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在大鼠神经病理性疼痛模型中,全身性联合使用 GlyT-1 和 GlyT-2 抑制剂增强抗痛觉过敏的药理学证据。

Pharmacological Evidence on Augmented Antiallodynia Following Systemic Co-Treatment with GlyT-1 and GlyT-2 Inhibitors in Rat Neuropathic Pain Model.

机构信息

Department of Pharmacology and Pharmacotherapy, Faculty of Medicine, Semmelweis University, Nagyvárad tér 4, P.O. Box 370, H-1445 Budapest, Hungary.

Department of Pharmacodynamics, Faculty of Pharmacy, Semmelweis University, Nagyvárad tér 4, H-1089 Budapest, Hungary.

出版信息

Int J Mol Sci. 2021 Mar 1;22(5):2479. doi: 10.3390/ijms22052479.

DOI:10.3390/ijms22052479
PMID:33804568
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7957511/
Abstract

The limited effect of current medications on neuropathic pain (NP) has initiated large efforts to develop effective treatments. Animal studies showed that glycine transporter (GlyT) inhibitors are promising analgesics in NP, though concerns regarding adverse effects were raised. We aimed to study NFPS and Org-25543, GlyT-1 and GlyT-2 inhibitors, respectively and their combination in rat mononeuropathic pain evoked by partial sciatic nerve ligation. Cerebrospinal fluid (CSF) glycine content was also determined by capillary electrophoresis. Subcutaneous (s.c.) 4 mg/kg NFPS or Org-25543 showed analgesia following acute administration (30-60 min). Small doses of each compound failed to produce antiallodynia up to 180 min after the acute administration. However, NFPS (1 mg/kg) produced antiallodynia after four days of treatment. Co-treatment with subanalgesic doses of NFPS (1 mg/kg) and Org-25543 (2 mg/kg) produced analgesia at 60 min and thereafter meanwhile increased significantly the CSF glycine content. This combination alleviated NP without affecting motor function. Test compounds failed to activate G-proteins in spinal cord. To the best of our knowledge for the first time we demonstrated augmented analgesia by combining GlyT-1 and 2 inhibitors. Increased CSF glycine content supports involvement of glycinergic system. Combining selective GlyT inhibitors or developing non-selective GlyT inhibitors might have therapeutic value in NP.

摘要

目前药物对神经病理性疼痛 (NP) 的疗效有限,这促使人们大力开发有效的治疗方法。动物研究表明,甘氨酸转运体 (GlyT) 抑制剂是 NP 有前途的镇痛药,但对其不良反应的担忧也随之产生。我们旨在研究 NFPS 和 Org-25543,分别是 GlyT-1 和 GlyT-2 抑制剂,并研究它们在部分坐骨神经结扎诱导的大鼠单神经病疼痛中的组合作用。还通过毛细管电泳测定脑脊液 (CSF) 中的甘氨酸含量。NFPS 或 Org-25543 的皮下 (s.c.) 4 mg/kg 剂量在急性给药后 30-60 分钟表现出镇痛作用。在急性给药后 180 分钟内,每种化合物的小剂量均未产生抗痛觉过敏作用。然而,NFPS (1 mg/kg) 在四天的治疗后产生了抗痛觉过敏作用。NFPS (1 mg/kg) 和 Org-25543 (2 mg/kg) 的亚治疗剂量联合治疗在 60 分钟后产生镇痛作用,同时 CSF 甘氨酸含量显著增加。这种组合缓解了 NP,而不影响运动功能。试验化合物未能在脊髓中激活 G 蛋白。据我们所知,这是首次证明通过联合使用 GlyT-1 和 2 抑制剂来增强镇痛作用。CSF 甘氨酸含量的增加支持甘氨酸能系统的参与。联合使用选择性 GlyT 抑制剂或开发非选择性 GlyT 抑制剂可能对 NP 具有治疗价值。

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