首页> 外文期刊>Diabetes care >Rosiglitazone-associated fractures in type 2 diabetes: an Analysis from A Diabetes Outcome Progression Trial (ADOPT).
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Rosiglitazone-associated fractures in type 2 diabetes: an Analysis from A Diabetes Outcome Progression Trial (ADOPT).

机译:罗格列酮相关的2型糖尿病骨折:糖尿病结果进展试验(ADOPT)的分析。

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OBJECTIVE: The purpose of this study was to examine possible factors associated with the increased risk of fractures observed with rosiglitazone in A Diabetes Outcome Progression Trial (ADOPT). RESEARCH DESIGN AND METHODS: Data from the 1,840 women and 2,511 men randomly assigned in ADOPT to rosiglitazone, metformin, or glyburide for a median of 4.0 years were examined with respect to time to first fracture, rates of occurrence, and sites of fractures. RESULTS: In men, fracture rates did not differ between treatment groups. In women, at least one fracture was reported with rosiglitazone in 60 patients (9.3% of patients, 2.74 per 100 patient-years), metformin in 30 patients (5.1%, 1.54 per 100 patient-years), and glyburide in 21 patients (3.5%, 1.29 per 100 patient-years). The cumulative incidence (95% CI) of fractures in women at 5 years was 15.1% (11.2-19.1) with rosiglitazone, 7.3% (4.4-10.1) with metformin, and 7.7% (3.7-11.7) with glyburide, representing hazard ratios (95% CI) of 1.81 (1.17-2.80) and 2.13 (1.30-3.51) for rosiglitazone compared with metformin and glyburide, respectively. The increase in fractures with rosiglitazone occurred in pre- and postmenopausal women, and fractures were seen predominantly in the lower and upper limbs. No particular risk factor underlying the increased fractures in female patients who received rosiglitazone therapy was identified. CONCLUSIONS: Further investigation into the risk factors and underlying pathophysiology for the increased fracture rate in women taking rosiglitazone is required to relate them to preclinical data and better understand the clinical implications of and possible interventions for these findings.
机译:目的:本研究的目的是检查与糖尿病结果进展试验(ADOPT)中罗格列酮观察到的骨折风险增加相关的可能因素。研究设计和方法:从ADOPT中随机分配到罗格列酮,二甲双胍或格列本脲4.0年的1,840名女性和2,511名男性的数据中,研究了首次骨折的时间,发生率和骨折部位。结果:在男性中,治疗组之间的骨折率没有差异。在女性中,至少有60例患者发生罗格列酮骨折(9.3%的患者,每100例患者年2.74例),二甲双胍在30例患者中(5.1%,每100例患者年1.54例)和格列本脲21例( 3.5%,每100病人年1.29)。罗格列酮治疗5年女性骨折的累积发生率(95%CI)为15.1%(11.2-19.1),二甲双胍为7.3%(4.4-10.1),格列本脲为7.7%(3.7-11.7),代表危险比与二甲双胍和格列本脲相比,罗格列酮的(95%CI)为1.81(1.17-2.80)和2.13(1.30-3.51)。罗格列酮增加的骨折发生在绝经前和绝经后的妇女中,骨折主要发生在下肢和上肢。在接受罗格列酮治疗的女性患者中,没有发现导致骨折增加的特殊危险因素。结论:需要进一步研究服用罗格列酮的女性骨折率升高的危险因素和潜在的病理生理学,以使其与临床前数据相关联,并更好地了解这些发现的临床意义和可能的干预措施。

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