Hyperalgesic Effect Evoked by il-16 and its Participation in Inflammatory Hypernociception in Mice.

IF 6.2
Sara González-Rodríguez, Christian Sordo-Bahamonde, Alejandro Álvarez-Artime, Ana Baamonde, Luis Menéndez
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Abstract

The systemic administration of interleukin-16 (IL-16, 3-30 ng/kg) induced thermal hyperalgesia in mice, that was prevented by the acute injection of an anti-CD4 antibody (1 µg/kg), the depletion of circulating white blood cells by cyclophosphamide or the specific reduction of circulating CD4+ cells provoked by a high dose of an anti-CD4 antibody (30 µg/mouse, 24 h before). IL-16-induced hyperalgesia was locally inhibited after intraplantar (i.pl.) administration of the non-selective cyclooxygenase (COX) inhibitor diclofenac, the COX-1 inhibitor SC-560, the COX-2 inhibitor celecoxib, the TRPV1 antagonist capsazepine or the TRPA1 antagonist HC030031, thus demonstrating that prostaglandins and TRP channels are involved in this effect. The i.pl. administration of low doses of IL-16 (0.1-1 ng) evoked local hyperalgesia suggesting the possibility that IL-16 could participate in hypernociception associated to local tissue injury. Accordingly, IL-16 concentration measured by ELISA was increased in paws acutely inflamed with carrageenan or chronically inflamed with complete Freund´s adjuvant (CFA). This augmentation was reduced after white cell depletion with cyclophosphamide or neutrophil depletion with an anti-Ly6G antibody. Immunofluorescence and flow cytometry experiments showed that the increased concentration of IL-16 levels found in acutely inflamed paws is mainly related to the infiltration of IL-16+ neutrophils, although a reduced number of IL-16+ lymphocytes was also detected in paws inflamed with CFA. Supporting the functional role of IL-16 in inflammatory hypernociception, the administration of an anti-IL-16 antibody dose-dependently reduced carrageenan- and CFA-induced thermal hyperalgesia and mechanical allodynia. The interest of IL-16 as a target to counteract inflammatory pain is suggested.

Abstract Image

il-16诱发的小鼠痛觉减退效应及其在炎症性痛觉减退中的参与作用
全身注射白细胞介素-16(IL-16,3-30 纳克/千克)会诱发小鼠热痛,而急性注射抗 CD4 抗体(1 微克/千克)、环磷酰胺消耗循环白细胞或高剂量抗 CD4 抗体(30 微克/只小鼠,24 小时前)特异性减少循环 CD4+ 细胞均可阻止热痛。在跖内注射非选择性环氧化酶(COX)抑制剂双氯芬酸、COX-1抑制剂SC-560、COX-2抑制剂塞来昔布、TRPV1拮抗剂卡扎平或TRPA1拮抗剂HC030031后,IL-16诱导的局部痛感受到抑制,从而证明前列腺素和TRP通道参与了这种效应。静脉注射低剂量的 IL-16(0.1-1 纳克)会诱发局部痛觉减退,这表明 IL-16 有可能参与了与局部组织损伤相关的痛觉减退。因此,用 ELISA 测量的 IL-16 浓度在角叉菜胶急性发炎或完全弗氏佐剂(CFA)慢性发炎的爪子中都有所增加。用环磷酰胺清除白细胞或用抗 Ly6G 抗体清除中性粒细胞后,这种增高现象会减弱。免疫荧光和流式细胞术实验表明,在急性发炎的爪子中发现的IL-16浓度水平升高主要与IL-16+中性粒细胞的浸润有关,尽管在使用CFA发炎的爪子中也检测到了IL-16+淋巴细胞数量的减少。为了证实 IL-16 在炎症性痛觉减退中的功能性作用,服用抗 IL-16 抗体可剂量依赖性地减轻角叉菜胶和 CFA 引起的热痛觉减退和机械痛觉减退。研究人员认为,IL-16 是对抗炎症性疼痛的一个靶点。
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