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比较地塞米松和地塞米松磷酸酯进入豚鼠外淋巴的情况以用于中耳应用

Dexamethasone and Dexamethasone Phosphate Entry into Perilymph Compared for Middle Ear Applications in Guinea Pigs.

作者信息

Salt Alec N, Hartsock Jared J, Piu Fabrice, Hou Jennifer

机构信息

Department of Otolaryngology, Washington University School of Medicine, St. Louis, Missouri, USA,

Department of Otolaryngology, Washington University School of Medicine, St. Louis, Missouri, USA.

出版信息

Audiol Neurootol. 2018;23(4):245-257. doi: 10.1159/000493846. Epub 2018 Nov 29.

Abstract

Dexamethasone phosphate is widely used for intratympanic therapy in humans. We assessed the pharmacokinetics of dexamethasone entry into perilymph when administered as a dexamethasone phosphate solution or as a micronized dexamethasone suspension, with and without inclusion of poloxamer gel in the medium. After a 1-h application to guinea pigs, 10 independent samples of perilymph were collected from the lateral semicircular canal of each animal, allowing entry at the round window and stapes to be independently assessed. Both forms of dexamethasone entered the perilymph predominantly at the round window (73%), with a lower proportion entering at the stapes (22%). When normalized by applied concentration, dexamethasone phosphate was found to enter perilymph far more slowly than dexamethasone, in accordance with its calculated lipid solubility and polar surface area properties. Dexamethasone phosphate therefore has a problematic combination of kinetic properties when used for local therapy of the ear. It is relatively impermeable and enters perilymph only slowly from the middle ear. It is then metabolized in the ear to dexamethasone, which is more permeable through tissue boundaries and is rapidly lost from perilymph. Understanding the influence of molecular properties on the distribution of drugs in perilymph provides a new level of understanding which may help optimize drug therapies of the ear.

摘要

地塞米松磷酸钠广泛用于人类的鼓室内治疗。我们评估了以地塞米松磷酸钠溶液或微粉化地塞米松混悬液给药时,地塞米松进入外淋巴的药代动力学,介质中添加或不添加泊洛沙姆凝胶。在对豚鼠给药1小时后,从每只动物的外侧半规管收集10个独立的外淋巴样本,从而能够分别评估圆窗和镫骨处的药物进入情况。两种形式的地塞米松主要通过圆窗进入外淋巴(73%),通过镫骨进入的比例较低(22%)。根据计算得出的脂溶性和极性表面积特性,按给药浓度进行归一化后,发现地塞米松磷酸钠进入外淋巴的速度比地塞米松慢得多。因此,地塞米松磷酸钠用于耳部局部治疗时,其动力学特性存在问题。它相对不易渗透,从中耳进入外淋巴的速度很慢。然后它在耳内代谢为地塞米松,地塞米松更容易透过组织边界,并且会迅速从外淋巴中消失。了解分子特性对外淋巴中药物分布的影响提供了一个新的理解层面,这可能有助于优化耳部药物治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a22/6492027/58a9d50bfa8c/nihms-1025445-f0001.jpg

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