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兔可控连续球周给药后地塞米松的分布特征

Dexamethasone distribution characteristic following controllable continuous sub-tenon drug delivery in rabbit.

作者信息

Huang Xuetao, Peng Manqiang, Yang Yezhen, Duan Yiqin, Li Kuanshu, Liu Shaogang, Ye Changhua, Lin Ding

机构信息

a Department of Ophthalmology , Changsha Aier Hospital, Aier School of Ophthalmology, Central South University , Changsha , China and.

b Advanced Research Center, Central South University , Changsha , China.

出版信息

Drug Deliv. 2017 Nov;24(1):818-824. doi: 10.1080/10717544.2017.1324531.

DOI:10.1080/10717544.2017.1324531
PMID:28509581
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8241131/
Abstract

Drug delivery systems are required to be safe, minimally invasive and effectively delivery drug to the target tissues. But delivery drugs to the eye has not yet satisfied this need. Here, we focused on examining the distribution of dexamethasone (DEX) in ocular and plasmic samples following controllable continuous sub-Tenon drug delivery (CCSDD) of dexamethasone disodium phosphate (DEXP) in rabbit, and to compare that with two traditional routes: subconjunctival injection and intravenous injection. The DEX concentration was analyzed by Shimadzu LC-MS 2010 system. In CCSDD group, during observed 24 h, the mean DEX level in collected samples from highest to lowest following in order: sclera, cornea, retina/choroid, iris, plasma, aqueous humor, lens and vitreous body. In ocular solid tissue, the DEX level in posterior segment is higher than in anatomic corresponding anterior segment, but it is opposite in ocular fluid tissue. High levels of DEX were maintained at 12 h in the ocular tissue immediately after the administration. Even at 24 h, the mean DEX concentration was 31.72 ng/ml and 22.40 ng/ml in aqueous and vitreous, respectively. In CCSDD group, the ocular DEX exposure (AUC) is much higher and plasma exposure is much less than IV group, and it is also similar in SC group except iris. The amount of DEX levels are markedly increased in ocular tissues but it yield lower plasma levels indicating reduction of systemic absorption by CCSDD. Thus, CCSDD is an effective method of delivering DEX into anterior and posterior segment of the eye.

摘要

药物递送系统需要具备安全性、微创性,并能有效地将药物递送至靶组织。但将药物递送至眼部尚未满足这一需求。在此,我们着重研究了在兔眼可控连续Tenon囊下药物递送(CCSDD)磷酸地塞米松二钠(DEXP)后,地塞米松(DEX)在眼部和血浆样本中的分布情况,并将其与两种传统给药途径:结膜下注射和静脉注射进行比较。通过岛津LC-MS 2010系统分析DEX浓度。在CCSDD组中,在观察的24小时内,收集样本中DEX平均水平从高到低依次为:巩膜、角膜、视网膜/脉络膜、虹膜、血浆、房水、晶状体和玻璃体。在眼部固体组织中,后段的DEX水平高于相应的前段解剖部位,但在眼内液体组织中情况相反。给药后立即在眼部组织中维持高水平的DEX达12小时。即使在24小时时,房水和玻璃体中的DEX平均浓度分别为31.72 ng/ml和22.40 ng/ml。在CCSDD组中,眼部DEX暴露量(AUC)远高于静脉注射组,血浆暴露量则远低于静脉注射组,除虹膜外,结膜下注射组的情况也与之相似。眼部组织中DEX水平显著升高,但血浆水平较低,表明CCSDD减少了全身吸收。因此,CCSDD是一种将DEX递送至眼前段和后段的有效方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/ec6d237d2b6e/IDRD_A_1324531_F0003_B.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/7f819889247b/IDRD_A_1324531_F0001_B.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/88de0a822078/IDRD_A_1324531_F0002_B.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/ec6d237d2b6e/IDRD_A_1324531_F0003_B.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/7f819889247b/IDRD_A_1324531_F0001_B.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/88de0a822078/IDRD_A_1324531_F0002_B.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b25a/8241131/ec6d237d2b6e/IDRD_A_1324531_F0003_B.jpg

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