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腔内胃泌素对小肠吸收的增强作用。

Enhancement of small intestine absorption by intraluminal gastrin.

作者信息

Schwartz M Z, Storozuk R B

出版信息

J Surg Res. 1986 May;40(5):421-5. doi: 10.1016/0022-4804(86)90209-x.

Abstract

Several studies have suggested that gastrointestinal peptides can produce trophic changes in the small intestine epithelium. In a previous study utilizing a rat fetal intestine transplant model, we reported that chronic, continuous, systemic administration of gastrin-17 increased carbohydrate absorption 2.5-fold and protein absorption 1.3-fold. The present study was designed to evaluate the effect of chronic luminal perfusion of gastrin on substrate absorption in rat mature small intestine. A 10-cm segment of mid small intestine was isolated with both ends brought out as abdominal wall stomas (creating a Thiry-Vella loop) and bowel continuity was established by end-to-end anastomosis. After a 1-week recovery, the tips of two catheters were positioned at approximately 3 and 6 cm from the proximal end of the isolated small intestine segment. A 14-day continuous luminal perfusion was accomplished by connecting the other ends of the catheters to subcutaneously placed osmotic pumps filled to deliver saline (control; N = 10) or gastrin-17 (13.5 nM/kg/day; N = 7). At the completion of the luminal perfusion, intestinal absorption was determined with labeled substrates [14C]galactose and [14C]glycine) using a closed, recirculation technique. Absorption (microM/cm2 small intestine) of galactose in the control animals was 1.44 +/- 0.18 and for the gastrin infused rats, it was 6.56 +/- 0.46. Glycine absorption was 1.63 +/- 0.31 for the control group and 7.83 +/- 0.62 for the gastrin infused group. Thus, in this rat model, intraluminal gastrin infusion was capable of increasing carbohydrate (galactose) absorption 456% (P less than 0.01) and protein (glycine) absorption 480% (P less than 0.01). These data represent the first demonstration that intraluminal gastrin can influence small intestine mucosal function by enhancing substrate absorption.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

多项研究表明,胃肠道肽可引起小肠上皮的营养性变化。在先前一项利用大鼠胎儿肠移植模型的研究中,我们报告称,长期、持续、全身性给予胃泌素 - 17可使碳水化合物吸收增加2.5倍,蛋白质吸收增加1.3倍。本研究旨在评估长期腔内灌注胃泌素对大鼠成熟小肠底物吸收的影响。分离出一段10厘米长的中小肠,两端引出作为腹壁造口(形成一个Thiry - Vella袢),通过端端吻合建立肠道连续性。经过1周恢复后,将两根导管的尖端置于距分离出的小肠段近端约3厘米和6厘米处。通过将导管的另一端连接到皮下放置的渗透泵来完成14天的持续腔内灌注,渗透泵填充以输送生理盐水(对照组;N = 10)或胃泌素 - 17(13.5 nM/kg/天;N = 7)。在腔内灌注结束时,使用封闭的再循环技术,用标记底物[¹⁴C]半乳糖和[¹⁴C]甘氨酸测定肠道吸收。对照组动物半乳糖的吸收(微摩尔/平方厘米小肠)为1.44±0.18,胃泌素灌注大鼠为6.56±0.46。对照组甘氨酸吸收为1.63±0.31,胃泌素灌注组为7.83±0.62。因此,在该大鼠模型中,腔内注入胃泌素能够使碳水化合物(半乳糖)吸收增加456%(P<0.01),蛋白质(甘氨酸)吸收增加480%(P<0.01)。这些数据首次证明腔内胃泌素可通过增强底物吸收来影响小肠黏膜功能。(摘要截短于250字)

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