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顺铂损害大鼠小肠中液体和电解质的吸收:5-羟色胺的作用。

Cisplatin impairs fluid and electrolyte absorption in rat small intestine: a role for 5-hydroxytryptamine.

作者信息

Bearcroft C P, Domizio P, Mourad F H, André E A, Farthing M J

机构信息

Digestive Diseases Research Centre, St Bartholomew's and Royal London, School of Medicine and Dentistry, Turner St, London E1 2AD, UK.

出版信息

Gut. 1999 Feb;44(2):174-9. doi: 10.1136/gut.44.2.174.

Abstract

BACKGROUND

The antineoplastic drug cisplatin has been widely used for the treatment of cancer in humans but its use has been limited by vomiting and diarrhoea. Cisplatin releases 5-hydroxytryptamine into the gut which is thought to be the major mediator of cisplatin induced vomiting.

AIM

To determine whether cisplatin affects fluid and electrolyte transport in rat jejunum and whether this change can be modulated by the 5-hydroxytryptamine3 receptor antagonist, ondansetron.

METHODS

Jejunal perfusion in rats in vivo was performed one hour after intraperitoneal cisplatin (5 and 10 mg/kg) administration. The effect of pretreatment with subcutaneous ondansetron 300 microg/kg was investigated.

RESULTS

Median net fluid absorption after cisplatin 10 mg/kg (67 microl/min/g dry intestinal weight (interquartile range 46 to 100); n = 15) was reduced compared with controls (120 (107 to 151) microl/min/g; n = 13; p<0.001). Ondansetron reversed the impairment of jejunal fluid absorption produced by cisplatin to normal (161 (130 to 176) microl/min/g; n = 11; p<0.001). Electrolyte movement paralleled fluid movement. Jejunal histological examination of sections from cisplatin treated animals showed villus damage, which was not prevented by pretreatment with ondansetron.

CONCLUSION

These findings suggest that diarrhoea during cisplatin therapy may be due to altered fluid transport in the small bowel. The reversal of fluid transport to normal in the presence of a 5-hydroxytryptamine3 receptor antagonist suggests that 5-hydroxytryptamine is a local mediator in the small intestine.

摘要

背景

抗肿瘤药物顺铂已广泛用于人类癌症治疗,但其应用受到呕吐和腹泻的限制。顺铂可将5-羟色胺释放到肠道中,这被认为是顺铂诱导呕吐的主要介质。

目的

确定顺铂是否影响大鼠空肠的液体和电解质转运,以及这种变化是否可被5-羟色胺3受体拮抗剂昂丹司琼调节。

方法

腹腔注射顺铂(5和10mg/kg)1小时后,对大鼠进行体内空肠灌注。研究皮下注射300μg/kg昂丹司琼预处理的效果。

结果

与对照组相比,顺铂10mg/kg组的中位净液体吸收量(67μl/min/g干肠重(四分位间距46至100);n = 15)降低(对照组为120(107至151)μl/min/g;n = 13;p<0.001)。昂丹司琼将顺铂引起的空肠液体吸收损害逆转至正常水平(161(130至176)μl/min/g;n = 11;p<0.001)。电解质移动与液体移动平行。对顺铂处理动物的空肠切片进行组织学检查显示有绒毛损伤,昂丹司琼预处理未能预防这种损伤。

结论

这些发现表明,顺铂治疗期间的腹泻可能是由于小肠液体转运改变所致。5-羟色胺3受体拮抗剂存在时液体转运恢复正常表明,5-羟色胺是小肠中的局部介质。

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