Department of Cell Biology, Neurobiology and Anatomy, Medical College of Wisconsin, Milwaukee, Wisconsin 53226.
Department of Cell Biology, Neurobiology and Anatomy, Medical College of Wisconsin, Milwaukee, Wisconsin 53226
J Neurosci. 2018 Jun 20;38(25):5807-5825. doi: 10.1523/JNEUROSCI.3565-17.2018.
Cutaneous somatosensory neurons convey innocuous and noxious mechanical, thermal, and chemical stimuli from peripheral tissues to the CNS. Among these are nociceptive neurons that express calcitonin gene-related peptide-α (CGRPα). The role of peripheral CGRPα neurons (CANs) in acute and injury-induced pain has been studied using diphtheria toxin ablation, but their functional roles remain controversial. Because ablation permanently deletes a neuronal population, compensatory changes may ensue that mask the physiological or pathophysiological roles of CANs, particularly for injuries that occur after ablation. Therefore, we sought to define the role of intact CANs under baseline and injury conditions by using noninvasive transient optogenetic inhibition. We assessed pain behavior longitudinally from acute to chronic time points. We generated adult male and female mice that selectively express the outward rectifying proton pump archaerhodopsin-3 (Arch) in CANs, and inhibited their peripheral cutaneous terminals in models of neuropathic (spared nerve injury) and inflammatory (skin-muscle incision) pain using transdermal light activation of Arch. After nerve injury, brief activation of Arch reversed the chronic mechanical, cold, and heat hypersensitivity, alleviated the spontaneous pain, and reversed the sensitized mechanical currents in primary afferent somata. In contrast, Arch inhibition of CANs did not alter incision-induced hypersensitivity. Instead, incision-induced mechanical and heat hypersensitivity was alleviated by peripheral blockade of CGRPα peptide-receptor signaling. These results reveal that CANs have distinct roles in the time course of pain during neuropathic and incisional injuries and suggest that targeting peripheral CANs or CGRPα peptide-receptor signaling could selectively treat neuropathic or postoperative pain, respectively. The contribution of sensory afferent CGRPα neurons (CANs) to neuropathic and inflammatory pain is controversial. Here, we left CANs intact during neuropathic and perioperative incision injury by using transient transdermal optogenetic inhibition of CANs. We found that peripheral CANs are required for neuropathic mechanical, cold, and heat hypersensitivity, spontaneous pain, and sensitization of mechanical currents in afferent somata. However, they are dispensable for incisional pain transmission. In contrast, peripheral pharmacological inhibition of CGRPα peptide-receptor signaling alleviated the incisional mechanical and heat hypersensitivity, but had no effect on neuropathic pain. These results show that CANs have distinct roles in neuropathic and incisional pain and suggest that their targeting via novel peripheral treatments may selectively alleviate neuropathic versus incisional pain.
皮肤躯体感觉神经元将无害和有害的机械、热和化学刺激从外周组织传递到中枢神经系统。其中包括表达降钙素基因相关肽-α (CGRPα) 的伤害感受神经元。使用白喉毒素消融术研究了外周 CGRPα 神经元 (CANs) 在急性和损伤诱导性疼痛中的作用,但它们的功能作用仍存在争议。因为消融术永久性地删除了一个神经元群体,所以可能会发生代偿性变化,从而掩盖 CANs 的生理或病理生理作用,特别是对于消融术之后发生的损伤。因此,我们试图通过非侵入性的短暂光遗传抑制来定义在基线和损伤条件下完整 CANs 的作用。我们从急性到慢性时间点纵向评估疼痛行为。我们生成了选择性地在 CANs 中表达外向整流质子泵 archerhodopsin-3 (Arch) 的成年雄性和雌性小鼠,并使用经皮光激活 Arch 在神经病理性 ( spared nerve injury, SNI) 和炎症性 (skin-muscle incision, SM incision) 疼痛模型中抑制其外周皮肤末端。在神经损伤后,短暂激活 Arch 逆转了慢性机械性、冷性和热性超敏反应,减轻了自发性疼痛,并逆转了初级传入体的敏化机械电流。相比之下,Arch 抑制 CANs 不会改变切口引起的超敏反应。相反,通过外周阻断 CGRPα 肽-受体信号转导可减轻切口引起的机械性和热超敏反应。这些结果表明,CANs 在神经病理性和切口性损伤过程中的疼痛时间进程中具有不同的作用,并表明针对外周 CANs 或 CGRPα 肽-受体信号转导可以分别选择性地治疗神经病理性或术后疼痛。感觉传入 CGRPα 神经元 (CANs) 对神经病理性和炎症性疼痛的贡献存在争议。在这里,我们通过短暂的经皮光遗传抑制 CANs 来保留神经病理性和围手术期切口损伤期间的 CANs。我们发现,外周 CANs 是神经病理性机械性、冷性和热性超敏反应、自发性疼痛以及传入体机械电流敏化所必需的。然而,它们对于切口疼痛传递是可有可无的。相反,外周药理学抑制 CGRPα 肽-受体信号转导减轻了切口的机械性和热超敏反应,但对神经病理性疼痛没有影响。这些结果表明,CANs 在神经病理性和切口性疼痛中具有不同的作用,并表明通过新的外周治疗靶向它们可能选择性地减轻神经病理性与切口性疼痛。
