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Retina Compatible Interactions and Effective Modulation of Blood Ocular Barrier P-gp Activity by Third-Generation Inhibitors Improve the Ocular Penetration of Loperamide
Authors:Karthik Yadav Janga  Akshaya Tatke  Surabhi Shukla  Surya P. Lamichhane  Bharathi Avula  XiangDi Wang  Monica M. Jablonski  Ikhlas A. Khan  Soumyajit Majumdar
Affiliation:1. Department of Pharmaceutics and Drug Delivery, School of Pharmacy, The University of Mississippi, Jackson, Mississippi 38677;2. National Center for Natural Products Research, The University of Mississippi, University, Mississippi 38655;3. Research Institute of Pharmaceutical Sciences, The University of Mississippi, University, Mississippi 38677;4. Department of Ophthalmology, The University of Tennessee Health Science Center, Hamilton Eye Institute, Cordova, Tennessee 38018
Abstract:Effective drug delivery to the deeper ocular tissues remains an unresolved conundrum mainly due to the expression of multidrug resistance efflux proteins, besides tight junction proteins, in the blood ocular barriers (BOBs). Hence, the purpose of the current research was to investigate the ability of the third-generation efflux protein inhibitors, elacridar (EQ), and tariquidar (TQ), to diminish P-glycoprotein (P-gp) mediated efflux transport of loperamide (LOP), a P-gp substrate, across the BOB in Sprague Dawley rats. Initially, Western blot analysis confirmed the expression of P-gp in the iris-ciliary bodies and the retina choroid in the wild type rats. Next, the ocular distribution of LOP, in the presence and absence of EQ/TQ (at 2 doses), was evaluated. The significantly higher aqueous humor/plasma (DAH) and vitreous humor (VH)/plasma (DVH) distribution ratios of LOP in the rats pretreated with EQ or TQ demonstrated effective inhibition of P-gp activity in the BOB. Interestingly, the modulation of P-gp activity by EQ/TQ was more pronounced at the lower dose. The normal functioning and architecture of the retina, as indicated by electroretinography studies, confirmed the cytocompatibility of LOP and EQ/TQ interactions at the doses tested.
Keywords:P-gp inhibitors  electroretinography  elacridar  tariquidar  blood aqueous barrier (BAB)  blood retinal barrier (BRB)  ABC  adenosine tri-phosphate–binding cassette  AH  aqueous humor  BAB  blood aqueous barrier  BM  Bruch's membrane  BOB  blood ocular barrier  BRB  blood retinal barrier  distribution ratio of loperamide from plasma to aqueous humor  distribution ratio of loperamide from plasma to vitreous humor  EE  extraction efficiency  EQ  elacridar  ERG  electroretinography  I.C.  iris-ciliary body  I.P.  intraperitoneal  IIG  inactive ingredients  IV  intravenous  LOD  limit of detection  LOP  loperamide  LOQ  limit of quantification  Mdr 1a  multidrug resistance 1a gene  P-gp  P-glycoprotein  PG  pigmented granules  Q-TOF  quadrupole time of flight  R.C.  retina choroid  SD  Sprague Dawley  TQ  tariquidar  UHPLC  ultra high performance liquid chromatography  VH  vitreous humor
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