A ‘sticky’ interhemispheric switch in bipolar disorder?

Despite years of research into bipolar disorder (manic depression), its underlying pathophysiology remains elusive. It is widely acknowledged that the disorder is strongly heritable, but the genetics are complex with less than full concordance in monozygotic twins and at least four susceptibility lo...

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Published inProceedings of the Royal Society. B, Biological sciences Vol. 265; no. 1411; pp. 2141 - 2148
Main Authors Pettigrew, J. D., Miller, S. M.
Format Journal Article
LanguageEnglish
Published England The Royal Society 22.11.1998
Subjects
Adult
Behavioral neuroscience
Binocular Rivalry
Bipolar Disorder
Bipolar Disorder - genetics
Bipolar Disorder - physiopathology
Brain - physiology
Brain - physiopathology
Cerebral hemispheres
Female
Functional Laterality
Genetic variation
Genetics
Humans
Interhemispheric Switching
Lesions
Male
Medical genetics
Middle Aged
Models, Neurological
Models, Psychological
Mood
Mood disorders
Oscillators
Prefrontal cortex
Psychomotor Performance - physiology
Reference Values
Rivalry
Vision, Binocular - genetics
Vision, Binocular - physiology
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Summary:Despite years of research into bipolar disorder (manic depression), its underlying pathophysiology remains elusive. It is widely acknowledged that the disorder is strongly heritable, but the genetics are complex with less than full concordance in monozygotic twins and at least four susceptibility loci identified. We propose that bipolar disorder is the result of a genetic propensity for slow interhemispheric switching mechanisms that become 'stuck' in one or the other state. Because slow switches are also 'sticky' when compared with fast switches, the clinical manifestations of bipolar disorder may be explained by hemispheric activation being 'stuck' on the left (mania) or on the right (depression). Support for this 'sticky' interhemispheric switching hypothesis stems from our recent observation that the rate of perceptual alternation in binocular rivalry is slow in euthymic subjects with bipolar disorder (n=18, median = 0.27Hz) compared with normal controls (n=49, median = 0.60Hz, p0.0005). We have presented evidence elsewhere that binocular rivalry is itself an interhemispheric switching phenomenon. The rivalry alternation rate (putative interhemispheric switch rate) is robust in a given individual, with a test-retest correlation of more than 0.8, making it suitable for genetic studies. The interhemispheric switch rate may provide a trait-dependent biological marker for bipolar disorder.
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ISSN:0962-8452
1471-2954
DOI:10.1098/rspb.1998.0551