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使用棕榈酰-L-肉碱提高头孢西丁的生物利用度。I. 在不同肠道区域的增强剂活性。

Enhanced bioavailability of cefoxitin using palmitoyl L-carnitine. I. Enhancer activity in different intestinal regions.

作者信息

Sutton S C, LeCluyse E L, Cammack L, Fix J A

机构信息

INTERx Research Corporation, MSDRL, Lawrence, Kansas 66047.

出版信息

Pharm Res. 1992 Feb;9(2):191-4. doi: 10.1023/a:1018977021183.

Abstract

The conditions under which the absorption enhancer palmitoyl L-carnitine chloride (PCC) improved the bioavailability of the poorly absorbed antibiotic cefoxitin throughout the rat intestine has been studied. Cefoxitin alone was appreciably absorbed only in the duodenum (31% vs less than 7% elsewhere). PCC solutions (3 mg/rat, pH 4.0) enhanced cefoxitin bioavailability (F) by 0-, 22-, 16-, and greater than 32-fold in the duodenum, jejunum, ileum, and colon regions, respectively. The inability of PCC to improve F in the duodenum could not likely be attributed to enzymatic degradation of the enhancer, since coadministration with protease and esterase inhibitors produced similar results (F = 30%). Coadministration of PCC solution with cefoxitin in the unligated or ligated colon, increased F to 33 and 76%, respectively. Qualitatively similar results were seen with PCC suspensions (3 mg/rat, pH 6.0). Maintaining a high concentration of cefoxitin and PCC in a restricted region (i.e., by ligating a 2- to 3-cm section of the colon) afforded a two- to threefold advantage over an unligated colon section. The difference in cefoxitin bioavailability between ligated and unligated colon was probably due to sample spreading and subsequent/simultaneous dilution.

摘要

研究了吸收促进剂氯化棕榈酰 -L-肉碱(PCC)提高吸收不良抗生素头孢西丁在整个大鼠肠道内生物利用度的条件。单独使用头孢西丁时,仅在十二指肠有明显吸收(31%,而其他部位低于7%)。PCC溶液(3mg/大鼠,pH 4.0)分别使头孢西丁在十二指肠、空肠、回肠和结肠区域的生物利用度(F)提高了0倍、22倍、16倍和大于32倍。PCC在十二指肠中不能提高F,这不太可能归因于增强剂的酶促降解,因为与蛋白酶和酯酶抑制剂共同给药产生了相似的结果(F = 30%)。在未结扎或结扎的结肠中,将PCC溶液与头孢西丁共同给药,F分别提高到33%和76%。PCC悬浮液(3mg/大鼠,pH 6.0)也观察到了定性相似的结果。在受限区域(即通过结扎2至3厘米长的结肠段)维持高浓度的头孢西丁和PCC比未结扎的结肠段有两到三倍的优势。结扎和未结扎结肠之间头孢西丁生物利用度的差异可能是由于样品扩散以及随后/同时的稀释。

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