Tabata Mitsuyasu, Terayama Ryuji, Maruhama Kotaro, Iida Seiji, Sugimoto Tomosada
a Department of Oral Function and Anatomy , Okayama University Graduate School of Medicine , Dentistry and Pharmaceutical Sciences , Okayama , Japan.
b Department of Oral and Maxillofacial Reconstructive Surgery , Okayama University Graduate School of Medicine , Dentistry and Pharmaceutical Sciences , Okayama , Japan.
Int J Neurosci. 2018 Mar;128(3):208-218. doi: 10.1080/00207454.2017.1381697. Epub 2017 Oct 2.
In this study, we compared induction of c-Fos and phosphorylated extracellular signal-regulated kinase (p-ERK) in the spinal dorsal horn after peripheral nerve injury.
We examined the spinal dorsal horn for noxious heat-induced c-Fos and p-ERK protein-like immunoreactive (c-Fos- and p-ERK-IR) neuron profiles after tibial nerve injury. The effect of administration of a MEK 1/2 inhibitor (PD98059) on noxious heat-induced c-Fos expression was also examined after tibial nerve injury.
A large number of c-Fos- and p-ERK-IR neuron profiles were induced by noxious heat stimulation to the hindpaw in sham-operated animals. A marked reduction in the number of c-Fos- and p-ERK-IR neuron profiles was observed in the medial 1/3 (tibial territory) of the dorsal horn at 3 and 7 days after nerve injury. Although c-Fos-IR neuron profiles had reappeared by 14 days after injury, the number of p-ERK-IR neuron profiles remained decreased in the tibial territory of the superficial dorsal horn. Double immunofluorescence labeling for c-Fos and p-ERK induced by noxious heat stimulation to the hindpaw at different time points revealed that a large number of c-Fos-IR, but not p-ERK-IR, neuron profiles were distributed in the tibial territory after injury. Although administration of a MEK 1/2 inhibitor to the spinal cord suppressed noxious heat-induced c-Fos expression in the peroneal territory, this treatment did not alter c-Fos induction in the tibial territory after nerve injury.
ERK phosphorylation may be involved in c-Fos induction in normal nociceptive responses, but not in exaggerated c-Fos induction after nerve injury.
在本研究中,我们比较了外周神经损伤后脊髓背角中c-Fos和磷酸化细胞外信号调节激酶(p-ERK)的诱导情况。
我们在胫神经损伤后,检测了脊髓背角中有害热诱导的c-Fos和p-ERK蛋白样免疫反应性(c-Fos-和p-ERK-IR)神经元分布情况。还检测了给予MEK 1/2抑制剂(PD98059)对胫神经损伤后有害热诱导的c-Fos表达的影响。
在假手术动物中,后爪受到有害热刺激可诱导大量c-Fos-和p-ERK-IR神经元分布。在神经损伤后3天和7天,在背角内侧1/3(胫神经分布区域)观察到c-Fos-和p-ERK-IR神经元分布数量显著减少。虽然损伤后14天c-Fos-IR神经元分布已重新出现,但浅表背角胫神经分布区域的p-ERK-IR神经元分布数量仍减少。对不同时间点后爪有害热刺激诱导的c-Fos和p-ERK进行双重免疫荧光标记显示,损伤后大量c-Fos-IR神经元分布于胫神经分布区域,但p-ERK-IR神经元分布较少。虽然向脊髓给予MEK 1/2抑制剂可抑制有害热诱导的腓总神经分布区域的c-Fos表达,但该处理并未改变神经损伤后胫神经分布区域的c-Fos诱导情况。
ERK磷酸化可能参与正常伤害性反应中的c-Fos诱导,但不参与神经损伤后过度的c-Fos诱导。
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