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吸收促进剂对大鼠直肠黏膜的体内局部作用。

Topical effects of absorption enhancing agents on the rectal mucosa of rats in vivo.

作者信息

van Hoogdalem E J, Vermeij-Kerrs C, de Boer A G, Breimer D D

机构信息

Center for Bio-Pharmaceutical Sciences, Sylvius Laboratories, State University of Leiden, The Netherlands.

出版信息

J Pharm Sci. 1990 Oct;79(10):866-70. doi: 10.1002/jps.2600791004.

DOI:10.1002/jps.2600791004
PMID:2280353
Abstract

In the present study, attempts have been made to assess the effects of cefoxitin formulations with various absorption promoters on mucosal integrity after rectal delivery in rats. Observations were made at 2 and 24 h following drug administration. On macroscopic and histologic evaluation, all drug formulations affected mucosal structure in terms of hyperemia, edema, loss of goblet cell vacuoles, detachment of enterocytes, and increase of the number of inflammatory cells; these effects were not reversible in 24 h. The effects of formulations with MGK (a mixture of glyceryl-1-monooctanoate, glyceryl-1,2-dioctanoate, glyceryl-1,3-dioctanoate, glyceryl trioctanoate, glycerol, and octanoic acid), monoglycerides, 3-amino-1-hydroxypropylidene-1,1-diphosphonate, and 4% (w/v) sodium tauro-24,25-dihydrofusidate (STDHF) tended to exceed those observed with sodium salicylate, medium-chain fatty acids, Azone, and lower STDHF concentrations. The clinically used suppository bases Witepsol H15 and PEG 1540/6000 and indomethacin suppositories also affected mucosal structure. Although the interanimal variability in scores was very substantial, results indicate that rectal absorption enhancement is associated with modification of paracellular transport after detachment of enterocytes. However, the extent of drug absorption enhancement appeared not to be directly related to the extent of mucosal damage.

摘要

在本研究中,已尝试评估含不同吸收促进剂的头孢西丁制剂经大鼠直肠给药后对黏膜完整性的影响。在给药后2小时和24小时进行观察。通过宏观和组织学评估发现,所有药物制剂均在充血、水肿、杯状细胞空泡丢失、肠上皮细胞脱落以及炎性细胞数量增加方面影响黏膜结构;这些影响在24小时内不可逆。含MGK(甘油单辛酸酯、甘油1,2 - 二辛酸酯、甘油1,3 - 二辛酸酯、三辛酸甘油酯、甘油和辛酸的混合物)、甘油单酯、3 - 氨基 - 1 - 羟基亚丙基 - 1,1 - 二膦酸酯以及4%(w/v)牛磺 - 24,25 - 二氢fusidate(STDHF)的制剂的影响往往超过水杨酸钠、中链脂肪酸、氮酮以及较低STDHF浓度时观察到的影响。临床使用的栓剂基质Witepsol H15和PEG 1540/6000以及吲哚美辛栓剂也影响黏膜结构。尽管动物间评分的变异性非常大,但结果表明直肠吸收增强与肠上皮细胞脱落后细胞旁转运的改变有关。然而,药物吸收增强的程度似乎与黏膜损伤的程度没有直接关系。

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