胆盐对体外胆囊运动影响的初步研究。

M F Stolk, B J Van de Heijning, K J Van Erpecum, A Verheem, L M Akkermans, G P Van Berge-Henegouwen
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引用次数: 0

摘要

餐后胆囊排空受损可能是胆固醇结晶沉淀和随后胆结石形成的重要因素。我们之前发现,与餐后胆囊收缩强烈(> 50%)的患者相比,餐后胆囊收缩弱(< 50%空腹容量)的胆结石患者胆汁中的胆盐浓度明显升高。因此,我们研究了不同相对疏水性的共轭和非共轭胆盐对胆囊切除术后胆囊肌条体外收缩力的潜在影响。条带与浓度为10(-8)-10(-4)M的胆盐孵育5分钟。测定了10(-3)M乙酰胆碱的作用,并与孵育前的控制值相关。所使用的胆汁盐,按照疏水性增加的顺序依次为:牛磺酸脱氧-、牛磺酸脱氧-、牛磺酸-、牛磺酸脱氧-和脱氧胆酸盐。熊脱氧胆酸盐和牛磺酸脱氧胆酸盐没有显著降低胆囊收缩力。牛磺胆酸盐在浓度为10(-6)M及以上、10(-7)M及以上和10(-5)M及以上时显著降低收缩力。胆盐浓度为10(-4)M时,乙酰胆碱10(-3)M诱导的收缩力分别为66.0 +/- 11.7%(牛磺胆酸盐)、50.2 +/- 6.2%(脱氧胆酸盐)和44.8 +/- 11.5%(牛磺胆酸盐)。胆盐的作用与其相对疏水性相关(r = -0.97;P < 0.01)。对胆囊肌条收缩力的抑制作用持续时间长,冲洗后仍能保持。结果表明,胆盐在生理剂量范围内对体外胆囊收缩有抑制作用。如果这一机制在体内存在,它可能对胆囊运动调节具有重要意义。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of bile salts on in vitro gallbladder motility: preliminary study.

Impaired postprandial gallbladder emptying may be an important factor in cholesterol crystals precipitation and subsequent gallstone formation. We previously found strongly increased bile salt concentrations in gallbladder bile of gallstone patients with weak (< 50% fasting volume) postprandial gallbladder contraction compared to patients with strong (> 50%) postprandial contraction. Therefore, we studied potential effects of various conjugated and unconjugated bile salts with different relative hydrophobicity on in vitro contractility of gallbladder muscle strips obtained at cholecystectomy. Strips were incubated 5 min with bile salt at concentrations of 10(-8)-10(-4)M. The effect of 10(-3)M acetylcholine was measured and related to preincubation control value. Bile salts used were, in order of increasing hydrophobicity: tauroursodeoxy-, ursodeoxy-, tauro-, taurodeoxy- and deoxycholate. Ursodeoxy- and tauroursodeoxycholate did not significantly reduce gallbladder contractility. Taurocholate significantly reduced contractility at concentrations of 10(-6) M and higher, taurodeoxycholate at 10(-7) M and higher and deoxycholate at 10(-5) M and higher. Contractility induced by acetylcholine 10(-3) M at a bile salt concentration of 10(-4) M was 66.0 +/- 11.7% (taurocholate), 50.2 +/- 6.2% (deoxycholate) and 44.8 +/- 11.5% (taurodeoxycholate) of control. The effect of bile salts correlated with their relative hydrophobicity (r = -0.97; p < 0.01). Suppressing effects on gallbladder muscle strip contractility were long lasting and remained after rinsing. Results show that bile salts in the physiological dose range inhibit in vitro gallbladder contraction. If this mechanism exists in vivo, it may have important implications for gallbladder motility regulation.

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