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首页> 外文期刊>Journal of Internal Medicine >Free fatty acid kinetics during long-term treatment with pioglitazone added to sulfonylurea or metformin in Type 2 diabetes.
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Free fatty acid kinetics during long-term treatment with pioglitazone added to sulfonylurea or metformin in Type 2 diabetes.

机译:在2型糖尿病患者中,将吡格列酮添加到磺酰脲或二甲双胍中长期治疗期间的游离脂肪酸动力学。

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BACKGROUND: Free fatty acids (FFAs) are linked to impaired insulin action, but their role in mediating long-term insulin sensitization during diabetes treatment is unclear. OBJECTIVES: To examine the effect of pioglitazone addition to existing therapy on FFA dynamics and insulin action. DESIGN: Two 2-year, randomized, parallel-group, double-blind, double-dummy, clinical trials. SETTING: One hundred and seventy-one centres in Europe, Australia and Canada. SUBJECTS: Male and female patients with Type 2 diabetes inadequately managed with metformin or sulfonylurea. INTERVENTIONS: Patients were randomized to pioglitazone (15-45 mg day(-1); n=319) or metformin (850-2550 mg day(-1); n=320) as add-on therapy to gliclazide or pioglitazone (n=317) versus gliclazide (80-320 mg day(-1); n=313) as add-on therapy to metformin. OUTCOME MEASURE: Plasma FFA profiles during oral glucose tolerance tests in selected centres before and during treatment (n=588). RESULTS: At Week 104, pioglitazone treatment decreased fastingFFAs by 0.08 mmol L(-1) when added to sulfonylurea and by 0.11 mmol L(-1) when added to metformin versus the respective sulfonylurea + metformin groups (0.03 mmol L(-1), P=0.05 and 0.04 mmol L(-1), P<0.05), and this was accompanied by significant improvements in fasting adipose tissue insulin sensitivity. Changes in postchallenge FFAs were similar between groups and not related to changes in liver transaminases, insulin action and secretion. However, the sensitivity of FFA to insulin was affected by treatment (P<0.001) and visit (P<0.05). Insulin sensitivity of FFA rose when pioglitazone was added to sulfonylurea (P<0.05), but decreased for gliclazide + metformin (P<0.05). CONCLUSION: Long-term improvements in adipose tissue insulin sensitivity and reduction in fasting FFAs with pioglitazone may help to reduce lipotoxicity in Type 2 diabetes.
机译:背景:游离脂肪酸(FFA)与胰岛素作用受损有关,但在糖尿病治疗期间它们在介导长期胰岛素增敏中的作用尚不清楚。目的:研究吡格列酮在现有治疗中的添加对FFA动力学和胰岛素作用的影响。设计:两项为期2年,随机,平行分组,双盲,双模拟的临床试验。地点:在欧洲,澳大利亚和加拿大的一百一十一个中心。研究对象:患有二甲双胍或磺脲类药物治疗不足的2型糖尿病男性和女性患者。干预措施:患者随机分为吡格列酮(15-45 mg day(-1); n = 319)或二甲双胍(850-2550 mg day(-1); n = 320)作为格列齐特或吡格列酮(n = 317)与格列齐特(80-320 mg day(-1); n = 313)作为二甲双胍的附加疗法。观察指标:治疗前和治疗中在选定中心进行的口服葡萄糖耐量试验期间的血浆FFA分布(n = 588)。结果:在第104周时,吡格列酮治疗与磺酰脲+二甲双胍组(0.03 mmol L(-1)相比,磺酰脲添加时的空腹FFA降低0.08 mmol L(-1),而二甲双胍则降低0.11 mmol L(-1)。 ,P = 0.05和0.04 mmol L(-1),P <0.05),并伴有对空腹脂肪组织胰岛素敏感性的显着改善。攻击后FFA的变化在各组之间相似,与肝转氨酶,胰岛素作用和分泌的变化无关。然而,FFA对胰岛素的敏感性受治疗(P <0.001)和就诊(P <0.05)的影响。在磺脲类中加入吡格列酮对FFA的胰岛素敏感性升高(P <0.05),但格列齐特+二甲双胍对FFA的胰岛素敏感性降低(P <0.05)。结论:吡格列酮对脂肪组织胰岛素敏感性的长期改善和空腹FFA的降低可能有助于减少2型糖尿病的脂毒性。

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