Regulation of CRAC channels by Ca2+-dependent inactivation

CRAC channels are a major route for Ca²⁺ influx in eukaryotic cells. The channels show prominent Ca²⁺-dependent inactivation through two spatially and temporally distinct mechanisms: fast inactivation, which develops over milliseconds and is triggered by Ca²⁺ near the mouth of the channel and slow inactivation, which arises over tens of seconds and requires a rise in global cytosolic Ca²⁺. Slow inactivation is controlled physiologically by Ca²⁺ uptake into mitochondria through the MCU. Site-directed mutagenesis studies on STIM1 and Orai1 have led to new molecular insight into how fast inactivation occurs. This review describes properties and molecular mechanisms that contribute to these important Ca²⁺-dependent inhibitory pathways.