ART26.12, a novel fatty acid-binding protein 5 inhibitor, shows efficacy in multiple preclinical neuropathy models.

IF 3.5 2区 医学 Q1 ANESTHESIOLOGY
W G Warren, M Osborn, A David-Pereira, C Tsantoulas, Wenwen Xue, A Yates, S E OSullivan
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引用次数: 0

Abstract

Background: Painful neuropathy is a pathological condition caused by numerous factors including diabetes, chemotherapy or cancer. ART26.12 is a novel fatty acid-binding protein 5 inhibitor, which our group showed could prevent and treat persistent pain in a preclinical model of oxaliplatin-induced peripheral neuropathy.

Methods: In the current study, the efficacy of orally dosed ART26.12 was tested in multiple neuropathy models of different aetiology. Paw withdrawal threshold to von Frey monofilaments and latency to escape a cold plate were used as measurements of mechanical and cold sensitivity.

Results: ART26.12 (25 and 50 mg/kg BID), dosed prior to the induction of paclitaxel-induced peripheral neuropathy (PIPN), reversed mechanical allodynia induced by paclitaxel in both male and female rats, and ART26.12 (50 mg/kg BID) prevented the induction of PIPN in female rats. ART26.12 (50 mg/kg BID) also had a protective effect on body weight in the PIPN model. ART26.12 (25 and 100 mg/kg BID) reversed mechanical allodynia when treating established streptozotocin-induced diabetic neuropathy in male rats. In a model of breast cancer-induced bone pain in female rats, ART26.12 (100 mg/kg BID) reversed mechanical allodynia within 1 h of dosing. In the same model, ART26.12 (25 mg/kg BID) reversed mechanical allodynia from day 4 of treatment.

Conclusion: Overall, these preclinical data suggest that ART26.12 is a safe and efficacious therapeutic drug for continued development towards the prevention and treatment of peripheral neuropathy.

Significance statement: This work now shows that ART26.12, a novel and selective inhibitor of FABP5, can prevent and treat multiple preclinical models of peripheral neuropathy. Given its excellent safety profile, further work is warranted to develop ART26.12 as a potential therapeutic tool for pain management.

新型脂肪酸结合蛋白 5 抑制剂 ART26.12 在多个临床前神经病变模型中显示出疗效。
背景:疼痛性神经病变是由糖尿病、化疗或癌症等多种因素引起的一种病理状态。ART26.12是一种新型脂肪酸结合蛋白5抑制剂,我们的研究小组发现它可以在奥沙利铂诱导的外周神经病变临床前模型中预防和治疗持续性疼痛:本研究在多种不同病因的神经病变模型中测试了口服剂量 ART26.12 的疗效。结果:ART26.12(25 和 50 mg/kg)对阿克拉苷外周神经病变的疗效非常显著:结果:在诱导紫杉醇诱导的周围神经病变(PIPN)之前服用 ART26.12(25 和 50 mg/kg BID),可逆转雄性和雌性大鼠由紫杉醇诱导的机械异动症,ART26.12(50 mg/kg BID)可防止诱导雌性大鼠的 PIPN。在 PIPN 模型中,ART26.12(50 mg/kg BID)还对体重具有保护作用。在治疗链脲佐菌素诱导的糖尿病神经病变雄性大鼠时,ART26.12(25 毫克和 100 毫克/公斤,每日两次)可逆转机械异感。在乳腺癌诱导的雌性大鼠骨痛模型中,ART26.12(100 mg/kg BID)可在给药 1 小时内逆转机械异感。在同一模型中,ART26.12(25 mg/kg BID)从治疗第 4 天起逆转了机械异感:总之,这些临床前数据表明,ART26.12 是一种安全、有效的治疗药物,可继续开发用于预防和治疗周围神经病变:这项研究表明,ART26.12 是一种新型的 FABP5 选择性抑制剂,能够预防和治疗多种临床前模型的周围神经病。鉴于 ART26.12 极佳的安全性,有必要进一步将其开发为一种潜在的疼痛治疗工具。
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来源期刊
European Journal of Pain
European Journal of Pain 医学-临床神经学
CiteScore
7.50
自引率
5.60%
发文量
163
审稿时长
4-8 weeks
期刊介绍: European Journal of Pain (EJP) publishes clinical and basic science research papers relevant to all aspects of pain and its management, including specialties such as anaesthesia, dentistry, neurology and neurosurgery, orthopaedics, palliative care, pharmacology, physiology, psychiatry, psychology and rehabilitation; socio-economic aspects of pain are also covered. Regular sections in the journal are as follows: • Editorials and Commentaries • Position Papers and Guidelines • Reviews • Original Articles • Letters • Bookshelf The journal particularly welcomes clinical trials, which are published on an occasional basis. Research articles are published under the following subject headings: • Neurobiology • Neurology • Experimental Pharmacology • Clinical Pharmacology • Psychology • Behavioural Therapy • Epidemiology • Cancer Pain • Acute Pain • Clinical Trials.
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