Literature DB >> 19878673

Nucleoside-derived antagonists to A3 adenosine receptors lower mouse intraocular pressure and act across species.

Zhao Wang1, Chi Wai Do, Marcel Y Avila, Kim Peterson-Yantorno, Richard A Stone, Zhan-Guo Gao, Bhalchandra Joshi, Pedro Besada, Lak Shin Jeong, Kenneth A Jacobson, Mortimer M Civan.   

Abstract

The purpose of the study was to determine whether novel, selective antagonists of human A3 adenosine receptors (ARs) derived from the A3-selective agonist Cl-IB-MECA lower intraocular pressure (IOP) and act across species. IOP was measured invasively with a micropipette by the Servo-Null Micropipette System (SNMS) and by non-invasive pneumotonometry during topical drug application. Antagonist efficacy was also assayed by measuring inhibition of adenosine-triggered shrinkage of native bovine nonpigmented ciliary epithelial (NPE) cells. Five agonist-based A3AR antagonists lowered mouse IOP measured with SNMS tonometry by 3-5 mm Hg within minutes of topical application. Of the five agonist derivatives, LJ 1251 was the only antagonist to lower IOP measured by pneumotonometry. No effect was detected pneumotonometrically over 30 min following application of the other four compounds, consonant with slower, smaller responses previously measured non-invasively following topical application of A3AR agonists and the dihydropyridine A3AR antagonist MRS 1191. Latanoprost similarly lowered SNMS-measured IOP, but not IOP measured non-invasively over 30 min. Like MRS 1191, agonist-based A3AR antagonists applied to native bovine NPE cells inhibited adenosine-triggered shrinkage. In summary, the results indicate that antagonists of human A3ARs derived from the potent, selective A3 agonist Cl-IB-MECA display efficacy in mouse and bovine cells, as well. When intraocular delivery was enhanced by measuring mouse IOP invasively, five derivatives of the A3AR agonist Cl-IB-MECA lowered IOP but only one rapidly reduced IOP measured non-invasively after topical application. We conclude that derivatives of the highly-selective A3AR agonist Cl-IB-MECA can reduce IOP upon reaching their intraocular target, and that nucleoside-based derivatives are promising A3 antagonists for study in multiple animal models.

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Year:  2009        PMID: 19878673      PMCID: PMC2789191          DOI: 10.1016/j.exer.2009.10.001

Source DB:  PubMed          Journal:  Exp Eye Res        ISSN: 0014-4835            Impact factor:   3.467


  33 in total

1.  A(1)-, A(2A)- and A(3)-subtype adenosine receptors modulate intraocular pressure in the mouse.

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2.  Reliable measurement of mouse intraocular pressure by a servo-null micropipette system.

Authors:  M Y Avila; D A Carré; R A Stone; M M Civan
Journal:  Invest Ophthalmol Vis Sci       Date:  2001-07       Impact factor: 4.799

3.  Inhibitors of NHE-1 Na+/H+ exchange reduce mouse intraocular pressure.

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6.  Noninvasive intraocular pressure measurements in mice by pneumotonometry.

Authors:  Marcel Y Avila; Alejandro Múnera; Arcadio Guzmán; Chi Wai Do; Zhao Wang; Richard A Stone; Mortimer M Civan
Journal:  Invest Ophthalmol Vis Sci       Date:  2005-09       Impact factor: 4.799

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Review 3.  G protein-coupled adenosine (P1) and P2Y receptors: ligand design and receptor interactions.

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Journal:  Biochim Biophys Acta       Date:  2010-12-23

6.  Adenosine receptor distribution in Rhesus monkey ocular tissue.

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Journal:  Exp Eye Res       Date:  2018-05-21       Impact factor: 3.467

7.  Selectivity is species-dependent: Characterization of standard agonists and antagonists at human, rat, and mouse adenosine receptors.

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Journal:  Purinergic Signal       Date:  2015-07-01       Impact factor: 3.765

Review 8.  Exciting directions in glaucoma.

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Review 9.  Ocular Purine Receptors as Drug Targets in the Eye.

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Review 10.  Genomic and proteomic pathophysiology of pseudoexfoliation glaucoma.

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Journal:  Int Ophthalmol Clin       Date:  2014
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