肝臓のナルディライジンは皮膚血流調節を介して褐色脂肪の適応熱産生を制御する

• Published in: 日本薬理学会年会要旨集 p. 2-O-025
• Main Authors: 大野, 美紀子, 今井, 隆行, 岩﨑, 広高, 茶谷, 元晴, 安川, 大貴, 西, 清人, 松田, 真太郎, 西, 英一郎
• Format: Journal Article
• Language: Japanese
• Published: 公益社団法人 日本薬理学会 2020
• Subjects: brown adipocyte; liver; peptidase; vagus nerve
• ISSN: 2435-4953
• DOI: 10.1254/jpssuppl.93.0_2-O-025

Adaptive thermogenesis is enhanced not only by cold exposure but also by feeding, which is considered as a partial defense mechanism against obesity. We have previously demonstrated that whole-body knockout mice of a metallopeptidase nardilysin (NRDC) show hypothermia and cold intolerance. Despite these phenotypes, NRDC-deficient mice (NRDC-KO) show enhanced adaptive thermogenesis in brown adipose tissue (BAT), which is due to the increased heat dissipation. Here we found that NRDC expression in the liver is increased by fasting and decreased by re-feeding in wild-type mice. To elucidate the liver-specific role of NRDC in energy metabolism, we established hepatocyte-specific NRDC deficient mice (LKO). Unexpectedly, LKO showed an enhanced BAT thermogenesis and whole-body energy expenditure, indicating the role of NRDC in inter-organ network of liver and BAT. Notably, the phenotypic difference between control and LKO was eliminated by hepatic vagotomy or the elevation of ambient temperature to thermoneutrality (30℃), suggesting that hepatic NRDC regulates BAT thermogenesis via the nervous control of heat dissipation. Indeed, LKO showed a significant increase in skin blood flow of the plantar at room temperature (23℃). Together, diet controls NRDC expression in liver, which in turn regulates adaptive thermogenesis in BAT through the control of skin blood flow.