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Allosteric Cannabinoid Receptor 1 (CB1) Ligands Reduce Ocular Pain and Inflammation

机译:变构大麻素受体1(CB1)配体减少眼部疼痛和炎症

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Cannabinoid receptor 1 (CB1) activation has been reported to reduce transient receptor potential cation channel subfamily V member 1 (TRPV1)-induced inflammatory responses and is anti-nociceptive and anti-inflammatory in corneal injury. We examined whether allosteric ligands, can modulate CB1 signaling to reduce pain and inflammation in corneal hyperalgesia. Corneal hyperalgesia was generated by chemical cauterization of cornea in wildtype and CB2 knockout (CB2?/?) mice. The novel racemic CB1 allosteric ligand GAT211 and its enantiomers GAT228 and GAT229 were examined alone or in combination with the orthosteric CB1 agonist Δ8-tetrahydrocannabinol (Δ8-THC). Pain responses were assessed following capsaicin (1 μM) stimulation of injured corneas at 6 h post-cauterization. Corneal neutrophil infiltration was also analyzed. GAT228, but not GAT229 or GAT211, reduced pain scores in response to capsaicin stimulation. Combination treatments of 0.5% GAT229 or 1% GAT211 with subthreshold Δ8-THC (0.4%) significantly reduced pain scores following capsaicin stimulation. The anti-nociceptive effects of both GAT229 and GAT228 were blocked with CB1 antagonist AM251, but remained unaffected in CB2?/? mice. Two percent GAT228, or the combination of 0.2% Δ8-THC with 0.5% GAT229 also significantly reduced corneal inflammation. CB1 allosteric ligands could offer a novel approach for treating corneal pain and inflammation.
机译:据报道,大麻素受体1(CB1)活化以减少瞬时受体电位阳离子通道亚家族V成分1(TRPV1)诱导炎症反应,并且是角膜损伤的抗伤害和抗炎。我们检查了仿生配体是否可以调节CB1信号,以减少角膜痛觉症的疼痛和炎症。角膜痛觉型是通过野生型和CB2敲除(CB2?/α)小鼠的角膜的化学腐蚀产生的。单独或与骨髓CB1激动剂δ8-四氢甘油(Δ8-THC)组合检查新型外消旋CB1颠振配体GAT211及其对映体GAT228和GAT229。在腐蚀后6小时,辣椒素(1μm)刺激后辣椒素(1μm)刺激评估疼痛反应。还分析了角膜中性粒细胞浸润。 GAT228,但不是GAT229或GAT211,响应辣椒素刺激而降低疼痛评分。用亚阈值Δ8-THC的0.5%GAT229或1%GAT211的组合处理(0.4%)显着降低辣椒素刺激后的疼痛评分。 GAT229和GAT228的抗伤害效果被CB1拮抗剂AM251封闭,但在CB2中保持不受影响?/?老鼠。两个百分比GAT228,或0.2%Δ8-THC的组合,0.5%GAT229也显着降低了角膜炎症。 CB1颠振配体可以提供一种治疗角膜疼痛和炎症的新方法。

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