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从使用 fMRI 在一种μ-阿片受体拮抗剂治疗强迫性消费障碍的早期临床开发中学到的经验。

Lessons learned from using fMRI in the early clinical development of a mu-opioid receptor antagonist for disorders of compulsive consumption.

机构信息

Experimental Medicine (Neuroscience), Sosei Heptares, Cambridge, UK.

Brain Mapping Unit, Department of Psychiatry, University of Cambridge, Cambridge, UK.

出版信息

Psychopharmacology (Berl). 2021 May;238(5):1255-1263. doi: 10.1007/s00213-019-05427-5. Epub 2020 Jan 4.

Abstract

Functional magnetic resonance imaging (fMRI) has been widely used to gain a greater understanding of brain circuitry abnormalities in CNS disorders. fMRI has also been used to examine pharmacological modulation of brain circuity and is increasingly being used in early clinical drug development as functional pharmacodynamic index of target engagement, and to provide early indication of clinical efficacy. In this short review, we summarize data from experimental medicine and early clinical development studies of a mu-opioid receptor antagonist, GSK1521498 developed for disorders of compulsive consumption including binge eating in obesity. We demonstrate how fMRI can be used to answer important questions of early clinical drug development relating to; (1) target engagement, (2) dose response relationships, (3) differential efficacy and (4) prediction of behavioural and clinically relevant outcomes. We also highlight important methodological factors that need to be considered when conducting fMRI studies in drug development given the challenges faced with small sample sizes in Phase 1 and early proof of mechanism studies. While these data highlight the value of fMRI as a biomarker in drug development, its use for making Go/No-go decisions is still faced with challenges given the variability of responses, interpretation of brain activation changes and the limited data linking drug induced changes in brain activity to clinical or behavioural outcome. These challenges need to be addressed to fulfil the promise of fMRI as a tool in clinical drug development.

摘要

功能磁共振成像(fMRI)已广泛用于深入了解中枢神经系统疾病中的大脑电路异常。fMRI 也被用于研究药物对大脑电路的调制作用,并在早期临床药物开发中越来越多地被用作靶标结合的功能药效学指标,以及提供临床疗效的早期迹象。在这篇简短的综述中,我们总结了用于治疗强迫性消费障碍(包括肥胖症中的暴食)的 μ 阿片受体拮抗剂 GSK1521498 的实验医学和早期临床开发研究的数据。我们展示了如何使用 fMRI 来回答早期临床药物开发中有关以下方面的重要问题:(1)靶标结合,(2)剂量反应关系,(3)疗效差异,以及(4)行为和临床相关结局的预测。我们还强调了在药物开发中进行 fMRI 研究时需要考虑的重要方法学因素,因为在 1 期和早期机制证明研究中面临样本量小的挑战。虽然这些数据突出了 fMRI 作为药物开发中的生物标志物的价值,但由于反应的可变性、大脑激活变化的解释以及将药物引起的大脑活动变化与临床或行为结果联系起来的有限数据,其用于做出是/否决策仍然面临挑战。需要解决这些挑战,以实现 fMRI 在临床药物开发中的工具的承诺。

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