Vatner Daniel F, Snikeris Jaclyn, Popov Violeta, Perry Rachel J, Rahimi Yasmeen, Samuel Varman T
Department of Internal Medicine,Yale University School of Medicine, New Haven, CT, United States of America.
Department of Cellular & Molecular Physiology, Yale University School of Medicine, New Haven, CT, United States of America.
PLoS One. 2015 Oct 20;10(10):e0140837. doi: 10.1371/journal.pone.0140837. eCollection 2015.
Thyroid hormone mimetics are alluring potential therapies for diseases like dyslipidemia, nonalcoholic fatty liver disease (NAFLD), and insulin resistance. Though diiodothyronines are thought inactive, pharmacologic treatment with 3,5- Diiodo-L-Thyronine (T2) reportedly reduces hepatic lipid content and improves glucose tolerance in fat-fed male rats. To test this, male Sprague Dawley rats fed a safflower-oil based high-fat diet were treated with T2 (0.25 mg/kg-d) or vehicle. Neither 10 nor 30 days of T2 treatment had an effect on weight, adiposity, plasma fatty acids, or hepatic steatosis. Insulin action was quantified in vivo by a hyperinsulinemic-euglycemic clamp. T2 did not alter fasting plasma glucose or insulin concentration. Basal endogenous glucose production (EGP) rate was unchanged. During the clamp, there was no difference in insulin stimulated whole body glucose disposal. Insulin suppressed EGP by 60% ± 10 in T2-treated rats as compared with 47% ± 4 suppression in the vehicle group (p = 0.32). This was associated with an improvement in hepatic insulin signaling; insulin stimulated Akt phosphorylation was ~2.5 fold greater in the T2-treated group as compared with the vehicle-treated group (p = 0.003). There was no change in expression of genes thought to mediate the effect of T2 on hepatic metabolism, including genes that regulate hepatic lipid oxidation (ppara, carnitine palmitoyltransferase 1a), genes that regulate hepatic fatty acid synthesis (srebp1c, acetyl coa carboxylase, fatty acid synthase), and genes involved in glycolysis and gluconeogenesis (L-pyruvate kinase, glucose 6 phosphatase). Therefore, in contrast with previous reports, in Sprague Dawley rats fed an unsaturated fat diet, T2 administration failed to improve NAFLD or whole body insulin sensitivity. Though there was a modest improvement in hepatic insulin signaling, this was not associated with significant differences in hepatic insulin action. Further study will be necessary before diiodothyronines can be considered an effective treatment for NAFLD and dyslipidemia.
甲状腺激素模拟物对于血脂异常、非酒精性脂肪性肝病(NAFLD)和胰岛素抵抗等疾病而言是颇具吸引力的潜在治疗方法。尽管二碘甲状腺原氨酸被认为无活性,但据报道,用3,5-二碘-L-甲状腺原氨酸(T2)进行药物治疗可降低高脂喂养雄性大鼠的肝脏脂质含量并改善糖耐量。为了对此进行验证,给喂食红花油基高脂饮食的雄性Sprague Dawley大鼠用T2(0.25毫克/千克-天)或赋形剂进行治疗。T2治疗10天和30天对体重、肥胖、血浆脂肪酸或肝脏脂肪变性均无影响。通过高胰岛素-正常血糖钳夹技术在体内对胰岛素作用进行定量分析。T2未改变空腹血糖或胰岛素浓度。基础内源性葡萄糖生成(EGP)率未发生变化。在钳夹期间,胰岛素刺激的全身葡萄糖处置无差异。与赋形剂组47%±4%的抑制率相比,T2治疗组中胰岛素将EGP抑制了60%±10%(p = 0.32)。这与肝脏胰岛素信号传导的改善相关;与赋形剂治疗组相比,T2治疗组中胰岛素刺激的Akt磷酸化水平高约2.5倍(p = 0.003)。被认为介导T2对肝脏代谢作用的基因表达没有变化,包括调节肝脏脂质氧化的基因(过氧化物酶体增殖物激活受体α、肉碱棕榈酰转移酶1a)、调节肝脏脂肪酸合成的基因(固醇调节元件结合蛋白1c、乙酰辅酶A羧化酶、脂肪酸合酶)以及参与糖酵解和糖异生的基因(L-丙酮酸激酶、葡萄糖6磷酸酶)。因此,与之前的报道相反,在喂食不饱和脂肪饮食的Sprague Dawley大鼠中,给予T2未能改善NAFLD或全身胰岛素敏感性。尽管肝脏胰岛素信号传导有适度改善,但这与肝脏胰岛素作用的显著差异无关。在二碘甲状腺原氨酸可被视为NAFLD和血脂异常的有效治疗方法之前,还需要进一步研究。
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