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Bottlenecks in the development of topical analgesics: molecule, formulation, dose-finding, and phase III design.局部用镇痛药研发中的瓶颈:分子、制剂、剂量确定及III期设计。
J Pain Res. 2017 Mar 20;10:635-641. doi: 10.2147/JPR.S131434. eCollection 2017.
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Topical phenytoin for the treatment of neuropathic pain.外用苯妥英钠治疗神经性疼痛。
J Pain Res. 2017 Feb 27;10:469-473. doi: 10.2147/JPR.S129749. eCollection 2017.
2
Skin matters! The role of keratinocytes in nociception: a rational argument for the development of topical analgesics.皮肤至关重要!角质形成细胞在伤害感受中的作用:局部镇痛药开发的合理依据。
J Pain Res. 2016 Dec 16;10:1-8. doi: 10.2147/JPR.S122765. eCollection 2017.
3
New topical treatment of vulvodynia based on the pathogenetic role of cross talk between nociceptors, immunocompetent cells, and epithelial cells.基于伤害感受器、免疫活性细胞和上皮细胞之间相互作用的发病机制,对外阴痛进行新的局部治疗。
J Pain Res. 2016 Oct 3;9:757-762. doi: 10.2147/JPR.S115407. eCollection 2016.
4
NRP-1 Receptor Expression Mismatch in Skin of Subjects with Experimental and Diabetic Small Fiber Neuropathy.实验性和糖尿病性小纤维神经病变患者皮肤中神经毡蛋白-1(NRP-1)受体表达失调
PLoS One. 2016 Sep 6;11(9):e0161441. doi: 10.1371/journal.pone.0161441. eCollection 2016.
5
Combination of pregabalin with duloxetine for fibromyalgia: a randomized controlled trial.普瑞巴林与度洛西汀联合治疗纤维肌痛:一项随机对照试验。
Pain. 2016 Jul;157(7):1532-40. doi: 10.1097/j.pain.0000000000000558.
6
Topical prazosin attenuates sensitivity to tactile stimuli in patients with complex regional pain syndrome.局部用哌唑嗪可减轻复杂性区域疼痛综合征患者对触觉刺激的敏感性。
Eur J Pain. 2016 Jul;20(6):926-35. doi: 10.1002/ejp.817. Epub 2015 Nov 16.
7
A Novel Compound Analgesic Cream (Ketamine, Pentoxifylline, Clonidine, DMSO) for Complex Regional Pain Syndrome Patients.一种用于复杂性区域疼痛综合征患者的新型复方镇痛乳膏(氯胺酮、己酮可可碱、可乐定、二甲基亚砜)
Pain Pract. 2016 Jan;16(1):E14-20. doi: 10.1111/papr.12404. Epub 2015 Nov 7.
8
Combination of morphine with nortriptyline for neuropathic pain.吗啡与去甲替林联合用于治疗神经性疼痛。
Pain. 2015 Aug;156(8):1440-1448. doi: 10.1097/j.pain.0000000000000149.
9
Analgesic effects of topical ketamine.局部用氯胺酮的镇痛作用。
Minerva Anestesiol. 2015 Apr;81(4):440-9. Epub 2014 May 22.
10
A phase III randomized, placebo-controlled study of topical amitriptyline and ketamine for chemotherapy-induced peripheral neuropathy (CIPN): a University of Rochester CCOP study of 462 cancer survivors.一项关于局部应用阿米替林和氯胺酮治疗化疗引起的周围神经病变(CIPN)的 III 期随机、安慰剂对照研究:罗切斯特大学 CCOP 对 462 名癌症幸存者的研究。
Support Care Cancer. 2014 Jul;22(7):1807-14. doi: 10.1007/s00520-014-2158-7. Epub 2014 Feb 16.

局部用镇痛药研发中的瓶颈:分子、制剂、剂量确定及III期设计。

Bottlenecks in the development of topical analgesics: molecule, formulation, dose-finding, and phase III design.

作者信息

Keppel Hesselink Jan M, Kopsky David J, Stahl Stephen M

机构信息

Institute Neuropathic Pain, Bosch en Duin, the Netherlands.

Institute Neuropathic Pain, Amsterdam, the Netherlands.

出版信息

J Pain Res. 2017 Mar 20;10:635-641. doi: 10.2147/JPR.S131434. eCollection 2017.

DOI:10.2147/JPR.S131434
PMID:28360532
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5365321/
Abstract

Topical analgesics can be defined as topical formulations containing analgesics or co-analgesics. Since 2000, interest in such formulations has been on the rise. There are, however, four critical issues in the research and development phases of topical analgesics: 1) The selection of the active pharmaceutical ingredient. Analgesics and co-analgesics differ greatly in their mechanism of action, and it is required to find the most optimal fit between such mechanisms of action and the pathogenesis of the targeted (neuropathic) pain. 2) Issues concerning the optimized formulation. For relevant clinical efficacy, specific characteristics for the selected vehicle (eg, cream base or gel base) are required, depending on the physicochemical characteristics of the active pharmaceutical ingredient(s) to be delivered. 3) Well-designed phase II dose-finding studies are required, and, unfortunately, such trials are missing. In fact, we will demonstrate that underdosing is one of the major hurdles to detect meaningful and statistically relevant clinical effects of topical analgesics. 4) Selection of clinical end points and innovatively designed phase III trials. End point selection can make or break a trial. For instance, to include numbness together with tingling as a composite end point for neuropathic pain seems stretching the therapeutic impact of an analgesic too far. Given the fast onset of action of topical analgesics (usually within 30 minutes), enrichment designs might enhance the chances for success, as the placebo response might decrease. Topical analgesics may become promising inroads for the treatment of neuropathic pain, once sufficient attention is given to these four key aspects.

摘要

局部用镇痛药可定义为含有镇痛药或辅助镇痛药的局部用制剂。自2000年以来,人们对这类制剂的兴趣一直在上升。然而,局部用镇痛药的研发阶段存在四个关键问题:1)活性药物成分的选择。镇痛药和辅助镇痛药的作用机制差异很大,需要在这些作用机制与目标(神经性)疼痛的发病机制之间找到最优化的契合点。2)关于优化制剂的问题。为了获得相关的临床疗效,根据待递送的活性药物成分的理化特性,需要所选载体(如乳膏基质或凝胶基质)具有特定特性。3)需要精心设计的II期剂量探索研究,但遗憾的是,这类试验缺失。事实上,我们将证明给药不足是检测局部用镇痛药有意义且具有统计学相关性的临床效果的主要障碍之一。4)临床终点的选择和创新性设计的III期试验。终点的选择可以决定一项试验的成败。例如,将麻木和刺痛作为神经性疼痛的复合终点似乎过度延伸了镇痛药的治疗效果。鉴于局部用镇痛药起效快(通常在30分钟内),富集设计可能会增加成功的机会,因为安慰剂反应可能会降低。一旦对这四个关键方面给予足够关注,局部用镇痛药可能会成为治疗神经性疼痛的有前景的方法。