive predictors, respectively, for the efficacy of metformin; the predictive accuracy was 55.5% (P < 0.05). Subsequent study indicated that OCT1 mRNA levels tended to be lower in human livers with the 408Met (1222A) variant, though the differences did not reach the level of significance. In this study it is suggested that OCT1 and OCT2 gene polymorphisms have little contribution to the clinical efficacy of metformin.

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Inhibitory effect of metformin on intestinal glucose absorption in the perfused rat intestine

Ikeda

Iwata

Murakami

2000

Biochemical Pharmacology

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Long-term effect of epalrestat on cardiac autonomic neuropathy in subjects with non-insulin dependent diabetes mellitus

Ikeda

Iwata

Tanaka

1999

Diabetes Research and Clinical Practice

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Effect of β-hydroxybutyrate and acetoacetate on insulin and glucagon secretion from perfused rat pancreas

Ikeda

Yoshida

Ito

et al. 1987

Archives of Biochemistry and Biophysics

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Effect of thyroid hormone on somatomedin-C release from perfused rat liver

et al. 1989

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The effect of thyroid hormone on plasma somatomedin-C (SmC) level and on SmC release from perfused rat liver was investigated. Plasma SmC levels and liver tissue SmC were significantly increased in thyroxine-treated rats. Physiological doses of triiodothyronine increased SmC release and SmC concentration in the perfused rat liver. These results indicate that thyroid hormone directly enhances the synthesis and release of SmC in the rat.

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Tadasu Ikeda

Human organic cation transporter (OCT1 and OCT2) gene polymorphisms and therapeutic effects of metformin

Inhibitory effect of metformin on intestinal glucose absorption in the perfused rat intestine

Long-term effect of epalrestat on cardiac autonomic neuropathy in subjects with non-insulin dependent diabetes mellitus

Effect of β-hydroxybutyrate and acetoacetate on insulin and glucagon secretion from perfused rat pancreas

Effect of thyroid hormone on somatomedin-C release from perfused rat liver

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