Manitpisitkul Prasarn, Flores Christopher M, Moyer John A, Romano Gary, Shalayda Kevin, Tatikola Kanaka, Hutchison James S, Mayorga Arthur J
Janssen Research and Development, LLC, NJ, USA.
Neuroscience Therapeutic Area, Janssen Research and Development, LLC, NJ, USA, Tel.: 609-730-6779.
Scand J Pain. 2018 Apr 25;18(2):151-164. doi: 10.1515/sjpain-2017-0184.
This double-blind (DB), randomized, placebo-controlled, sequential-group, multiple-ascending dose, phase 1 study evaluated safety, pharmacokinetics and pharmacodynamics of JNJ-39439335 in healthy men (part 1), and in participants with knee osteoarthritis (part 2).
Both parts 1 and 2 consisted of screening (upto 21 days), 21-day DB treatment phase [eight participants/group: JNJ-39439335 (part 1: 2-50 mg; part 2: 10-50 mg): n=6; placebo: n=2] and follow-up (total study duration ~10 weeks).
Plasma concentrations and systemic exposure of JNJ-39439335 increased in slightly higher than dose-proportional fashion (steady-state reached by day 14). Renal excretion of JNJ-39439335 was negligible. Marked dose-related increases in pharmacodynamic heat pain assessments were observed in JNJ-39439335-treated participants, which persisted throughout the treatment with no signs of tolerance with repeated dosing. No effect on pharmacodynamic cold pain or mechanical pain assessments were seen. Effects on pharmacodynamic capsaicin-induced flare assessments in JNJ-39439335-treated participants versus placebo were consistent with effects observed with single-dose, and did not demonstrate tolerance with multiple dosing. In participants with knee osteoarthritis, significant improvements versus placebo were observed in a stair-climbing-induced pain model. All JNJ-39439335-treated participants reported ≥1 treatment-emergent adverse events (TEAE); most common (≥50% incidence) TEAEs in part 1 were feeling hot (79%), thermohypoesthesia (71%), paresthesia (58%) and feeling cold (50%), and in part 2, were minor thermal burns (50%).
JNJ-39439335 (doses 2-50 mg) was well-tolerated, and associated with acceptable multiple-dose pharmacokinetic profile. JNJ-39439335 demonstrated sustained pharmacodynamic effects (heat pain perception, heat pain latency, capsaicin-induced flare), and an efficacy signal in participants with osteoarthritis pain.
Given the efficacy signal observed and the unique safety profile, larger phase 2 studies are needed to better understand the potential of JNJ-39439335 in the treatment of chronic pain. Analgesic efficacy of lower doses administered over a longer period of time and improved patient counseling techniques to reduce the minor thermal burns can be explored to minimize the adverse events.
这项双盲(DB)、随机、安慰剂对照、序贯分组、多剂量递增的1期研究评估了JNJ-39439335在健康男性(第1部分)和膝骨关节炎参与者(第2部分)中的安全性、药代动力学和药效学。
第1部分和第2部分均包括筛查(最长21天)、21天的双盲治疗阶段[每组8名参与者:JNJ-39439335(第1部分:2 - 50毫克;第2部分:10 - 50毫克):n = 6;安慰剂:n = 2]和随访(总研究持续时间约10周)。
JNJ-39439335的血浆浓度和全身暴露量以略高于剂量比例的方式增加(在第14天达到稳态)。JNJ-39439335的肾排泄可忽略不计。在接受JNJ-39439335治疗的参与者中,药效学热痛评估出现明显的剂量相关增加,在整个治疗过程中持续存在,且重复给药无耐受迹象。对药效学冷痛或机械痛评估未见影响。与安慰剂相比,JNJ-39439335治疗的参与者对药效学辣椒素诱导的红斑评估的影响与单剂量观察到的影响一致,且多剂量给药未显示耐受。在膝骨关节炎参与者中,在爬楼梯诱导的疼痛模型中观察到与安慰剂相比有显著改善。所有接受JNJ-39439335治疗的参与者均报告了≥1次治疗中出现的不良事件(TEAE);第1部分中最常见(发生率≥50%)的TEAE是感觉热(79%)、热感觉减退(71%)、感觉异常(58%)和感觉冷(50%),第2部分中是轻微热灼伤(50%)。
JNJ-39439335(剂量2 - 50毫克)耐受性良好,且具有可接受的多剂量药代动力学特征。JNJ-39439335表现出持续的药效学作用(热痛觉、热痛潜伏期、辣椒素诱导的红斑),以及在骨关节炎疼痛参与者中的疗效信号。
鉴于观察到的疗效信号和独特的安全性特征,需要进行更大规模的2期研究以更好地了解JNJ-39439335在治疗慢性疼痛方面的潜力。可以探索长时间给予较低剂量的镇痛效果以及改进患者咨询技巧以减少轻微热灼伤,从而尽量减少不良事件。
