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When Enough Is Enough: Decision Criteria for Moving a Known Drug into Clinical Testing for a New Indication in the Absence of Preclinical Efficacy Data.适可而止:在缺乏临床前疗效数据的情况下,将已知药物用于新适应症临床测试的决策标准。
Assay Drug Dev Technol. 2017 Dec;15(8):354-361. doi: 10.1089/adt.2017.821. Epub 2017 Dec 1.
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Alternative strategies in drug development: clinical pharmacological aspects.药物研发中的替代策略:临床药理学方面。
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本文引用的文献

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Using Human 'Experiments of Nature' to Predict Drug Safety Issues: An Example with PCSK9 Inhibitors.利用人体“自然实验”预测药物安全问题:以 PCSK9 抑制剂为例。
Drug Saf. 2018 Mar;41(3):303-311. doi: 10.1007/s40264-017-0616-0.
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Man is the new mouse: Elective surgery as a key translational model for multi-organ dysfunction and sepsis.人类成为新的小白鼠:择期手术作为多器官功能障碍和脓毒症的关键转化模型。
J Intensive Care Soc. 2015 May;16(2):154-163. doi: 10.1177/1751143714564826. Epub 2015 Jan 7.
3
Generation of a Chronic Obstructive Pulmonary Disease Model in Mice by Repeated Ozone Exposure.通过反复暴露于臭氧建立小鼠慢性阻塞性肺疾病模型
J Vis Exp. 2017 Aug 25(126):56095. doi: 10.3791/56095.
4
Cognitive effects of electro-acupuncture and pregabalin in a trigeminal neuralgia rat model induced by cobra venom.电针和普瑞巴林对眼镜蛇毒诱导的三叉神经痛大鼠模型的认知影响
J Pain Res. 2017 Aug 8;10:1887-1897. doi: 10.2147/JPR.S140840. eCollection 2017.
5
Human immune system mouse models of Ebola virus infection.埃博拉病毒感染的人类免疫系统小鼠模型。
Curr Opin Virol. 2017 Aug;25:90-96. doi: 10.1016/j.coviro.2017.07.028. Epub 2017 Aug 12.
6
Exploring Animal Models That Resemble Idiopathic Pulmonary Fibrosis.探索类似特发性肺纤维化的动物模型。
Front Med (Lausanne). 2017 Jul 28;4:118. doi: 10.3389/fmed.2017.00118. eCollection 2017.
7
Stable engraftment of human microbiota into mice with a single oral gavage following antibiotic conditioning.经抗生素处理后,单次口服灌胃即可使人类微生物群稳定定植于小鼠体内。
Microbiome. 2017 Aug 1;5(1):87. doi: 10.1186/s40168-017-0306-2.
8
Do Animal Models of Acute Pancreatitis Reproduce Human Disease?急性胰腺炎动物模型能复制人类疾病吗?
Cell Mol Gastroenterol Hepatol. 2017 Jun 10;4(2):251-262. doi: 10.1016/j.jcmgh.2017.05.007. eCollection 2017 Sep.
9
Reverse Translation for Assessment of Confidence in Animal Models of Multiple Sclerosis for Drug Discovery.多发性硬化症药物发现中动物模型置信度评估的反向翻译。
Clin Pharmacol Ther. 2018 Feb;103(2):262-270. doi: 10.1002/cpt.801. Epub 2017 Aug 29.
10
Animal models of rheumatoid pain: experimental systems and insights.类风湿性疼痛的动物模型:实验系统与见解
Arthritis Res Ther. 2017 Jun 30;19(1):146. doi: 10.1186/s13075-017-1361-6.

适可而止:在缺乏临床前疗效数据的情况下,将已知药物用于新适应症临床测试的决策标准。

When Enough Is Enough: Decision Criteria for Moving a Known Drug into Clinical Testing for a New Indication in the Absence of Preclinical Efficacy Data.

作者信息

Pulley Jill M, Jerome Rebecca N, Zaleski Nicole M, Shirey-Rice Jana K, Pruijssers Andrea J, Lavieri Robert R, Chettiar Somsundaram N, Naylor Helen M, Aronoff David M, Edwards David A, Niswender Colleen M, Dugan Laura L, Crofford Leslie J, Bernard Gordon R, Holroyd Kenneth J

机构信息

1 Vanderbilt Institute for Clinical and Translational Research, Vanderbilt University Medical Center , Nashville, Tennessee.

2 Center for Knowledge Management, Vanderbilt University Medical Center , Nashville, Tennessee.

出版信息

Assay Drug Dev Technol. 2017 Dec;15(8):354-361. doi: 10.1089/adt.2017.821. Epub 2017 Dec 1.

DOI:10.1089/adt.2017.821
PMID:29193979
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5731541/
Abstract

Many animal models of disease are suboptimal in their representation of human diseases and lack of predictive power in the success of pivotal human trials. In the context of repurposing drugs with known human safety, it is sometimes appropriate to conduct the "last experiment first," that is, progressing directly to human investigations. However, there are not accepted criteria for when to proceed straight to humans to test a new indication. We propose a specific set of criteria to guide the decision-making around when to initiate human proof of principle without preclinical efficacy studies in animal models. This approach could accelerate the transition of novel therapeutic approaches to human applications.

摘要

许多疾病的动物模型在模拟人类疾病方面并不理想,且在关键人体试验成功方面缺乏预测能力。在重新利用已知对人类安全的药物的背景下,有时进行“先做最后一项实验”是合适的,即直接进入人体研究。然而,对于何时直接开展人体试验以测试新适应症,目前尚无公认的标准。我们提出了一套具体标准,以指导在何时不进行动物模型的临床前疗效研究就启动人体原理验证的决策过程。这种方法可以加速新型治疗方法向人体应用的转化。