Research on Contents of Radix Ophiopogon Japonicas Polysaccharides MDG-1 Changing in Rrats Gastrointestinal Tract by HPGPC

XIE Hua-tong; WANG Shuo; RUAN Ke-feng; Feng Yi; XU De-sheng

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Research on Contents of Radix Ophiopogon Japonicas Polysaccharides MDG-1 Changing in Rrats Gastrointestinal Tract by HPGPC

更新时间：2024-01-04

- Research on Contents of Radix Ophiopogon Japonicas Polysaccharides MDG-1 Changing in Rrats Gastrointestinal Tract by HPGPC
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 18, Issue 13, Pages: 139-145(2012)
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- Published：2012
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XIE Hua-tong, WANG Shuo, RUAN Ke-feng, et al. Research on Contents of Radix Ophiopogon Japonicas Polysaccharides MDG-1 Changing in Rrats Gastrointestinal Tract by HPGPC[J]. Chinese journal of experimental traditional medical formulae, 2012, 18(13): 139-145.
DOI：

XIE Hua-tong, WANG Shuo, RUAN Ke-feng, et al. Research on Contents of Radix Ophiopogon Japonicas Polysaccharides MDG-1 Changing in Rrats Gastrointestinal Tract by HPGPC[J]. Chinese journal of experimental traditional medical formulae, 2012, 18(13): 139-145. DOI：

摘要

目的: 探讨口服麦冬多糖MDG-1后在胃肠道内的变化。方法: 采用异硫氰酸荧光素(FITC)对麦冬多糖MDG-1进行标记

测定取代度。采用荧光凝胶色谱法(HPGPC)对消化道内含量进行测定。胃内含量变化测定:SD雄性大鼠随机分成6组

其中5组分别口服给予不同剂量F-MDG-1

空白组给予水

在1 h时测定含量;另取SD雄性大鼠随机分成6组

其中5组分别经口给予相同剂量F-MDG-1

空白组给予水

分别在0

4 h时测定含量。小肠道内含量测定:SD-雄性大鼠分成4组

空白组1组及给药组3组

经胃幽门部注射给药后立即分别结扎胃幽门部及小肠末端

空白组给予水适量

给药组给予F-MDG-1溶液适量

分别在1

4 h测定内容物内F-MDG-1含量。大肠内含量测定:SD-雄性大鼠分成4组

空白组1组及给药组3组

每组6只

给药方法:经小肠末端部注射给药后立即分别结扎小肠末端及大肠末端近肛门部。空白组给予水适量

给药组给予F-MDG-1溶液适量

分别在1

4 h测定大肠内容物内F-MDG-1含量。结果: 给予相同剂量的F-MDG-1

随着药物在胃内驻留时间的延长

其浓度下降。而在给予不同浓度F-MDG-1后

在1 h时测得浓度占给药量的百分比随着给药剂量的增加而增加;但将pH调7.2后

其含量未变化。分别单次给予小肠、大肠F-MDG-1后

随着药物在肠道内驻留时间的延长

其含量逐渐降低。结论: 采用FITC对MDG-1进行标记

并采用荧光色谱法对MDG-1在胃肠道内含量变化进行研究是可行的。MDG-1在胃内不分解

其主要代谢部位在肠道

其原因可能是肠道内环境及细菌共同作用的结果。

Abstract

Objective: To investigate the contents change after oral Radix Ophiopogon Japonicas polysaccharides MDG-1 in rats by high performance gel permeation chromatograph(HPGPC). Method: Labeling the MDG-1 and detecting replacement of fluoresciniso thiocyate(FITC) then using the HCGPC was in order to detect the contents of MDG-1 in stomach

small intestine

large intestine. To the various parts of the gastrointestinal tract

the stomach were given different doses of F-MDG-1 after pylorus ligation

then suture abdominal while contents were immediately harvested at times 1 h postdose; the stomach were given doses of F-MDG-1 after pylorus ligation

then suture abdominal while contents were immediately harvested at predefined times. The small intestine near the bottom of the cecum were ligated after small intestine were given F-MDG-1 from duodenum near the pylorus then suture abdominal while contents were harvested at predefined times;the large intestine near the anus were ligated after the large intestine were given F-MDG-1 from end of the small intestine near the cecum then suture abdominal while contents were harvested at predefined times

all these contents stored at -20℃ until analysis. Result: The F-MDG-1 in rats stomach following oral administration at different doses of F-MDG-1 after pylorus ligation were described with a degradation model and indicated that F-MDG-1 increases the decomposition along with the dosage to reduce in the stomach

while after oral the same dose indicated that F-MDG-1 increases the decomposition along with the time

but the determination result showed that the content unchanged after pH was adjusted to be neutrality(7.2). The small intestine and the large intestine metabolite process indicated that decomposition of F-MDG-1 increased along with time. Conclusion: The combination of the FITC prelabeling method with the highperformance gel permeation chromatography was confirmed and tested and was feasibile.This methodology should be helpful to other polysaccharides research in gastrointestinal tract. In this study

F-MDG-1 was not decomposition in stomach and mainly metabolism in the intestinal tract as a result of effects of gastrointestinal tract condition and bacterium together.

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