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地塞米松纳米混悬剂作为鼓室内注射治疗急性听力损失的疗效。

Efficiency of a dexamethasone nanosuspension as an intratympanic injection for acute hearing loss.

机构信息

Department of Otolaryngology, College of Medicine, The Catholic University of Korea, Daejeon, Republic of Korea.

Bio-Synectics, Inc., Seoul, Republic of Korea.

出版信息

Drug Deliv. 2022 Dec;29(1):149-160. doi: 10.1080/10717544.2021.2021320.

DOI:10.1080/10717544.2021.2021320
PMID:34967280
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8725939/
Abstract

Dexamethasone sodium phosphate (Dex-SP) is the most commonly used drug administered via intratympanic injection for the treatment of acute hearing loss, but its penetration efficiency into the inner ear is very low. To address this problem, we evaluated the possibility of administering dexamethasone nanosuspensions via intratympanic injection because hydrophobic drugs might be more effective in penetrating the inner ear. Three types of dexamethasone nanosuspensions were prepared; the dexamethasone nanoparticles in the three nanosuspensions were between approximately 250 and 350 nm in size. To compare the efficiency of Dex-SP and dexamethasone nanosuspension in delivering dexamethasone to the inner ear, the concentrations of dexamethasone in perilymph and cochlear tissues were compared by liquid chromatography-mass spectrometry. The dexamethasone nanosuspensions resulted in significantly higher drug concentrations in perilymph and cochlear tissues than Dex-SP at 6 h; interestingly, animals treated with nanosuspensions showed a 26-fold higher dexamethasone concentrations in their cochlear tissues than animals treated with Dex-SP. In addition, dexamethasone nanosuspension caused better glucocorticoid receptor phosphorylation than Dex-SP both and , and in the ototoxic animal model, the nanosuspension showed a significantly better hearing-protective effect against ototoxic drugs than Dex-SP. In the safety evaluation, the nanosuspension showed no toxicity at concentrations up to 20 mg/mL. In conclusion, a nanosuspension of dexamethasone was able to deliver dexamethasone to the cochlea very safely and efficiently and showed potential as a formula for intratympanic injection.

摘要

地塞米松磷酸钠(Dex-SP)是治疗急性听力损失最常用的经鼓室内注射药物,但它在内耳中的渗透效率非常低。为了解决这个问题,我们评估了通过鼓室内注射给予地塞米松纳米混悬剂的可能性,因为疏水性药物可能更有效地穿透内耳。我们制备了三种类型的地塞米松纳米混悬剂;这三种纳米混悬剂中的地塞米松纳米粒大小约为 250 至 350nm。为了比较 Dex-SP 和地塞米松纳米混悬剂将地塞米松递送至内耳的效率,通过液相色谱-质谱法比较了地塞米松在外淋巴液和耳蜗组织中的浓度。与 Dex-SP 相比,地塞米松纳米混悬剂在 6 小时时在外淋巴液和耳蜗组织中导致地塞米松浓度显著升高;有趣的是,用纳米混悬剂治疗的动物的耳蜗组织中的地塞米松浓度比用 Dex-SP 治疗的动物高 26 倍。此外,地塞米松纳米混悬剂引起的糖皮质激素受体磷酸化作用优于 Dex-SP 两者均在 30 分钟和 6 小时时,并且在耳毒性动物模型中,纳米混悬剂显示出比 Dex-SP 更好的对抗耳毒性药物的听力保护作用。在安全性评估中,纳米混悬剂在高达 20mg/mL 的浓度下没有显示出毒性。总之,地塞米松纳米混悬剂能够非常安全有效地将地塞米松递送至耳蜗,并显示出作为鼓室内注射配方的潜力。

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本文引用的文献

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Intratympanic administration of alpha-lipoic acid-loaded pluronic F-127 nanoparticles ameliorates acute hearing loss.经鼓室内给予负载 α-硫辛酸的普朗尼克 F-127 纳米粒可改善急性听力损失。
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Therapeutic glucocorticoids: mechanisms of actions in rheumatic diseases.
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