Abstract
ObjectiveAtriopeptin, acting through cGMP, inhibits NHE1 in the bovine ocular non‐pigmented ciliary epithelium (NPE)1. Here we examined NHE isoforms and tested whether SNP, a NO donor and a stimulator of cGMP, alters intracellular pH (pHi) responses.MethodsNHE isoforms in native and cultured NPE were detected by immunohistochemistry and immunoblot. BCECF fluorescence imaging was used to study the effect of drugs on pHi recovery after an acid load.ResultsNative and cultured NPE expressed NHE1 and NHE4 isoforms. pHi recovery in NPE was Na‐dependent and had DIDS and amiloride sensitive components. SNP inhibited pHi recovery concentration‐dependently. L‐arginine, the NOS substrate, also slowed pHi recovery. Dimethyl amiloride (DMA), a potent inhibitor of NHE, caused substantial inhibition of pHi recovery at 100μM. In cells exposed to both SNP and DMA, the degree of inhibition of pHi recovery was similar to that elicited by SNP alone. The cyclic GMP analog 8‐pCPT‐cGMP (10μM) mimicked the SNP effect. The inhibitory effect of SNP on pHi recovery was suppressed by 1μM H‐8, an inhibitor of cGMP‐dependent protein kinase.ConclusionPrimary cultures of porcine NPE express NHE isoforms found in native cells. NO donors slow pHi recovery through inhibition of NHE. The effect of NO donors on NHE involves a cGMP‐PKG signal transduction pathway.Funding: NIH‐EY06915
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