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The use of gastrointestinal intubation studies for controlled release development.

机译:胃肠道插管研究用于控制释放的发展。

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AIMS: This review describes clinical results of gastrointestinal intubation studies of eight controlled release (CR) candidates under development during the 1990s and offers suggestions for determining why, when and how to conduct human intubation studies. METHODS: Experience with the administration of the following eight compounds to various regions of the gastrointestinal tract is described: CJ-13,610, CP-195,543, CP-331,684, CP-409,092, CP-424,391, azithromycin, sertraline, and trovafloxacin. Also included are human pharmacokinetic studies with prototype CR dosage forms for CJ-13,610 and CP-424,391. RESULTS: Intubation studies, while appearing invasive, are safe and not unpleasant procedures that have been found to be valuable in the development of CR formulations. CONCLUSIONS: The following recommendations are made regarding intubation studies: (i) no intubation study is recommended for compounds with high permeability, since these compounds are likely to be well absorbed from the colon; (ii) compounds with moderate permeability may require an intubation study if the dog colon and in silico models predict a marginally acceptable CR concentration-time profile; (iii) use a dose that approximates 1 h of the intended CR delivery rate; (iv) use the smallest volume possible; (v) define and record tubing placement; (vi) use a thermodynamically stable solution or/and suspension.
机译:目的:该综述描述了1990年代正在开发的八种控释(CR)候选药物在胃肠道插管研究中的临床结果,并为确定为什么,何时以及如何进行人体插管研究提供了建议。方法:描述了以下八种化合物在胃肠道各个区域的给药经验:CJ-13,610,CP-195,543,CP-331,684,CP-409,092,CP-424,391,阿奇霉素,舍曲林和曲伐沙星。还包括针对CJ-13,610和CP-424,391的原型CR剂型的人体药代动力学研究。结果:插管研究虽然具有侵入性,但它是安全且并非令人不愉快的程序,已被发现对CR制剂的开发具有重要意义。结论:关于插管研究,提出了以下建议:(i)不建议对高渗透性化合物进行插管研究,因为这些化合物很可能从结肠吸收良好; (ii)如果狗结肠和计算机模型预测的CR浓度-时间曲线在可接受范围内,则具有中等渗透性的化合物可能需要进行插管研究; (iii)使用的剂量应接近预期CR释放速率的1小时; (iv)尽可能使用最小的体积; (v)定义并记录油管的位置; (vi)使用热力学稳定的溶液或悬浮液。

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