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首页> 外文期刊>Clinical Pharmacology and Therapeutics >Can modeling of health outcomes facilitate regulatory decision making? The benefit-risk tradeoff for rosiglitazone in 1999 vs. 2007.
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Can modeling of health outcomes facilitate regulatory decision making? The benefit-risk tradeoff for rosiglitazone in 1999 vs. 2007.

机译:健康结果的建模是否可以促进监管决策?罗格列酮在1999年与2007年的收益风险权衡。

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摘要

Rosiglitazone was initially approved for type 2 diabetes monotherapy. We tested health-outcomes modeling as an aid to regulatory decision making by quantifying the incremental net benefit (INB) value of rosiglitazone (relative to a comparator), both at the time of first approval (1999) and at the FDA advisory committee review (2007). Using 1999 data, rosiglitazone was projected to provide an additional 0.639 years of life (0.373 quality-adjusted life years (QALYs)) relative to placebo but a loss of 0.312 years (0.173 QALYs) relative to glyburide, with uncertainty in reduction of hemoglobin A(1c) (HbA(1c)) level having the greatest impact on the benefit-risk profile. By 2007, rosiglitazone was projected to provide an additional 0.222 years (0.091 QALYs) vs. glyburide and 0.026 years vs. metformin (0.009 QALYs). Modeling suggested that the use of rosiglitazone as monotherapy was not initially warranted, given the uncertainty with regard to benefit. Despite similar net benefit (NB) as metformin shown in postmarketing data, residual cardiovascular (CV) concerns did not support the use of rosiglitazone as first-line therapy. We adapted a mathematical diabetes model to estimate NB and uncertainty of diabetes monotherapy.
机译:罗格列酮最初被批准用于2型糖尿病单药治疗。在首次批准时(1999年)和FDA咨询委员会审查时,我们通过量化罗格列酮(相对于比较者)的增量净收益(INB)值,测试了健康结局模型,以帮助制定法规。 2007)。使用1999年的数据,罗格列酮预计相对于安慰剂可提供额外的0.639年寿命(0.373质量调整生命年(QALYs)),但相对于格列本脲,则可减少0.312年(0.173 QALYs),且血红蛋白A减少的不确定性(1c)(HbA(1c))水平对利益风险曲线的影响最大。到2007年,罗格列酮预计将比格列本脲提供0.222年(0.091 QALYs),比二甲双胍(0.009 QALYs)提供0.026年。建模表明,鉴于获益的不确定性,最初不需使用罗格列酮单药治疗。尽管上市后的数据显示出与二甲双胍类似的净收益(NB),但对残留心血管(CV)的担忧并不支持使用罗格列酮作为一线治疗。我们采用了数学上的糖尿病模型来估计NB和糖尿病单药治疗的不确定性。

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