A promising drug candidate for the treatment of glaucoma based on a P2Y6-receptor agonist

Tali Fishman Jacob, Vijay Singh, Mudit Dixit, Tamar Ginsburg-Shmuel, Begoña Fonseca, Jesus Pintor, Moussa B.H. Youdim, Dan T. Major, Orly Weinreb, Bilha Fischer

Research output: Contribution to journalArticlepeer-review

13 Scopus citations

Abstract

Extracellular nucleotides can regulate the production/drainage of the aqueous humor via activation of P2 receptors, thus affecting the intraocular pressure (IOP). We evaluated 5-OMe-UDP(α-B), 1A, a potent P2Y6-receptor agonist, for reducing IOP and treating glaucoma. Cell viability in the presence of 1A was measured using [3-(4, 5-dimethyl-thiazol-2-yl) 2, 5-diphenyl-tetrazolium bromide] (MTT) assay in rabbit NPE ciliary non-pigmented and corneal epithelial cells, human retinoblastoma, and liver Huh7 cells. The effect of 1A on IOP was determined in acute glaucomatous rabbit hyaluronate model and phenol-induced chronic glaucomatous rabbit model. The origin of activity of 1A was investigated by generation of a homology model of hP2Y6-R and docking studies. 1A did not exert cytotoxic effects up to 100 mM vs. trusopt and timolol in MTT assay in ocular and liver cells. In normotensive rabbits, 100 μM 1A vs. xalatan, trusopt, and pilocarpine reduced IOP by 45 vs. 20–30%, respectively. In the phenol animal model, 1A (100 μM) showed reduction of IOP by 40 and 20%, following early and late administration, respectively. Docking results suggest that the high activity and selectivity of 1A is due to intramolecular interaction between Pα-BH3 and C5-OMe which positions 1A in a most favorable site inside the receptor. P2Y6-receptor agonist 1A effectively and safely reduces IOP in normotense, acute, and chronic glaucomatous rabbits, and hence may be suggested as a novel approach for the treatment of glaucoma.

Original languageEnglish
Pages (from-to)271-284
Number of pages14
JournalPurinergic Signalling
Volume14
Issue number3
DOIs
StatePublished - 1 Sep 2018

Bibliographical note

Publisher Copyright:
© 2018, Springer Nature B.V.

Funding

Acknowledgements The authors gratefully acknowledge the support of the Office of the Israeli Chief Scientist, and Youdim Pharmaceuticals Ltd. Israel. The authors gratefully acknowledge the support of the Office of the Israeli Chief Scientist, and Youdim Pharmaceuticals Ltd. Israel. ? Patent?US Application No. 61/344,972 of 01/12/2010 and US Application No. 61/467,108 of 24/03/2011 International Filing: e :01/12/2011 Authors Orly Weinreb and Tali Fishman-Jacob received research grants from the Office of the Israeli Chief Scientist, and Youdim Pharmaceuticals Ltd. Israel. Conflict of interest Authors Orly Weinreb and Tali Fishman-Jacob received research grants from the Office of the Israeli Chief Scientist, and Youdim Pharmaceuticals Ltd. Israel.

FundersFunder number
Office of the Israeli Chief Scientist
Youdim Pharmaceuticals Ltd01/12/2010, 61/467,108, 61/344,972
Chief Scientist Office

    Keywords

    • 5-OMe-uridine-5′-α-borano-diphosphate
    • Glaucoma
    • Human P2Y6 receptor
    • Intraocular pressure
    • P2Y6 receptor agonist

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