The Value-of-Information and Value-of-Implementation from Clinical Trials of Diagnostic Tests for HIV-Associated Tuberculosis: A Modeling Analysis.

IF 1.9 Q3 HEALTH CARE SCIENCES & SERVICES MDM Policy and Practice Pub Date : 2023-09-22 eCollection Date: 2023-07-01 DOI:10.1177/23814683231198873
Pamela P Pei, Kieran P Fitzmaurice, Mylinh H Le, Christopher Panella, Michelle L Jones, Ankur Pandya, C Robert Horsburgh, Kenneth A Freedberg, Milton C Weinstein, A David Paltiel, Krishna P Reddy
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We employed an extended framework that includes value-of-implementation (VOM)-the benefit of encouraging adoption of an optimal strategy-and estimated how future trials of diagnostic tests for HIV-associated tuberculosis could improve public health decision making and clinical and economic outcomes. <b>Methods.</b> We evaluated the clinical outcomes and costs, given current information, of 3 tuberculosis screening strategies among hospitalized people with HIV in South Africa: sputum Xpert (<i>Xpert</i>), sputum Xpert plus urine AlereLAM (<i>Xpert+AlereLAM</i>), and sputum Xpert plus the newer, more sensitive, and costlier urine FujiLAM (<i>Xpert+FujiLAM</i>). We projected the incremental net monetary benefit (INMB) of decision making based on results of a trial comparing mortality with each strategy, rather than decision making based solely on current knowledge of FujiLAM's improved diagnostic performance. We used a validated microsimulation to estimate VOI (the INMB of reducing parameter uncertainty before decision making) and VOM (the INMB of encouraging adoption of an optimal strategy). <b>Results.</b> With current information, adopting <i>Xpert+FujiLAM</i> yields 0.4 additional life-years/person compared with current practices (assumed 50% <i>Xpert</i> and 50% <i>Xpert+AlereLAM</i>). While the decision to adopt this optimal strategy is unaffected by information from the clinical trial (VOI = $ 0 at $3,000/year-of-life saved willingness-to-pay threshold), there is value in scaling up implementation of <i>Xpert+FujiLAM</i>, which results in an INMB (representing VOM) of $650 million over 5 y. <b>Conclusions.</b> Conventional VOI methods account for the value of switching to a new optimal strategy based on trial data but fail to account for the persuasive value of trials in increasing uptake of the optimal strategy. Evaluation of trials should include a focus on their value in reducing barriers to implementation.</p><p><strong>Highlights: </strong>In conventional VOI analysis, it is assumed that the optimal decision will always be adopted even without a trial. This can potentially lead to an underestimation of the value of trials when adoption requires new clinical trial evidence. To capture the influence that a trial may have on decision makers' willingness to adopt the optimal decision, we also consider value-of-implementation (VOM), a metric quantifying the benefit of new study information in promoting wider adoption of the optimal strategy. The overall value-of-a-trial (VOT) includes both VOI and VOM.Our model-based analysis suggests that the information obtained from a trial of screening strategies for HIV-associated tuberculosis in South Africa would have no value, when measured using traditional methods of VOI assessment. A novel strategy, which includes the urine FujiLAM test, is optimal from a health economic standpoint but is underutilized. A trial would reduce uncertainties around downstream health outcomes but likely would not change the optimal decision. The high VOT (nearly $700 million over 5 y) lies solely in promoting uptake of FujiLAM, represented as VOM.Our results highlight the importance of employing a more comprehensive approach for evaluating prospective trials, as conventional VOI methods can vastly underestimate their value. Trialists and funders can and should assess the VOT metric instead when considering trial designs and costs. 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Abstract

Objectives. Conventional value-of-information (VOI) analysis assumes complete uptake of an optimal decision. We employed an extended framework that includes value-of-implementation (VOM)-the benefit of encouraging adoption of an optimal strategy-and estimated how future trials of diagnostic tests for HIV-associated tuberculosis could improve public health decision making and clinical and economic outcomes. Methods. We evaluated the clinical outcomes and costs, given current information, of 3 tuberculosis screening strategies among hospitalized people with HIV in South Africa: sputum Xpert (Xpert), sputum Xpert plus urine AlereLAM (Xpert+AlereLAM), and sputum Xpert plus the newer, more sensitive, and costlier urine FujiLAM (Xpert+FujiLAM). We projected the incremental net monetary benefit (INMB) of decision making based on results of a trial comparing mortality with each strategy, rather than decision making based solely on current knowledge of FujiLAM's improved diagnostic performance. We used a validated microsimulation to estimate VOI (the INMB of reducing parameter uncertainty before decision making) and VOM (the INMB of encouraging adoption of an optimal strategy). Results. With current information, adopting Xpert+FujiLAM yields 0.4 additional life-years/person compared with current practices (assumed 50% Xpert and 50% Xpert+AlereLAM). While the decision to adopt this optimal strategy is unaffected by information from the clinical trial (VOI = $ 0 at $3,000/year-of-life saved willingness-to-pay threshold), there is value in scaling up implementation of Xpert+FujiLAM, which results in an INMB (representing VOM) of $650 million over 5 y. Conclusions. Conventional VOI methods account for the value of switching to a new optimal strategy based on trial data but fail to account for the persuasive value of trials in increasing uptake of the optimal strategy. Evaluation of trials should include a focus on their value in reducing barriers to implementation.

Highlights: In conventional VOI analysis, it is assumed that the optimal decision will always be adopted even without a trial. This can potentially lead to an underestimation of the value of trials when adoption requires new clinical trial evidence. To capture the influence that a trial may have on decision makers' willingness to adopt the optimal decision, we also consider value-of-implementation (VOM), a metric quantifying the benefit of new study information in promoting wider adoption of the optimal strategy. The overall value-of-a-trial (VOT) includes both VOI and VOM.Our model-based analysis suggests that the information obtained from a trial of screening strategies for HIV-associated tuberculosis in South Africa would have no value, when measured using traditional methods of VOI assessment. A novel strategy, which includes the urine FujiLAM test, is optimal from a health economic standpoint but is underutilized. A trial would reduce uncertainties around downstream health outcomes but likely would not change the optimal decision. The high VOT (nearly $700 million over 5 y) lies solely in promoting uptake of FujiLAM, represented as VOM.Our results highlight the importance of employing a more comprehensive approach for evaluating prospective trials, as conventional VOI methods can vastly underestimate their value. Trialists and funders can and should assess the VOT metric instead when considering trial designs and costs. If VOI is low, the VOM and cost of a trial can be compared with the benefits and costs of other outreach programs to determine the most cost-effective way to improve uptake.

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HIV相关结核病诊断测试临床试验的信息价值和实施价值:建模分析。
目标。传统的信息价值(VOI)分析假设完全接受最优决策。我们采用了一个扩展的框架,其中包括实施价值(VOM)——鼓励采用最佳策略的好处,并估计了未来HIV相关结核病诊断测试的试验如何改善公共卫生决策以及临床和经济结果。方法。根据目前的信息,我们评估了南非HIV住院患者中3种结核病筛查策略的临床结果和成本:痰Xpert(Xpert)、痰Xpert+尿AlertAM(Xpert+AlerAM)和痰Xpert加上更新、更敏感、更昂贵的尿FujiLAM(Xpert+FujiLAM)。我们根据比较死亡率与每种策略的试验结果预测了决策的增量净货币收益(INMB),而不是仅根据FujiLAM改进诊断性能的现有知识进行决策。我们使用经过验证的微观模拟来估计VOI(决策前减少参数不确定性的INMB)和VOM(鼓励采用最佳策略的INMB。后果根据目前的信息,与目前的做法(假设50%的Xpert和50%的Xpert+AlereLAM)相比,采用Xpert+FujiLAM可使每个人多活0.4年。虽然采用这种最佳策略的决定不受临床试验信息的影响(VOI = $ 0为3000美元/年的救命意愿支付阈值),扩大Xpert+FujiLAM的实施是有价值的,这将导致INMB(代表VOM)在5年内达到6.5亿美元 y.结论。传统的VOI方法考虑了基于试验数据切换到新的最优策略的价值,但未能考虑到试验在增加对最优策略的理解方面的说服价值。对试验的评估应包括重点关注其在减少实施障碍方面的价值。亮点:在传统的VOI分析中,假设即使没有试验,也会始终采用最佳决策。当采用需要新的临床试验证据时,这可能会导致低估试验的价值。为了了解试验可能对决策者采用最佳决策的意愿产生的影响,我们还考虑了实施价值(VOM),这是一种量化新研究信息在促进更广泛采用最佳策略方面的益处的指标。试验总价值(VOT)包括VOI和VOM。我们基于模型的分析表明,当使用传统的VOI评估方法进行测量时,从南非HIV相关结核病筛查策略试验中获得的信息没有价值。一种新的策略,包括尿液FujiLAM测试,从健康经济的角度来看是最佳的,但没有得到充分利用。试验将减少下游健康结果的不确定性,但可能不会改变最佳决策。高VOT(超过5 y) 仅在于促进对以VOM为代表的FujiLAM的吸收。我们的研究结果强调了采用更全面的方法评估前瞻性试验的重要性,因为传统的VOI方法可能会大大低估其价值。Trialist和资助者在考虑试验设计和成本时,可以也应该评估VOT指标。如果VOI较低,则可以将试验的VOM和成本与其他外展项目的收益和成本进行比较,以确定提高接受率的最具成本效益的方法。
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来源期刊
MDM Policy and Practice
MDM Policy and Practice Medicine-Health Policy
CiteScore
2.50
自引率
0.00%
发文量
28
审稿时长
15 weeks
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