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大鼠脉络丛体外转运苄青霉素的研究。

Transport of benzylpenicillin by the rat choroid plexus in vitro.

作者信息

Suzuki H, Sawada Y, Sugiyama Y, Iga T, Hanano M

出版信息

J Pharmacol Exp Ther. 1987 Aug;242(2):660-5.

PMID:3612557
Abstract

To characterize the transport system by which benzylpenicillin, an organic anion, is accumulated by the isolated rat choroid plexus, kinetic analysis of benzylpenicillin transport was performed. Accumulation of benzylpenicillin was against an electrochemical potential gradient via a saturable process (Km = 58 microM and Vmax = 84 nmol/ml of tissue per min) that was inhibited by sulfhydryl reagents (p-hydroxymercuribenzoate and N-ethylmaleimide), metabolic inhibitors (KCN and 2,4-dinitrophenol) and anion exchange inhibitors (4-acetamide-4'-isothiocyanatostilbene-2,2'-disulfonic acid and 4,4'-diisothiocyanatostilbene-2,2'-disulfonic acid), but is major transport system did not require the inward Na+ gradient. Organic anions, such as 5-hydroxyindoleacetic acid, homovanillic acid, p-aminohippuric acid and probenecid inhibited the accumulation of benzylpenicillin, whereas dipeptides did not affect it. Kinetic analysis of the accumulation of benzylpenicillin suggests that both phenoxymethylpenicillin and cefpiramide are also transported via the benzylpenicillin transport system. Other penicillin and cephalosporin derivatives inhibited the accumulation of benzylpenicillin with different affinities. Penicillin derivatives without dissociating groups in the side chain had the higher affinity for the benzylpenicillin transport system than other beta-lactam antibiotics did. Among penicillin derivatives examined, a good correlation (r = 0.92) was observed between the lipophilicity and the affinity for the benzylpenicillin transport system, whereas no correlation was observed among the cephalosporin derivatives. These findings suggest that the major transport system of benzylpenicillin in the rat choroid plexus is via a carrier-mediated active anion transport process which is distinct from that of dipeptides, and does not require the inward Na+ gradient.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

为了描述有机阴离子苄青霉素被分离的大鼠脉络丛积累的转运系统,对苄青霉素的转运进行了动力学分析。苄青霉素的积累是通过一个可饱和过程逆电化学势梯度进行的(Km = 58微摩尔,Vmax = 84纳摩尔/毫升组织每分钟),该过程受到巯基试剂(对羟基汞苯甲酸和N - 乙基马来酰胺)、代谢抑制剂(氰化钾和2,4 - 二硝基苯酚)以及阴离子交换抑制剂(4 - 乙酰胺 - 4'-异硫氰酸基芪 - 2,2'-二磺酸和4,4'-二异硫氰酸基芪 - 2,2'-二磺酸)的抑制,但主要转运系统不需要内向的钠离子梯度。有机阴离子,如5 - 羟吲哚乙酸、高香草酸、对氨基马尿酸和丙磺舒抑制苄青霉素的积累,而二肽则不影响。苄青霉素积累的动力学分析表明苯氧甲基青霉素和头孢匹胺也通过苄青霉素转运系统进行转运。其他青霉素和头孢菌素衍生物以不同亲和力抑制苄青霉素的积累。侧链中无解离基团的青霉素衍生物对苄青霉素转运系统的亲和力高于其他β - 内酰胺抗生素。在所研究的青霉素衍生物中,亲脂性与对苄青霉素转运系统的亲和力之间观察到良好的相关性(r = 0.92),而在头孢菌素衍生物中未观察到相关性。这些发现表明,大鼠脉络丛中苄青霉素的主要转运系统是通过载体介导的活性阴离子转运过程,这与二肽的转运过程不同,且不需要内向的钠离子梯度。(摘要截断于250字)

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