Hirschowitz B I, Molina E, Ou Tim L, Helman C
Dig Dis Sci. 1984 Sep;29(9):790-6. doi: 10.1007/BF01318420.
Muscarinic mechanisms in basal acid and pepsin secretion in man were quantitated by graded intravenous doses of atropine (1-16 micrograms/kg). Secretion was dose-responsively inhibited in six healthy controls. For the mean dose response, maximum inhibition (Imax) was 100%, and D50 (dose inhibiting 50%) was 0.31 +/- 0.06 and 0.93 +/- 0.13 micrograms/kg, respectively, for acid and pepsin. In 24 patients with duodenal ulcer (DU), calculated Imax was also 100%, and D50S were 1.2 +/- 0.27 and 1.7 +/- 0.3 micrograms/kg, respectively. The low D50 values and the 100% calculated maximum inhibition indicated that in both groups basal secretion was largely or completely cholinergic dependent. We also found that atropine raised heart rate in controls by 44 +/- 1 beats per min (bpm) (D50 = 6 +/- 1.1 micrograms/kg), while the mean maximum increase in DU was only 23 +/- 2 bpm (P less than 0.01) with (D50 = 5.3 +/- 1.0 micrograms/kg (NS)). In DU atropine increased fasting serum gastrin from 62 to 82 pg/ml (P less than 0.05); the increase in normals from 32 to 38 pg/ml was not significant. Thus, while both normals and DU exhibited the same qualitative responses to muscarinic receptor antagonism by atropine with respect to gastric secretion, gastrin levels, and heart rate, there were quantitative differences in all three parameters.
通过静脉注射不同剂量(1 - 16微克/千克)的阿托品,对人体基础胃酸和胃蛋白酶分泌中的毒蕈碱机制进行了定量研究。在6名健康对照者中,分泌呈剂量依赖性受到抑制。对于平均剂量反应,胃酸和胃蛋白酶的最大抑制率(Imax)均为100%,半数抑制剂量(D50)分别为0.31±0.06微克/千克和0.93±0.13微克/千克。在24名十二指肠溃疡(DU)患者中,计算得出的Imax同样为100%,D50分别为1.2±0.27微克/千克和1.7±0.3微克/千克。较低的D50值和100%的计算最大抑制率表明,两组的基础分泌在很大程度上或完全依赖胆碱能。我们还发现,阿托品使对照组心率每分钟提高44±1次(bpm)(D50 = 6±1.1微克/千克),而在DU患者中,平均最大心率增加仅为23±2次/分钟(P < 0.01),D50为5.3±1.0微克/千克(无显著性差异)。在DU患者中,阿托品使空腹血清胃泌素从62 pg/ml升高至82 pg/ml(P < 0.05);而正常组从32 pg/ml升高至38 pg/ml则无显著差异。因此,虽然正常人和DU患者在胃分泌、胃泌素水平和心率方面对阿托品拮抗毒蕈碱受体表现出相同的定性反应,但在这三个参数上存在定量差异。
