Inositol polyphosphates and intracellular calcium release

Abstract

The hydrolysis of inositol lipids triggered by the occupation of cell surface receptors generates several intracellular messengers. Many different inositol phosphate isomers accumulate in stimulated cells. Of these d- myo-inositol 1,4,5-trisphosphate (Ins 1,4,5-P 3) is responsible for discharging Ca 2+ from intracellular stores. Specific membrane binding sites for Ins 1,4,5-P 3 have been detected. The properties of these sites and their possible relationship to the calcium release process is reviewed. Ins 1,4,5-P 3 binding sites may be present in discrete subcellular structures (“calciosomes”). Kinetic and some electrophysiological evidence indicates that Ins 1,4,5-P 3 acts to open a Ca 2+ channel. Recent progress on the purification of the receptor from neuronal tissues is summarized. Phosphorylation of Ins 1,4,5-P 3 by a specific kinase results in the production of d- myo-inositol 1,3,4,5-tetraphosphate (Ins 1,3,4,5-P 4). This inositol phosphate has been reported to increase the entry of Ca 2+ across the plasma membrane, activate nonspecific ion channels in the plasma membrane, alter the Ca 2+ content of the Ins 1,4,5-P 3-releasable store, and bind to and alter the activity of certain enzymes. These data and the possible biological significance of Ins 1,3,4,5-P 4 are discussed.