LAUSR

Sustained and intermittent hypoxia produces vasoconstriction, arterial remodeling, and hypertension in the lung. Stromal interaction molecule (STIM)-activated Transient Receptor Potential Channels (TRPC) and Calcium Release-Activated Calcium Channel Protein (ORAI) Channels (STOC) play a key role in the progression of pulmonary hypertension in pre-clinical models of animals submitted to sustained and intermittent hypoxia. The available evidence supports the theory that oxidative stress and hypoxic inducible factors upregulate and activate STIM-activated TRPC-ORAI Ca2+ channels, contributing to the pulmonary remodeling and hypertension induced by sustained hypoxia. However, less is known about the effects of oxidative stress and hypoxic inducible factors on the modulation of STIM-activated TRPC-ORAI channels following chronic intermittent hypoxia. In this review, we examined the emerging evidence supporting the theory that oxidative stress and hypoxic inducible factors induced by intermittent hypoxia upregulate and activate STIM-activated TRPC-ORAI Ca2+ channels. In addition, we used bioinformatics tools to search in public databases for the genes involved in the upregulation of STIM-activated TRPC-ORAI Ca2+ channels, and to compare the differential gene expression and biological processes induced by intermittent and sustained hypoxia in lung cells.