Type I nitric oxide synthase fully accounts for NADPH-diaphorase in rat striatum, but not cortex

Abstract

The novel gaseous neuromediator nitric oxide is thought to play an important role in development and plasticity. Despite this, gene-knockout mice lacking neuronal (Type I) nitric oxide synthase exhibit relatively normal brain development and behavior. The nervous system of these mice (especially the forebrain) retains some calcium-dependent nitric oxide synthesis, presumably reflecting other isozymes. Type I nitric oxide synthase has NADPH-dependent diaphorase activity. However, this stain also recognizes other isozymes, and it remains controversial whether all diaphorase-positive neurons contain Type I nitric oxide synthase. To assess whether neurons containing another isoform of nitric oxide synthase may be present in the forebrain of normal rodents, we studied co-localization of diaphorase staining with immunocytochemistry for Type I nitric oxide synthase. Co-localization was complete in the striatum, but some neurons deep in cortex were diaphorase-positive and immunonegative, and therefore may contain a splice variant or novel isozyme of nitric oxide synthase.