Long-term Safety and Tolerability of NKTR-181 in Patients with Moderate to Severe Chronic Low Back Pain or Chronic Noncancer Pain: A Phase 3 Multicenter, Open-Label, 52-Week Study (SUMMIT-08 LTS)

Pain Medicine: The Official Journal of the American Academy of Pain Medicine Pub Date : 2019-07-30 DOI:10.1093/pm/pnz169

J. Gudin, R. Rauck, C. Argoff, Eva Agaiby, J. Gimbel, Nathaniel Katz, S. Doberstein, M. Tagliaferri, M. Tagliaferri, J. Potts, James E Wild, Lin Lu, S. Siddhanti, M. Hale, J. Markman

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引用次数: 11

Abstract

Abstract Objective To evaluate the long-term safety of NKTR-181, a novel mu-opioid receptor agonist that may have reduced human abuse potential, in patients with moderate to severe chronic low back pain (CLBP) or other chronic noncancer pain (CNP). Design Uncontrolled, multicenter, open-label, long-term study of NKTR-181 comprised of three periods: screening (≤21 days), treatment (52 weeks), and safety follow-up (∼14 days after the last dose of NKTR-181). Setting Multicenter, long-term clinical research study. Methods NKTR-181 administered at doses of 100–600 mg twice daily (BID) was evaluated in opioid-naïve and opioid-experienced patients. Patients were enrolled de novo or following completion of the randomized, placebo-controlled phase 3 efficacy study (SUMMIT-07). Safety assessments included adverse event documentation, measurements of opioid withdrawal, and clinical laboratory tests. Effectiveness was assessed using the modified Brief Pain Inventory Short Form (mBPI-SF). Results The study enrolled 638 patients. The most frequently reported treatment-emergent adverse events (TEAEs) were constipation (26%) and nausea (12%). Serious TEAEs, reported in 5% of patients, were deemed by investigators to be unrelated to NKTR-181. There were no deaths or reported cases of respiratory depression. A sustained reduction in mBPI-SF pain intensity and pain interference from baseline to study termination was observed throughout treatment. Only 2% of patients discontinued NKTR-181 due to lack of efficacy, and 11% discontinued due to treatment-related AEs. NKTR-181 doses of up to 600 mg BID were generally well tolerated, and patients experienced low rates of opioid-related adverse events. Conclusions The study results support the premise that NKTR-181 is a safe and effective option for patients with moderate to severe CLBP or CNP.

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NKTR-181治疗中重度慢性腰痛或慢性非癌性疼痛患者的长期安全性和耐受性:一项多中心、开放标签、52周的3期研究(顶08 LTS)

目的评价NKTR-181(一种新型的mu-阿片受体激动剂，可降低人类滥用的可能性)在中重度慢性腰痛(CLBP)或其他慢性非癌性疼痛(CNP)患者中的长期安全性。NKTR-181的非对照、多中心、开放标签、长期研究包括三个阶段:筛选(≤21天)、治疗(52周)和安全性随访(NKTR-181末次给药后~ 14天)。多中心、长期临床研究。方法观察NKTR-181在opioid-naïve和有阿片类药物经历的患者中给药100 ~ 600 mg，每日2次(BID)。患者是在从头开始或完成随机、安慰剂对照的3期疗效研究(SUMMIT-07)后入组的。安全性评估包括不良事件记录、阿片类药物戒断测量和临床实验室检查。使用改进的简短疼痛量表(mBPI-SF)评估疗效。结果共纳入638例患者。最常见的治疗不良事件(teae)是便秘(26%)和恶心(12%)。研究人员认为，5%的患者报告的严重teae与NKTR-181无关。没有死亡或报告的呼吸抑制病例。在整个治疗过程中，观察到mBPI-SF疼痛强度和疼痛干扰从基线到研究结束的持续降低。只有2%的患者因缺乏疗效而停用NKTR-181, 11%的患者因治疗相关不良反应而停用。NKTR-181高达600 mg BID的剂量通常耐受性良好，患者经历阿片类药物相关不良事件的发生率较低。研究结果支持NKTR-181是中重度CLBP或CNP患者安全有效的选择的前提。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Pain Medicine: The Official Journal of the American Academy of Pain Medicine

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