Striatal Dopaminergic Deficit and Sleep in Idiopathic Rapid Eye Movement Behaviour Disorder: An Explorative Study

• Published in: Nature and science of sleep Vol. 13; pp. 1 - 9
• Main Authors: Wasserman, Danielle, Bindman, Dorothea, Nesbitt, Alexander D, Cash, Diana, Milosevic, Milan, Francis, Paul T, Chaudhuri, K Ray, Leschziner, Guy D, Ferini-Strambi, Luigi, Ballard, Clive, Eccles, Amy, Rosenzweig, Ivana
• Format: Journal Article
• Language: English
• Published: New Zealand Dove Medical Press Limited 01.01.2021; Dove; Dove Medical Press
• Subjects: Brain research; datscan; isolated rapid eye movement behaviour disorder; Medical research; Medicine, Experimental; Mental illness; Muscles; Original Research; polysomnography; Sleep; sleep architecture; striatal dopamine transporter uptake tracer signalling imaging; striatum; Tracers (Biology); United Kingdom; DaTSCAN; sleep architecture; isolated rapid eye movement behaviour disorder; polysomnography; striatal dopamine transporter uptake tracer signalling imaging; striatum
• ISSN: 1179-1608; 1179-1608
• DOI: 10.2147/NSS.S267037

Idiopathic rapid eye movement (REM) sleep behavior disorder (iRBD) is increasingly recognised as an important precursor disease state of alpha-synucleinopathies. This parasomnia is characterized by a history of recurrent nocturnal dream enactment behaviour, loss of skeletal muscle atonia, and increased phasic muscle activity during REM sleep. Neuroimaging studies of striatal dopamine transporter uptake tracer signaling suggest increasing dopaminergic deficit across the continuum of the alpha-synucleinopathies, with early sleep dysfunction suggestive of early caudate dysfunction. Henceforth, we set out to investigate the relationship between early sleep changes and the striatal dopaminergic availability in iRBD. Twelve patients with iRBD, who had undergone a video polysomnography and a neuroimaging assessment of striatal dopamine transporter (DaT) uptake tracer signaling, and 22 matched controls who had similarly undergone a video polysomnography were retrospectively identified. Data were statistically analyzed to identify altered sleep parameters and correlate them with striatal dopamine transporter uptake tracer signaling. The iRBD patients exhibited an increased number of periodic limb movements during sleep ( =0.001), compared to 22 age-matched healthy subjects. In addition, several significant links were found between regional DaT-uptakes and sleep architecture. Correlational analyses suggested a strong positive association between sleep fragmentation and dopamine deficiency in left caudate (r=-0.630, =0.028), whilst an increased uptake in the whole striatum was strongly linked to the sleep efficiency, and to a lesser degree to the length of sleep duration. To the best of our knowledge, this is the first demonstration of a close relationship between dopaminergic availability in striatum and the quality of sleep in iRBD. Taken together, our exploratory findings suggest that subtle but functionally significant striatal changes in early stages of iRBD may contribute to the further shaping of sleep architecture.