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通过应用黏液溶解剂和非离子表面活性剂协同增强鲑鱼降钙素的吸收及可逆性黏膜损伤。

Synergistic absorption enhancement of salmon calcitonin and reversible mucosal injury by applying a mucolytic agent and a non-ionic surfactant.

作者信息

Takatsuka Shinya, Morita Takahiro, Koguchi Atsushi, Horikiri Yuji, Yamahara Hiroshi, Yoshino Hiroyuki

机构信息

Pharmaceutical Development Laboratories, Tanabe Seiyaku Co. Ltd., 3-16-89 Kashima, Yodogawa-ku, Osaka 532-8505, Japan.

出版信息

Int J Pharm. 2006 Jun 19;316(1-2):124-30. doi: 10.1016/j.ijpharm.2006.02.053. Epub 2006 Apr 5.

Abstract

The present study investigated the intestinal absorption enhancement of salmon calcitonin (SCT) and the intestinal mucosal damage when a mucolytic agent and a non-ionic surfactant were administered simultaneously to rats. N-acetylcysteine (NAC) and p-t-octyl phenol polyoxyethylene-9.5 (Triton X -100, TX-100) were chosen as the model mucolytic agent and the non-ionic surfactant, respectively. Dosing solutions containing these agents were administered directly into the rat jejunum, and the bioavailability of SCT up to 2 h was determined. NAC and TX-100, when they were used alone at a dose of 1 mg/head, did not show the apparent enhancement compared to the control. However, simultaneous use of NAC and TX-100 enhanced the intestinal absorption of SCT in a synergistic manner, and absolute bioavailability increased 12.5-fold compared to the control. The effect of NAC and TX-100 on SCT absorption was not dependent on their doses over the range of 0.2-2 mg/head, and the maximum effect was obtained at a dose of 1mg/head. Absorption enhancement of SCT by a combination of NAC and TX-100 was compared to those from the classical absorption enhancers. Absorption-enhancing ability of the combination of NAC and TX-100 was significantly higher than those of sodium deoxycholate, citrate, and the combination of citrate and taurocholate, and was comparable with that of the combination of citrate and taurodeoxycholate. Finally, the intestinal mucosal damage caused by the combination of NAC and TX-100 was assessed using a capsule device. Acute damage on intestinal mucosa was observed when they were exposed into rat intestine, but this morphological damage was found to be reversible. All these results suggest that simultaneous use of a mucolytic agent and a non-ionic surfactant would offer a potentiality for peroral delivery of peptide drugs like SCT.

摘要

本研究考察了在大鼠同时给予黏液溶解剂和非离子表面活性剂时,鲑鱼降钙素(SCT)的肠道吸收增强情况以及肠道黏膜损伤情况。分别选用N-乙酰半胱氨酸(NAC)和对叔辛基苯酚聚氧乙烯醚-9.5( Triton X -100,TX-100)作为模型黏液溶解剂和非离子表面活性剂。将含有这些药剂的给药溶液直接注入大鼠空肠,并测定2小时内SCT的生物利用度。与对照组相比,NAC和TX-100单独以1mg/只的剂量使用时,未显示出明显的增强作用。然而,NAC和TX-100同时使用可协同增强SCT的肠道吸收,与对照组相比,绝对生物利用度提高了12.5倍。在0.2 - 2mg/只的剂量范围内,NAC和TX-100对SCT吸收的影响不依赖于它们的剂量,在1mg/只的剂量时可获得最大效果。将NAC和TX-100联合使用对SCT吸收的增强作用与传统吸收增强剂进行了比较。NAC和TX-100联合使用的吸收增强能力显著高于脱氧胆酸钠、柠檬酸盐以及柠檬酸盐与牛磺胆酸盐的组合,与柠檬酸盐和牛磺脱氧胆酸盐的组合相当。最后,使用胶囊装置评估了NAC和TX-100联合使用对肠道黏膜造成的损伤。当它们暴露于大鼠肠道时,观察到肠道黏膜有急性损伤,但发现这种形态学损伤是可逆的。所有这些结果表明,黏液溶解剂和非离子表面活性剂同时使用可为SCT等肽类药物的口服给药提供一种可能性。

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