Rivera-García Luis G, Francis-Malavé Adela M, Castillo Zachary W, Uong Calvin D, Wilson Torri D, Ferchmin P A, Eterovic Vesna, Burton Michael D, Carrasquillo Yarimar
Division of Intramural Research National Center for Complementary and Integrative Health, 35 Convent Drive, Building 35A / Room 1E-410, Bethesda, MD, 20892, USA.
Department of Neuroscience, Universidad Central Del Caribe School of Medicine, Bayamon, Puerto Rico, USA.
J Inflamm (Lond). 2024 Jan 24;21(1):2. doi: 10.1186/s12950-023-00373-8.
4R is a tobacco cembranoid that binds to and modulates cholinergic receptors and exhibits neuroprotective and anti-inflammatory activity. Given the established function of the cholinergic system in pain and inflammation, we propose that 4R is also analgesic. Here, we tested the hypothesis that systemic 4R treatment decreases pain-related behaviors and peripheral inflammation via modulation of the alpha 7 nicotinic acetylcholine receptors (α7 nAChRs) in a mouse model of inflammatory pain. We elicited inflammation by injecting Complete Freund's Adjuvant (CFA) into the hind paw of male and female mice. We then assessed inflammation-induced hypersensitivity to cold, heat, and tactile stimulation using the Acetone, Hargreaves, and von Frey tests, respectively, before and at different time points (2.5 h - 8d) after a single systemic 4R (or vehicle) administration. We evaluated the contribution of α7 nAChRs 4R-mediated analgesia by pre-treating mice with a selective antagonist of α7 nAChRs followed by 4R (or vehicle) administration prior to behavioral tests. We assessed CFA-induced paw edema and inflammation by measuring paw thickness and quantifying immune cell infiltration in the injected hind paw using hematoxylin and eosin staining. Lastly, we performed immunohistochemical and flow cytometric analyses of paw skin in α7 nAChR-cre::Ai9 mice to measure the expression of α7 nAChRs on immune subsets. Our experiments show that systemic administration of 4R decreases inflammation-induced peripheral hypersensitivity in male and female mice and inflammation-induced paw edema in male but not female mice. Notably, 4R-mediated analgesia and anti-inflammatory effects lasted up to 8d after a single systemic administration on day 1. Pretreatment with an α7 nAChR-selective antagonist prevented 4R-mediated analgesia and anti-inflammatory effects, demonstrating that 4R effects are via modulation of α7 nAChRs. We further show that a subset of immune cells in the hind paw expresses α7 nAChRs. However, the number of α7 nAChR-expressing immune cells is unaltered by CFA or 4R treatment, suggesting that 4R effects are independent of α7 nAChR-expressing immune cells. Together, our findings identify a novel function of the 4R tobacco cembranoid as an analgesic agent in both male and female mice that reduces peripheral inflammation in a sex-dependent manner, further supporting the pharmacological targeting of the cholinergic system for pain treatment.
4R是一种烟草西柏烷类化合物,它能与胆碱能受体结合并对其进行调节,具有神经保护和抗炎活性。鉴于胆碱能系统在疼痛和炎症中的既定功能,我们提出4R也具有镇痛作用。在此,我们测试了以下假设:在炎症性疼痛小鼠模型中,全身性给予4R可通过调节α7烟碱型乙酰胆碱受体(α7 nAChRs)来减少疼痛相关行为和外周炎症。我们通过向雄性和雌性小鼠的后爪注射完全弗氏佐剂(CFA)来引发炎症。然后,在单次全身性给予4R(或赋形剂)之前以及给药后不同时间点(2.5小时 - 8天),分别使用丙酮试验、哈格里夫斯试验和von Frey试验评估炎症诱导的对冷、热和触觉刺激的超敏反应。我们通过在行为测试前用α7 nAChRs的选择性拮抗剂预处理小鼠,然后给予4R(或赋形剂),来评估α7 nAChRs在4R介导的镇痛中的作用。我们通过测量爪厚度并使用苏木精和伊红染色对注射后爪中的免疫细胞浸润进行定量,来评估CFA诱导的爪水肿和炎症。最后,我们对α7 nAChR-cre::Ai9小鼠的爪皮肤进行免疫组织化学和流式细胞术分析,以测量免疫亚群上α7 nAChRs的表达。我们的实验表明,全身性给予4R可降低雄性和雌性小鼠炎症诱导的外周超敏反应,以及雄性小鼠炎症诱导的爪水肿,但对雌性小鼠无效。值得注意的是,在第1天单次全身性给药后,4R介导的镇痛和抗炎作用可持续长达8天。用α7 nAChR选择性拮抗剂预处理可阻止4R介导的镇痛和抗炎作用,表明4R的作用是通过调节α7 nAChRs实现的。我们进一步表明,后爪中的一部分免疫细胞表达α7 nAChRs。然而,CFA或4R处理并未改变表达α7 nAChRs的免疫细胞数量,这表明4R的作用独立于表达α7 nAChRs的免疫细胞。总之,我们的研究结果确定了4R烟草西柏烷类化合物在雄性和雌性小鼠中作为镇痛剂的新功能,它以性别依赖的方式减轻外周炎症,进一步支持了将胆碱能系统作为疼痛治疗的药理学靶点。
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