Conte A1,2, McGovern E3,4, Narasiham S5,6,7, Beck R5,6,7, Killian O5,6,7, Oriordan S3,4,
Reilly RB5,6,7, Hutchinson M3,4
Front Neurol. 2017 Nov 28;8:625. doi: 10.3389/fneur.2017.00625. eCollection 2017.
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1 |
Department of Neurology and Psychiatry, Sapienza, University of Rome, Rome, Italy. |
2 |
IRCCS Neuromed, Pozzilli, Isernia, Italy. |
3 |
Department of Neurology, St Vincent’s University Hospital Dublin, Dublin, Ireland. |
4 |
School of Medicine and Medical Science, University College Dublin, Dublin, Ireland. |
5 |
Trinity Centre for Bioengineering, Trinity College, The University of Dublin, Dublin, Ireland. |
6 |
School of Medicine, Trinity College, The University of Dublin, Dublin, Ireland. |
7 |
School of Engineering, Trinity College, The University of Dublin, Dublin, Ireland. |
ABSTRACT:
Temporal discrimination is the ability to determine that two sequential sensory stimuli are separated in time. For any individual, the temporal discrimination threshold (TDT) is the minimum interval at which paired sequential stimuli are perceived as being asynchronous; this can be assessed, with high test-retest and inter-rater reliability, using a simple psychophysical test. Temporal discrimination is disordered in a number of basal ganglia diseases including adult-onset dystonia, of which the two most common phenotypes are cervical dystonia and blepharospasm. The causes of adult-onset focal dystonia are unknown; genetic, epigenetic, and environmental factors are relevant. Abnormal TDTs in adult-onset dystonia are associated with structural and neurophysiological changes considered to reflect defective inhibitory interneuronal processing within a network which includes the superior colliculus, basal ganglia, and primary somatosensory cortex. It is hypothesized that abnormal temporal discrimination is a mediational endophenotype and, when present in unaffected relatives of patients with adult-onset dystonia, indicates non-manifesting gene carriage. Using the mediational endophenotype concept, etiological factors in adult-onset dystonia may be examined including (i) the role of environmental exposures in disease penetrance and expression; (ii) sexual dimorphism in sex ratios at age of onset; (iii) the pathogenesis of non-motor symptoms of adult-onset dystonia; and (iv) subcortical mechanisms in disease pathogenesis.
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Copyright: © 2017 Conte, McGovern, Narasimham, Beck, Killian, O’Riordan, Reilly and Hutchinson. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) or licensor are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.