Physiological and pathological regulation of ca2+ dynamics
occur in myocytes through a number of kinases including the CaMKII
(Ca2+/calmodulin-kinase type-II), PKA (protein kinase A), JNK
(c-Jun N-terminal kinase) signaling pathways. Sleep disordered breathing (SDB)
facilitates proarrhythmic activities and atrial fibrillation through a
CaMKII-dependent dysregulation of INa,L and sarcoplasmic reticulum
(SR) Ca2+ mishandling. SDB may act as a cellular stressor manifesting
its affects via hypoxia-ischemic input which could involve the PKA and JNK
pathways or other yet to be identified pathways. β-AR indicates
β-adrenergic receptor; AC, adenylyl cyclase; c-AMP, cyclic adenine
monophosphate; CaM, calmodulin; DAD, delayed afterdepolarization; EAD, early
afterdepolarization; INa,L, late Na channel; ICa,
Ca2+ current; NCX, Na+/Ca2+ exchanger; PLB,
phospholipase B; and ROS, reactive oxygen species.