Washabau R J, Fudge M, Price W J, Barone F C
Department of Clinical Studies, School of Veterinary Medicine, University of Pennsylvania, Philadelphia 19104-6010, USA.
Brain Res Bull. 1995;38(6):587-94. doi: 10.1016/0361-9230(95)02038-7.
Gamma-aminobutyric acid (GABA) antagonist (bicuculline methiodide, BIC; picrotoxin, PIC) or agonist (muscimol, MUS) microinjections were made into the dorsal motor nucleus of the vagus nerve (DMV), and effects on lower esophageal sphincter pressure (LESP), gastric motility, and gastric acid secretion were determined in chloralose-anesthetized cats. Right or left DMV sites were microinjected with BIC, PIC, MUS, or isotonic tonic saline (140 nl) through a glass micropipette having a tip diameter of 15-21 microns. Esophageal body, LESP, and gastric fundic pressures were measured manometrically. Circular smooth muscle contractions of the antrum and pylorus were recorded with strain-gauge force transducers. Gastric acid secretion was measured every 15 min through a gastric cannula and titrated to pH 7.0. DMV microinjection sites were verified histologically. Direct BIC microinjections (0.275 or 0.550 nmol) into the DMV primarily produced a decrease in LESP (71% of all sites tested), with mean LESP changing from 23.2 +/- 1.7 mmHg to 3.7 +/- 0.7 mmHg (p < 0.01). Tonic LESP increases and phasic LESP contractile activity occurred less frequently. BIC-induced LESP responses were abolished by vagotomy or by microinjections of MUS (0.5 to 10 nmol) into the DMV. Direct PIC microinjection (0.232 nmol) into the DMV produced a pattern of responses similar to those observed with BIC (which were also abolished by vagotomy or by MUS microinjections into the DMV). The antrum and pylorus were also responsive to DMV microinjections of both GABA antagonists. Microinjections of BIC or PIC into the DMV produced increases in gastric circular muscle activity that occurred less frequently than LESP effects, but also were eliminated by vagotomy. The high (0.550 nmol) dose of BIC increased gastric motility significantly more often than the low dose of BIC (p < 0.05). In addition, BIC (0.550 nmol) microinjections into the DMV increased gastric secretory volume (from 0.6 +/- 0.2 to 6.0 +/- 2.5 ml/15 min; p < 0.01) and total titratible acid (from 34.4 +/- 8.9 to 86.0 +/- 19.1 mEq/15 min; p < 0.01), and decreased gastric pH (from 4.63 +/- 0.44 to 3.50 +/- 0.49; p < 0.05). Vagotomy also eliminated the gastric secretory effects of DMV BIC. Direct microinjections of MUS into the DMV also blocked BIC- or PIC-induced changes in gastric motility and/or gastric acid secretion. Isotonic saline microinjected into the DMV did not increase basal or decrease stimulated gastric esophageal motility or gastric secretion. These data indicate that LESP, gastric motility, and gastric secretion are influenced by a tonic DMV inhibition mediated by GABAA receptor stimulation of the DMV. Because disinhibition of these receptors clearly activates the upper gut, future work should focus on identifying the nuclei providing this synaptic input to the DMV that might be involved in the functional regulation of upper gut motor and secretory function.
向氯醛糖麻醉的猫的迷走神经背运动核(DMV)内微量注射γ-氨基丁酸(GABA)拮抗剂(碘化荷包牡丹碱,BIC;印防己毒素,PIC)或激动剂(蝇蕈醇,MUS),并测定其对食管下括约肌压力(LESP)、胃动力和胃酸分泌的影响。通过尖端直径为15 - 21微米的玻璃微量移液管,将BIC、PIC、MUS或等渗生理盐水(140 nl)微量注射到右侧或左侧DMV部位。通过测压法测量食管体、LESP和胃底压力。用应变片式力传感器记录胃窦和幽门的环形平滑肌收缩。每隔15分钟通过胃插管测量胃酸分泌,并滴定至pH 7.0。通过组织学方法验证DMV微量注射部位。向DMV直接微量注射BIC(0.275或0.550 nmol)主要导致LESP降低(在所有测试部位中占71%),平均LESP从23.2±1.7 mmHg变为3.7±0.7 mmHg(p < 0.01)。LESP的张力性增加和相位性收缩活动发生频率较低。切断迷走神经或向DMV微量注射MUS(0.5至10 nmol)可消除BIC诱导的LESP反应。向DMV直接微量注射PIC(0.232 nmol)产生的反应模式与BIC相似(切断迷走神经或向DMV微量注射MUS也可消除这些反应)。胃窦和幽门对DMV微量注射两种GABA拮抗剂也有反应。向DMV微量注射BIC或PIC会使胃环形肌活动增加,但其发生频率低于对LESP的影响,且切断迷走神经也可消除这种影响。高剂量(0.550 nmol)的BIC比低剂量的BIC更常显著增加胃动力(p < 0.05)。此外,向DMV微量注射BIC(0.550 nmol)会增加胃酸分泌量(从0.6±0.2增加到6.0±2.5 ml/15分钟;p < 0.01)和总可滴定酸(从34.4±8.9增加到86.0±19.1 mEq/15分钟;p < 0.01),并降低胃pH(从4.63±0.44降低到3.50±0.49;p < 0.05)。切断迷走神经也可消除DMV中BIC对胃酸分泌的影响。向DMV直接微量注射MUS也可阻断BIC或PIC诱导的胃动力和/或胃酸分泌变化。向DMV微量注射等渗生理盐水不会增加基础状态下的或降低刺激后的胃食管动力或胃酸分泌。这些数据表明,LESP、胃动力和胃酸分泌受DMV中由GABAA受体刺激介导的紧张性抑制的影响。由于这些受体的去抑制明显激活上消化道,未来的工作应集中于确定向DMV提供这种突触输入的核团,这些核团可能参与上消化道运动和分泌功能的功能调节。
