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胃肠激素能增强肠道吸收吗?

Can gastrointestinal hormones enhance intestinal absorption?

作者信息

Schwartz M Z, Storozuk R B

出版信息

Surgery. 1985 Sep;98(3):430-6.

PMID:4035565
Abstract

Recent studies have suggested that certain gastrointestinal peptides exert a trophic effect on the small intestine. We chose to evaluate the effect of glucagon and cholecystokinin-octapeptide (CCK-OP) on absorption of substrates in both developing and mature small intestine. Developing small intestine was evaluated in a rat fetal intestine transplant model, and mature rat small intestine was studied in in situ but isolated 10 cm segments of jejunum and ileum. Glucagon, 10 micrograms/kg/day, and CCK-OP, 45 micrograms/kg/day, were delivered continuously for 14 days through a subcutaneous osmotic pump. Intestinal absorption was determined with labeled substrates (14C-galactose and 14C-glycine) by a recirculation perfusion technique. Absorption results were expressed as percentage increase over control. The fetal intestine response to glucagon infusion was a 13% rise in galactose absorption and a 27% rise in glycine absorption. After CCK-OP infusion, fetal galactose absorption was 11% and glycine absorption rose 17%. Mature jejunal galactose absorption rose 53% and glycine absorption rose 55% after glucagon infusion. The ileal response to glucagon was a 271% rise in galactose absorption (p less than 0.05) and a 21% increase in glycine absorption. Infusion of CCK-OP decreased jejunal galactose absorption 3% but increased glycine absorption 41%. The ileal response was a 224% increase in galactose absorption (p less than 0.05) and a 19% increase in glycine absorption. Our data suggest that chronic administration of glucagon and CCK-OP can increase substrate absorption in developing and mature rat small intestine. Perhaps manipulation of the gastrointestinal hormone environment may result in increased absorption in man.

摘要

最近的研究表明,某些胃肠肽对小肠具有营养作用。我们选择评估胰高血糖素和八肽胆囊收缩素(CCK-OP)对发育中和成熟小肠中底物吸收的影响。在大鼠胎儿肠移植模型中评估发育中的小肠,在原位但分离出10厘米长的空肠和回肠段研究成熟大鼠小肠。通过皮下渗透泵连续14天给予10微克/千克/天的胰高血糖素和45微克/千克/天的CCK-OP。通过再循环灌注技术用标记底物(14C-半乳糖和14C-甘氨酸)测定肠道吸收。吸收结果表示为相对于对照的百分比增加。胎儿肠对胰高血糖素输注的反应是半乳糖吸收增加13%,甘氨酸吸收增加27%。输注CCK-OP后,胎儿半乳糖吸收为11%,甘氨酸吸收增加17%。胰高血糖素输注后,成熟空肠半乳糖吸收增加53%,甘氨酸吸收增加55%。回肠对胰高血糖素的反应是半乳糖吸收增加271%(p<0.05),甘氨酸吸收增加21%。输注CCK-OP使空肠半乳糖吸收降低3%,但使甘氨酸吸收增加41%。回肠的反应是半乳糖吸收增加224%(p<0.05),甘氨酸吸收增加19%。我们的数据表明,长期给予胰高血糖素和CCK-OP可增加发育中和成熟大鼠小肠中的底物吸收。或许对胃肠激素环境的调控可能会使人类的吸收增加。

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