4.7 Article

Distribution of Small Molecular Weight Drugs into the Porcine Lens: Studies on Imaging Mass Spectrometry, Partition Coefficients, and Implications in Ocular Pharmacokinetics

期刊

MOLECULAR PHARMACEUTICS
卷 16, 期 9, 页码 3968-3976

出版社

AMER CHEMICAL SOC
DOI: 10.1021/acs.molpharmaceut.9b00585

关键词

lens; drug distribution; ocular; pharmacokinetics; imaging mass spectrometry; MALDI-IMS

资金

  1. Doctoral Programme in Drug Research (University of Eastern Finland)
  2. Academy of Finland [233114]
  3. Biocenter Kuopio
  4. Biocenter Finland
  5. Paivildci and Sakari Sohlberg Foundation
  6. European Union [799880]
  7. Marie Curie Actions (MSCA) [799880] Funding Source: Marie Curie Actions (MSCA)

向作者/读者索取更多资源

Lens is the avascular tissue in the eye between the aqueous humor and vitreous. Drug binding to the lens might affect ocular pharmacokinetics, and the binding may also have a pharmacological role in drug-induced cataract and cataract treatment. Drug distribution in the lens has been studied in vitro with many compounds; however, the experimental methods vary, no detailed information on distribution between the lens sublayers exist, and the partition coefficients are reported rarely. Therefore, our objectives were to clarify drug localization in the lens layers and establish partition coefficients for a wide range of molecules. Furthermore, we aimed to illustrate the effect of lenticular drug binding on overall ocular drug pharmacokinetics. We studied the distribution of 16 drugs and three fluorescent dyes in whole porcine lenses in vitro with imaging mass spectrometry and fluorescence microscopy techniques. Furthermore, we determined lens/buffer partition coefficients with the same experimental setup for 28 drugs with mass spectrometry. Finally, the effect of lenticular binding of drugs on aqueous humor drug exposure was explored with pharmacokinetic simulations. After 4 h, the drugs and the dyes distributed only to the outermost lens layers (capsule and cortex). The lens/buffer partition coefficients for the drugs were low, ranging from 0.05 to 0.8. On the basis of the pharmacokinetic simulations, a high lens-aqueous humor partition coefficient increases drug exposure in the lens but does not significantly alter the pharmacokinetics in the aqueous humor. To conclude, the lens seems to act mainly as a physical barrier for drug distribution in the eye, and drug binding to the lens affects mainly the drug pharmacokinetics in the lens.

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