Instituto de Neurociencias de Alicante, Universidad Miguel Hernández-CSIC, 03550 San Juan de Alicante, Spain.
Instituto Universitario Fernández-Vega, Universidad de Oviedo & Fundación de Investigación Oftalmológica, Oviedo, Spain, and.
J Neurosci. 2019 Feb 6;39(6):949-969. doi: 10.1523/JNEUROSCI.1726-18.2018. Epub 2018 Dec 13.
TRPM8 is a polymodal, nonselective cation channel activated by cold temperature and cooling agents that plays a critical role in the detection of environmental cold. We found that TRPM8 is a pharmacological target of tacrolimus (FK506), a macrolide immunosuppressant with several clinical uses, including the treatment of organ rejection following transplants, treatment of atopic dermatitis, and dry eye disease. Tacrolimus is an inhibitor of the phosphatase calcineurin, an action shared with cyclosporine. Tacrolimus activates TRPM8 channels in different species, including humans, and sensitizes their response to cold temperature by inducing a leftward shift in the voltage-dependent activation curve. The effects of tacrolimus on purified TRPM8 in lipid bilayers demonstrates conclusively that it has a direct gating effect. Moreover, the lack of effect of cyclosporine rules out the canonical signaling pathway involving the phosphatase calcineurin. Menthol (TRPM8-Y745H)- and icilin (TRPM8-N799A)-insensitive mutants were also activated by tacrolimus, suggesting a different binding site. In cultured mouse DRG neurons, tacrolimus evokes an increase in intracellular calcium almost exclusively in cold-sensitive neurons, and these responses were drastically blunted in mice or after the application of TRPM8 antagonists. Cutaneous and corneal cold thermoreceptor endings are also activated by tacrolimus, and tacrolimus solutions trigger blinking and cold-evoked behaviors. Together, our results identify TRPM8 channels in sensory neurons as molecular targets of the immunosuppressant tacrolimus. The actions of tacrolimus on TRPM8 resemble those of menthol but likely involve interactions with other channel residues. TRPM8 is a polymodal TRP channel involved in cold temperature sensing, thermoregulation, and cold pain. TRPM8 is also involved in the pathophysiology of dry eye disease, and TRPM8 activation has antiallodynic and antipruritic effects, making it a prime therapeutic target in several cutaneous and neural diseases. We report the direct agonist effect of tacrolimus, a potent natural immunosuppressant with multiple clinical applications, on TRPM8 activity. This interaction represents a novel neuroimmune interface. The identification of a clinically approved drug with agonist activity on TRPM8 channels could be used experimentally to probe the function of TRPM8 in humans. Our findings may explain some of the sensory and anti-inflammatory effects described for this drug in the skin and the eye surface.
瞬时受体电位阳离子通道亚家族 M 成员 8(TRPM8)是一种多模式非选择性阳离子通道,可被低温和冷却剂激活,在环境冷觉检测中发挥关键作用。我们发现,TRPM8 是他克莫司(FK506)的药理学靶点,他克莫司是一种大环内酯类免疫抑制剂,具有多种临床用途,包括治疗移植后的器官排斥反应、治疗特应性皮炎和干眼症。他克莫司是钙调神经磷酸酶的抑制剂,这与环孢素的作用相同。他克莫司激活包括人类在内的不同物种的 TRPM8 通道,并通过诱导电压依赖性激活曲线向左移来敏化其对冷温度的反应。他克莫司在脂质双层中对纯化的 TRPM8 的作用表明它具有直接的门控作用。此外,环孢素缺乏作用排除了涉及磷酸酶钙调神经磷酸酶的经典信号通路。薄荷醇(TRPM8-Y745H)和异丁香酚(TRPM8-N799A)不敏感突变体也被他克莫司激活,这表明存在不同的结合位点。在培养的小鼠背根神经节神经元中,他克莫司几乎仅在冷敏感神经元中引起细胞内钙增加,并且在 小鼠或应用 TRPM8 拮抗剂后,这些反应明显减弱。皮肤和角膜冷感受器末端也被他克莫司激活,他克莫司溶液引发眨眼和冷诱发行为。总之,我们的研究结果将感觉神经元中的 TRPM8 通道确定为免疫抑制剂他克莫司的分子靶标。他克莫司对 TRPM8 的作用类似于薄荷醇,但可能涉及与其他通道残基的相互作用。TRPM8 是一种多模式的 TRP 通道,参与冷温度感知、体温调节和冷痛。TRPM8 还参与干眼症的病理生理学,TRPM8 的激活具有抗痛觉过敏和止痒作用,使其成为几种皮肤和神经疾病的主要治疗靶点。我们报告了一种具有多种临床应用的强效天然免疫抑制剂他克莫司对 TRPM8 活性的直接激动剂作用。这种相互作用代表了一种新的神经免疫界面。具有 TRPM8 通道激动剂活性的临床批准药物的鉴定可用于实验性地研究 TRPM8 在人类中的功能。我们的发现可以解释在皮肤和眼表面描述的这种药物的一些感觉和抗炎作用。
