人IL-1 β合成非肽片段163-171的代谢行为及分布

Lymphokine research Pub Date : 1990-01-01
G P Pessina, V Bocci, C Nicoletti, C Becherucci, R Presentini, L Parente, L Villa, A Tagliabue, D Boraschi
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引用次数: 0

摘要

分析佐剂合成非肽VQGEESNDK(与人IL-1中163-171位片段对应)经不同途径给兔给药后的药动学参数及分布。放射性标记的肽不与血浆蛋白结合,当静脉注射时,它很快从循环中消失,t1/2 α为1分钟,t1/2 β为166分钟。通过i.m.s.c.和口服给药,Cmax在接种后30至90分钟达到,范围在给药剂量的7%至4%之间。器官分布表明,放射性主要集中在肾脏,并随尿液排出。从Sephadex G-10层析中,静脉注射后4小时尿液中回收的肽约60%是完整的,而通过其他途径给药时,降解率超过85%。尿液中完整肽的回收量通过不同途径与生物有效性相关,提示体内的佐剂作用是由完整肽发挥的,而不是由其代谢物发挥的。
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Metabolic behavior and distribution of the synthetic nonapeptide fragment 163-171 of human IL-1 beta.

The pharmacokinetic parameters and distribution of the adjuvant synthetic nonapeptide VQGEESNDK, corresponding to the fragment in position 163-171 in human IL-1, were analyzed after administration to rabbit through different routes. The radiolabeled peptide did not bind to plasma proteins and, when inoculated i.v., it disappeared very rapidly from the circulation, with a t1/2 alpha of 1 min and a t 1/2 beta of 166 min. Upon administration through i.m., s.c. and oral route, the Cmax was reached between 30 and 90 min after inoculum and ranged between 7 and 4% of the administered dose. Organ distribution showed that most of the radioactivity was concentrated in kidneys and excreted in urine. From Sephadex G-10 chromatography, about 60% of the peptide recovered in the urine 4h after i.v. inoculum was intact, whereas it was more than 85% degraded when administered by other routes. The amount of intact peptide recovered in the urine correlated with the biological effectiveness through different routes, suggesting that the adjuvant effect in vivo is exerted by the intact peptide, rather than by its metabolites.

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