The Relationship between Paroxysmal Kinesigenic Choreoathetosis and Epilepsy

Ohmori, Iori; Ohtsuka, Yoko; Ogino, T.; Yoshinaga, Harumi; Kobayashi, Katsuhiro; Oka, Eiji

doi:10.1055/s-2002-23594

Cited by 24 publications

(12 citation statements)

References 20 publications

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“…Clinically, paroxysmal dyskinesias display common features with other paroxysmal central nervous system disorders considered to be disorders of ion channels, thus suggesting a common pathophysiologic mechanism: episodic attacks on a normal interictal background and similar precipitating causes. Moreover, all these paroxysmal disorders exhibit analogies and associations between them, also in the same family (Ohmori et al 2002;Margari et al 2005). As low doses of carbamazepine are highly effective in PKC, and it acts by inhibiting the excitability of cellular membranes through inactivating the sodium channel (Wein et al 1996), a mutation of an ion-channel gene is suspected to underlie PKC.…”

Section: Discussionmentioning

confidence: 99%

Localization and Mutation Detection for Paroxysmal Kinesigenic Choreoathetosis

Bao

Wang

et al. 2007

J Mol Neurosci

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Section: Discussionmentioning

confidence: 99%

Localization and Mutation Detection for Paroxysmal Kinesigenic Choreoathetosis

Bao

Wang

et al. 2007

J Mol Neurosci

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“…However, increased understanding of the genetics underpinnings of epilepsy syndromes and PxDs have provided insights into the shared mechanisms of these two conditions, revealing the role of ion channels, and of proteins associated to the vesical synaptic cycle or involved in energy metabolism (figure 3) [14,31,36,38,43,53,70–72]. Nevertheless, there remains controversy about the extent to which paroxysmal movement disorder may have epileptic components, as variably measured by video-EEG monitoring [9,73–75], recognizing that abnormally organized electrical activity of subcortical structures (“subcortical seizures”) may not be readily recorded with scalp electrodes. In general, a clear differentiation between the pathophysiology of purely subcortical and cortical events risks to be an oversimplification due to the strong reciprocal interconnectivity between basal ganglia and cerebral cortex, particularly within the fronto-striatal network, as well as the differential age-related expression of dysfunction in these structures.…”

Section: Knowledge Gaps and Future Perspectivesmentioning

confidence: 99%

The epileptic and nonepileptic spectrum of paroxysmal dyskinesias: Channelopathies, synaptopathies, and transportopathies

et al. 2017

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Historically, the syndrome of primary paroxysmal dyskinesias was considered a group of disorders due to ion channel dysfunction. This proposition was primarily based on the discovery of mutations in ion channels, which caused other episodic neurological disorders such as epilepsy and migraine and also supported by the frequent association between paroxysmal dyskinesias and epilepsy. However, the discovery of the genes responsible for the three classic forms of paroxysmal dyskinesias disproved this ion channel theory. On the other hand, novel gene mutations implicating ion channels have been recently reported to produce episodic movement disorders clinically similar to the classical paroxysmal dyskinesias. Here, we review the clinical and pathophysiological aspects of the paroxysmal dyskinesias, further proposing a pathophysiological framework according to which they can be classified as synaptopathies (PRRT2 and MR1), channelopathies (KCNMA1 and SCN8A) or transportopathies (SLC2A1). This proposal might serve to explain similarities and differences among the various paroxysmal dyskinesias in terms of clinical features, treatment response, and natural history.

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“…The brief, stereotyped nature and the dramatic response to anticonvulsants argue for an epileptic origin 13. However, EEG studies and sleep EEGs fail to show typical ictal or interictal changes14 with few exceptions 15–17. Thus, some suggest a subcortical origin of the epileptogenic source, in the basal ganglia 16…”

Section: Paroxysmal Kinesigenic Dyskinesia (Pkd)mentioning

confidence: 99%

Paroxysmal dyskinesias

Bhatia¹

2011

Movement Disorders

158

127

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Paroxysmal movement disorders are a relatively rare and heterogenous group of conditions manifesting as episodic dyskinesia lasting a brief duration. Three forms are clearly recognized, namely, paroxysmal kinesigenic (PKD), nonkinisegenic (PNKD), and exercise induced (PED). There have been major advances in the understanding of the pathophysiological mechanisms and the genetics of these disorders, leading to better clinical definitions based on genotype-phenotype correlations in the familial idiopathic forms. PKD is genetically heterogenous, but there is linkage to chromosome 16 in a number of families. PNKD is due to mutations of the MR-1 gene. PED is genetically heterogenous, but a number of familial and sporadic cases may be due to GLUT-1 gene mutations. The GLUT1 gene-related form of PED may respond to a ketogenic diet. Potassium and calcium channel mutations underlie the 2 main forms of episodic ataxia (EA1 and EA2), whereas benign torticollis of infancy may also be a calcium channel disorder.

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The Relationship between Paroxysmal Kinesigenic Choreoathetosis and Epilepsy

Abstract: It appears that patients who suffer from both PKC and epilepsy have a functional abnormality of the cerebral cortex, particularly in the perirolandic and frontal regions.

Cited by 24 publications

References 20 publications

Localization and Mutation Detection for Paroxysmal Kinesigenic Choreoathetosis

Localization and Mutation Detection for Paroxysmal Kinesigenic Choreoathetosis

The epileptic and nonepileptic spectrum of paroxysmal dyskinesias: Channelopathies, synaptopathies, and transportopathies

Paroxysmal dyskinesias

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