Health Technol Assess. 2024 Oct;28(75):1-75. doi: 10.3310/TGAC4201.
Neonates with suspected sepsis are commonly treated with gentamicin, an aminoglycoside. These antibiotics are associated with high risk of ototoxicity, including profound bilateral deafness, in people with the m.1555A>G mitochondrial genetic variant.
This early value assessment summarised and critically assessed the clinical effectiveness and cost-effectiveness of the Genedrive MT-RNR1 ID Kit for identifying the gene m.1555A>G variant in neonates and mothers of neonates needing antibiotics or anticipated to need antibiotics. Following feedback from the scoping workshop and specialist assessment subgroup meeting, we also considered the Genedrive MT-RNR1 ID Kit for identifying the m.1555A>G variant in mothers prior to giving birth.
For clinical effectiveness, we searched three major databases in October 2022: MEDLINE, EMBASE and CINAHL (Cumulative Index to Nursing and Allied Health Literature). For cost-effectiveness, in addition to the three mentioned databases we searched Cochrane and RePEc-IDEAS.
Study selection and risk-of-bias assessment were conducted by two independent reviewers (Ryan PW Kenny and Akvile Stoniute for clinical effectiveness and Hosein Shabaninejad and Tomos Robinson for cost-effectiveness). Any differences were resolved through discussion, or by a third reviewer (Nick Meader).
Risk of bias was assessed using Quality Assessment of Diagnostic Accuracy Studies-2. One study ( = 751 neonates recruited) was included in the clinical effectiveness review and no studies were included in the cost-effectiveness review. All except one outcome (test failure rate: low risk of bias) were rated as being at moderate risk of bias. The study reported accuracy of the test (sensitivity 100%, 95% confidence interval 29.2% to 100%; specificity 99.2%, 95% confidence interval 98% to 99.7%), number of neonates successfully tested ( = 424/526 admissions), test failure rate (17.1%, although this was reduced to 5.7%), impact on antibiotic use (all those with a m.1555A>G genotype avoided aminoglycosides), time taken to obtain a sample (6 minutes), time to genotyping (26 minutes), time to antibiotic treatment (55.18 minutes) and the number of neonates with m.1555A>G ( = 3).
The economic component of this work identified key evidence gaps for which further data are required before a robust economic evaluation can be conducted. These include the sensitivity of the Genedrive MT-RNR1 ID Kit for identifying the gene m.1555A>G variant in neonates, the magnitude of risk for aminoglycoside-induced hearing loss in neonates with m.1555A>G, and the prevalence of the m.1555A>G variant. Other potentially important gaps include how data regarding maternal inheritance may potentially be used in the clinical pathway.
This early value assessment suggests that the Genedrive MT-RNR1 ID Kit has the potential to identify the m.1555A>G variant and to be cost-effective. The Genedrive MT-RNR1 ID Kit dominates the current standard of care over the lifetime, as it is less costly and more effective. For a 50-year time horizon, the Genedrive MT-RNR1 ID Kit was also the dominant strategy. For a 10-year time horizon, the incremental cost-effectiveness ratio was estimated to be £103 per quality-adjusted life-year gained. Nevertheless, as anticipated, there is insufficient evidence to conduct a full diagnostic assessment of the clinical effectiveness and cost-effectiveness of the Genedrive MT-RNR1 ID Kit in neonates directly or in their mothers. This report includes a list of research priorities to reduce the uncertainty around this early value assessment and to provide the additional data needed to inform a full diagnostic assessment, including cost-effectiveness modelling.
This study is registered as PROSPERO (CRD42022364770).
This award was funded by the National Institute for Health and Care Research (NIHR) Evidence Synthesis programme (NIHR award ref: NIHR135636) and is published in full in ; Vol. 28, No. 75. See the NIHR Funding and Awards website for further award information.
患有疑似败血症的新生儿通常会接受氨基糖苷类抗生素庆大霉素治疗。这些抗生素与耳毒性风险高有关,包括携带 m.1555A>G 线粒体遗传变异的人发生严重双侧耳聋。
本早期价值评估总结并批判性评估了 Genedrive MT-RNR1 ID 试剂盒在识别需要抗生素或预期需要抗生素的新生儿及其母亲的基因 m.1555A>G 变异方面的临床有效性和成本效益。在反馈了范围界定研讨会和专家评估小组会议的意见后,我们还考虑了 Genedrive MT-RNR1 ID 试剂盒在母亲分娩前识别 m.1555A>G 变异的情况。
对于临床有效性,我们在 2022 年 10 月检索了三个主要数据库:MEDLINE、EMBASE 和 CINAHL( Cumulative Index to Nursing and Allied Health Literature )。对于成本效益,除了这三个数据库,我们还检索了 Cochrane 和 RePEc-IDEAS。
两名独立评审员(Ryan PW Kenny 和 Akvile Stoniute 进行临床有效性评审,Hosein Shabaninejad 和 Tomos Robinson 进行成本效益评审)进行了研究选择和偏倚风险评估。任何差异均通过讨论或由第三名评审员(Nick Meader)解决。
使用诊断准确性研究质量评估-2 评估偏倚风险。一项研究(纳入 751 名新生儿)纳入了临床有效性评价,没有研究纳入成本效益评价。除了一个结局(检测失败率:低偏倚风险),所有结局的偏倚风险均被评为中度。该研究报告了检测的准确性(灵敏度 100%,95%置信区间 29.2%至 100%;特异性 99.2%,95%置信区间 98%至 99.7%)、成功检测的新生儿数量(=424/526 人次)、检测失败率(17.1%,尽管降至 5.7%)、对抗生素使用的影响(所有 m.1555A>G 基因型的人避免了氨基糖苷类药物)、获取样本的时间(6 分钟)、基因分型的时间(26 分钟)、抗生素治疗的时间(55.18 分钟)以及 m.1555A>G 的新生儿数量(=3)。
这项工作的经济部分确定了关键的证据差距,在进行稳健的经济评估之前需要进一步的数据。这些差距包括 Genedrive MT-RNR1 ID 试剂盒识别新生儿中 m.1555A>G 基因变异的敏感性、m.1555A>G 基因型新生儿中氨基糖苷类药物引起听力损失的风险程度,以及 m.1555A>G 变异的流行程度。其他潜在的重要差距包括如何在临床途径中使用关于母体遗传的数据。
本早期价值评估表明,Genedrive MT-RNR1 ID 试剂盒有可能识别 m.1555A>G 变异,并具有成本效益。在一生中,Genedrive MT-RNR1 ID 试剂盒优于当前的标准治疗方法,因为它更便宜且更有效。在 50 年的时间范围内,Genedrive MT-RNR1 ID 试剂盒也是主导策略。在 10 年的时间范围内,增量成本效益比估计为每获得一个质量调整生命年增加 103 英镑。然而,正如预期的那样,目前还没有足够的证据直接在新生儿或其母亲中进行 Genedrive MT-RNR1 ID 试剂盒的临床有效性和成本效益的全面诊断评估。本报告包括一系列研究重点,以降低对该早期价值评估的不确定性,并提供进行全面诊断评估所需的额外数据,包括成本效益建模。
本研究在 PROSPERO 中注册(CRD42022364770)。
该奖项由英国国家卫生与保健研究所(NIHR)证据综合计划(NIHR 奖 REF:NIHR135636)资助,并全文发表于 ; Vol. 28, No. 75. 请访问 NIHR 资助和奖项网站以获取更多奖项信息。
