Atriopeptin, sodium azide and cyclic GMP reduce secretion of aqueous humour and inhibit intracellular calcium release in bovine cultured ciliary epithelium

This study examined the involvement of cyclic GMP, protein kinase G and intracellular Ca 2+ movements in the modulation of aqueous humour formation. Using the bovine arterially‐perfused eye preparation, drug effects on intraocular pressure and aqueous humour formation rate were measured by manometry and fluorescein dilution, respectively. Drug effects on intracellular [Ca 2+ ] were determined by fura‐2 fluorescence ratio technique in non‐transformed, cultured ciliary epithelium. Intra‐arterial injection of atriopeptin (50 pmol) or sodium azide (10 nmol) produced significant reduction in aqueous humour formation (>38%). This was blocked by selective inhibition (KT‐5823) of protein kinase G, but not by selective inhibition (KT‐5720) of protein kinase A. Reductions of intraocular pressure produced by atriopeptin or azide were almost completely blocked by KT‐5823. ATP (100 μ M ) caused rapid, transient increase in intracellular Ca 2+ followed by a slow decline and prolonged plateau. This response showed concentration‐dependent inhibition by atriopeptin, azide or 8‐bromo cyclic GMP, and this inhibition of the rapid (peak) Ca 2+ increase was enhanced by zaprinast (100 μ M ; phosphodiesterase inhibitor). KT‐5823 blocked the suppression of the peak Ca 2+ response but not suppression of the plateau. Arterial perfusion of ATP (0.1–100 μ M ) produced a concentration‐dependent decrease in aqueous humour formation. Aqueous humour formation in the bovine eye can be manipulated through cyclic GMP, operating via protein kinase G. Close parallels appear when Ca 2+ movements are modified by similar manipulations of cyclic GMP, suggesting that Ca 2+ transients may play an important role in aqueous humour formation and that interplay occurs between cyclic GMP and Ca 2+ .British Journal of Pharmacology (1999) 127 , 1438–1446; doi: 10.1038/sj.bjp.0702681