Coordinated Regulation of Fat-specific and Liver-specific Glycerol Channels, Aquaporin Adipose and Aquaporin 9

Overview

Journal Diabetes

Specialty Endocrinology

Date 2002 Sep 28

PMID 12351427

Citations 73

Authors

Hiroshi Kuriyama

Iichiro Shimomura

Ken Kishida

Hidehiko Kondo

Naoki Furuyama

Hitoshi Nishizawa

Norikazu Maeda

Morihiro Matsuda

Hiroyuki Nagaretani

Shinji Kihara

Tadashi Nakamura

Yoshihiro Tochino

Tohru Funahashi

Yuji Matsuzawa

Affiliations

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Abstract

Plasma glycerol is a major substrate for hepatic gluconeogenesis. Aquaporin adipose (AQPap/7), an adipose-specific glycerol channel, provides fat-derived glycerol into plasma. In the present study, we cloned the coding and promoter regions of mouse aquaporin 9 (AQP9), a liver-specific glycerol channel. Fasting and refeeding of mice increased and decreased hepatic AQP9 mRNA levels, respectively. Insulin deficiency induced by streptozotocin resulted in increased hepatic AQP9 mRNA. These changes in hepatic AQP9 mRNA were accompanied by those of hepatic gluconeogenic mRNAs and plasma glycerol levels. In cultured hepatocytes, insulin downregulated AQP9 mRNA. The AQP9 promoter contained the negative insulin response element TGTTTTC at -496/-502, similar to the promoter of the AQPap/7 gene. In contrast, in insulin-resistant db+/db+ mice, AQPap/7 mRNA in fat and AQP9 mRNA in liver were increased, despite hyperinsulinemia, with high plasma glycerol and glucose levels. Glycerol infusion in the db+/db+ mice augmented hepatic glucose output. Our results indicate that coordinated regulations of fat-specific AQPap/7 and liver-specific AQP9 should be crucial to determine glucose metabolism in physiology and insulin resistance.

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