Tanaka Naoki, Nagaya Tadanobu, Komatsu Michiharu, Horiuchi Akira, Tsuruta Goro, Shirakawa Haruaki, Umemura Takeji, Ichijo Tetsuya, Matsumoto Akihiro, Yoshizawa Kaname, Aoyama Toshifumi, Kiyosawa Kendo, Tanaka Eiji
Department of Metabolic Regulation, Shinshu University Graduate School of Medicine, Matsumoto, Japan.
Liver Int. 2008 Sep;28(8):1104-11. doi: 10.1111/j.1478-3231.2008.01737.x. Epub 2008 Apr 7.
BACKGROUND/AIMS: Recent studies using transgenic mouse models have demonstrated that the presence of hepatitis C virus (HCV) singularly induces insulin resistance (IR). When evaluated in humans, the exclusion of other factors influencing IR, such as obesity, alcohol intake, hepatic inflammation and steatosis is needed, but only few studies have been performed to these ends. Therefore, we aimed at exploring the singular effects of HCV on glucose metabolism through analysis of HCV carriers with persistently normal serum aminotransferase.
Non-obese, non-diabetic and non-alcoholic HCV carriers (n=30) were enrolled with 30 hepatitis B virus carriers matched by age, gender, body mass index and waist-to-hip ratio. All patients maintained normal serum aminotransferase (<30 U/L), hyaluronic acid (<50 ng/ml) and platelet count (>150 x 10(3)/microl) for more than 5 years without additional treatments, and had no signs of steatosis. We then compared fasting plasma glucose, serum insulin and adiponectin, and homoeostasis model assessment of IR (HOMA-IR) and HOMA-beta indices between the groups.
There were no significant differences in IR/secretion-associated markers or serum adiponectin. Multivariate analysis demonstrated that the presence of HCV was not an independent predictor of IR. HOMA-IR was strongly correlated with waist circumferences and serum gamma-glutamyltransferase in HCV carriers, but not with serum aminotransferase, high-sensitivity C-reactive protein, hyaluronic acid or HCV core antigen.
These results suggest that the presence of HCV alone does not affect IR. Coexistence of hepatitis, steatosis and/or fibrosis may be important to the pathogenesis of IR induced by chronic HCV infection.
背景/目的:最近使用转基因小鼠模型的研究表明,丙型肝炎病毒(HCV)单独存在可诱导胰岛素抵抗(IR)。在人类中进行评估时,需要排除其他影响IR的因素,如肥胖、酒精摄入、肝脏炎症和脂肪变性,但为此目的仅进行了少数研究。因此,我们旨在通过分析血清氨基转移酶持续正常的HCV携带者来探讨HCV对葡萄糖代谢的单独影响。
纳入非肥胖、非糖尿病且不饮酒的HCV携带者(n = 30),并与30名年龄、性别、体重指数和腰臀比相匹配的乙型肝炎病毒携带者进行对照。所有患者在未接受额外治疗的情况下,血清氨基转移酶(<30 U/L)、透明质酸(<50 ng/ml)和血小板计数(>150×10³/微升)持续正常超过5年,且无脂肪变性迹象。然后我们比较了两组之间的空腹血糖、血清胰岛素和脂联素,以及IR的稳态模型评估(HOMA-IR)和HOMA-β指数。
IR/分泌相关标志物或血清脂联素无显著差异。多变量分析表明,HCV的存在不是IR的独立预测因素。在HCV携带者中,HOMA-IR与腰围和血清γ-谷氨酰转移酶密切相关,但与血清氨基转移酶、高敏C反应蛋白、透明质酸或HCV核心抗原无关。
这些结果表明,单独存在HCV并不影响IR。肝炎、脂肪变性和/或纤维化的共存可能对慢性HCV感染诱导的IR发病机制很重要。
