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酵母聚糖诱导大鼠后爪炎症之前及期间,初级传入神经和脊髓背角神经元对热刺激和机械刺激的反应。

Responses of primary afferents and spinal dorsal horn neurons to thermal and mechanical stimuli before and during zymosan-induced inflammation of the rat hindpaw.

作者信息

Randich A, Meller S T, Gebhart G F

机构信息

Department of Psychology, University of Alabama at Birmingham, 35294, USA.

出版信息

Brain Res. 1997 Oct 24;772(1-2):135-48. doi: 10.1016/s0006-8993(97)00883-4.

DOI:10.1016/s0006-8993(97)00883-4
PMID:9406965
Abstract

Intraplantar administration of zymosan produces inflammation and results in behavioral evidence of hyperalgesia to mechanical and thermal stimuli in the rat. In the present studies, responses of primary afferents and spinal dorsal horn neurons to mechanical and thermal stimuli were examined before and during zymosan-induced inflammation of the hindpaw. In tests of responses of primary afferents to mechanical stimuli, group mean mechanical response thresholds of C-mechanonociceptor (CMN) units significantly decreased after zymosan administration. The group mean mechanical response thresholds of low threshold mechanoreceptor (LTM) units, A-mechanoheat (AMH) units, high threshold mechanoreceptor (HTM) units, and C-mechanoheat (CMH) units showed either no change or were increased significantly by intraplantar administration of zymosan. The group mean total discharges evoked during the 10 s mechanical stimulus were significantly increased after zymosan administration in CMN units. The group mean total discharges were either significantly decreased or unchanged in LTM, AMH, HTM, and CMH units. In tests of responses of spinal dorsal horn neurons to mechanical stimuli, the group mean mechanical response threshold of nociceptive specific (NS) units decreased significantly 1 h following administration of zymosan, whereas no significant changes occurred in the mechanical response thresholds of wide dynamic range (WDR) neurons in zymosan-injected rats, WDR neurons in saline-injected rats, or NS neurons in saline-injected rats. The group mean total discharges of only NS neurons were significantly increased during the 10 s mechanical stimulus 3 and 4 h after zymosan administration. In tests of responses of primary afferents to thermal stimuli, intraplantar administration of zymosan resulted in significant decreases in group mean response thresholds of CMH units and significant increases in group mean response thresholds of AMH units. The group mean total discharges of CMH units was either unchanged or significantly increased during thermal stimuli depending on both the time of testing and the temperature of the test stimulus. The group mean total number of discharges of AMH units was significantly decreased during tests of all thermal stimuli. In tests of responses of spinal dorsal horn neurons to thermal stimuli, intraplantar administration of zymosan resulted in significant decreases in thermal response thresholds of both WDR and NS units of zymosan-injected rats, but no changes in WDR and NS units of saline-injected rats. The group mean total discharges evoked by the 15 s thermal stimuli also increased significantly in both WDR and NS units after zymosan administration. Zymosan administration resulted in increased background activity only in CMH units. These increases occurred immediately following the injection and dissipated by the first hourly test period. Significant changes in background discharges of both WDR and NS units occurred at some hourly test intervals following administration of zymosan, but these changes were not consistent with respect to either unit type or modality of the test stimulus. These data suggest that the zymosan-induced hyperalgesia to mechanical stimuli observed in behavioral studies reflects decreases in response thresholds of peripheral CMN units and spinal NS neurons. Hyperalgesia to thermal stimuli reflects decreases in response thresholds of peripheral CMH units, spinal WDR neurons, and spinal NS neurons. These data support the view that different physiological substrates mediate hyperalgesia to either thermal or mechanical stimuli following intraplantar administration of zymosan.

摘要

在大鼠足底注射酵母聚糖会引发炎症,并导致对机械和热刺激出现痛觉过敏的行为表现。在本研究中,我们检测了酵母聚糖诱导后爪炎症发生之前及期间,初级传入神经和脊髓背角神经元对机械和热刺激的反应。在初级传入神经对机械刺激的反应测试中,注射酵母聚糖后,C类机械伤害性感受器(CMN)单位的组平均机械反应阈值显著降低。低阈值机械感受器(LTM)单位、A类机械热感受器(AMH)单位、高阈值机械感受器(HTM)单位和C类机械热感受器(CMH)单位的组平均机械反应阈值,在足底注射酵母聚糖后要么没有变化,要么显著升高。在10秒机械刺激期间,CMN单位在注射酵母聚糖后的组平均总放电量显著增加。LTM、AMH、HTM和CMH单位的组平均总放电量要么显著减少,要么没有变化。在脊髓背角神经元对机械刺激的反应测试中,注射酵母聚糖1小时后,伤害性特异性(NS)单位的组平均机械反应阈值显著降低,而在注射酵母聚糖的大鼠中,广动力范围(WDR)神经元、注射生理盐水的大鼠中的WDR神经元或注射生理盐水的大鼠中的NS神经元的机械反应阈值没有显著变化。仅NS神经元在注射酵母聚糖后3小时和4小时的10秒机械刺激期间,组平均总放电量显著增加。在初级传入神经对热刺激的反应测试中,足底注射酵母聚糖导致CMH单位的组平均反应阈值显著降低,而AMH单位的组平均反应阈值显著升高。根据测试时间和测试刺激温度的不同,CMH单位在热刺激期间的组平均总放电量要么没有变化,要么显著增加。在所有热刺激测试中,AMH单位的组平均总放电次数显著减少。在脊髓背角神经元对热刺激的反应测试中,足底注射酵母聚糖导致注射酵母聚糖的大鼠的WDR和NS单位的热反应阈值显著降低,但注射生理盐水的大鼠的WDR和NS单位没有变化。注射酵母聚糖后,15秒热刺激引发的WDR和NS单位的组平均总放电量也显著增加。酵母聚糖注射仅导致CMH单位的背景活动增加。这些增加在注射后立即出现,并在第一个小时的测试期消散。在注射酵母聚糖后的一些小时测试间隔中,WDR和NS单位的背景放电出现了显著变化,但这些变化在单位类型或测试刺激模式方面并不一致。这些数据表明,行为研究中观察到的酵母聚糖诱导的对机械刺激的痛觉过敏反映了外周CMN单位和脊髓NS神经元反应阈值的降低。对热刺激的痛觉过敏反映了外周CMH单位、脊髓WDR神经元和脊髓NS神经元反应阈值的降低。这些数据支持这样一种观点,即不同的生理底物介导了足底注射酵母聚糖后对热或机械刺激的痛觉过敏。

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