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首页> 外文期刊>Archives of Pharmacal Research >The influence of stabilizer and bioadhesive polymer on the permeation-enhancing effect of AT1002 in the nasal delivery of a paracellular marker
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The influence of stabilizer and bioadhesive polymer on the permeation-enhancing effect of AT1002 in the nasal delivery of a paracellular marker

机译:稳定剂和生物粘附性聚合物对AT1002在旁细胞标记物鼻腔输送中的渗透增强作用的影响

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Permeation enhancers are of major interest to improve the low bioavailability of therapeutic agents due to poor membrane permeation. AT1002, a six-amino acid fragment of Zonula occludens toxin, was reported to possess permeation-enhancing effects. However, further studies were suggested to focus on the peptide nature of AT1002 like stability and membrane clearance to accurately reflect its permeation-enhancing potential. Thus, this paper focused on the susceptibility of AT1002 for identifying additives to minimize the instability of AT1002, and the permeation-enhancing effect of AT1002 when co-administered with a bioadhesive polymer. The stability study showed that AT1002 were unstable in neutral to basic pH conditions and with increasing incubation time, and 5% dextrose and the 1% mixture of amino acids (arginine, cysteine, glycine) significantly minimized the instability of AT1002 at pH 7.4 for at least 6 hours, respectively. In the intranasal study of a paracellular marker, the administration of mannitol with AT1002 in 5% dextrose solution led to statistically significant 3.14- and 2.17-fold increases in Cmax and AUC0-360min in the presence of carrageenan over the control. Thus, the addition of carrageenan as a bioadhesive polymer and dextrose as a stabilizer together with AT1002 may allow the development of the mucosal drug delivery of low-bioavailability therapeutic agents.
机译:渗透促进剂对于改善由于膜渗透性差的治疗剂的低生物利用度具有重大意义。据报道,AT1002是Zonula闭塞毒素的六氨基酸片段,具有增强渗透的作用。但是,建议进一步研究集中于AT1002的肽性质,如稳定性和膜清除率,以准确反映其渗透增强潜力。因此,本文着重研究了AT1002在识别添加剂时的敏感性,以最大程度地降低AT1002的不稳定性,以及与生物粘合剂聚合物共同使用时AT1002的渗透增强作用。稳定性研究表明,AT1002在中性至碱性pH条件下以及随着孵育时间的增加而不稳定,5%的葡萄糖和1%的氨基酸混合物(精氨酸,半胱氨酸,甘氨酸)显着最小化了AT1002在pH 7.4下的不稳定性。至少分别需要6个小时。在鼻内旁细胞标记物研究中,甘露醇与AT1002在5%葡萄糖溶液中的给药导致C sub 和AUC 0-360min < / sub>中存在角叉菜胶的控制。因此,将角叉菜胶作为生物粘附性聚合物和右旋糖作为稳定剂与AT1002一起添加可促进低生物利用度治疗剂的粘膜药物递送。

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