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Hyperkinetic Movement Disorders

Chapter by: Ramdhani, Ritesh A; Frucht, Steven J
in: Mount Sinai expert guides : Neurology by Sealfon, Stuart C; Motiwala, Rajeev; Stacy, Charles B (Eds)
Chichester, West Sussex ; Hoboken, NJ : John Wiley & Sons Inc., 2016
pp. 282-294
ISBN: 1118621085paperback
CID: 2764092

Early Use of 60 Hz Frequency Subthalamic Stimulation in Parkinson's Disease: A Case Series and Review [Case Report]

Ramdhani, Ritesh A; Patel, Amar; Swope, David; Kopell, Brian H
BACKGROUND: Deep brain stimulation (DBS) is effective in treating the segmental symptoms of Parkinson's disease (PD) as well as axial symptoms that are levodopa responsive. PD patients on chronic DBS who develop axial symptoms and gait disturbances several years later oftentimes are refractory to high frequency stimulation (HFS). Several studies report benefit produced by low frequency subthalamic nucleus (STN) stimulation in such patients, though the sustainability of the effects has been mixed. OBJECTIVE: To report the clinical outcomes of a series of patients with Parkinson's disease and levodopa responsive axial and gait disturbances who were switched to 60 Hz stimulation within one year of their DBS surgery. METHODS: A retrospective review of 5 patients, whose severe pre-DBS, levodopa responsive gait disorders worsened on HFS STN-DBS and were subsequently switched to 60 Hz stimulation within 1 year of their surgery. RESULTS: The median age of this cohort was 66 years with median disease duration of 14 years. Four of 5 patients' experienced acute worsening of their axial and gait UPDRS III scores on HFS. All patients' gait disorder improved with 60 Hz along with amelioration of their segmental symptoms and reduction of their levodopa induced dyskinesia. The median time on HFS prior to switching to 60 Hz was two months. Stimulation through the ventral contacts was utilized in all patients with relatively modest changes achieved in levodopa equivalent daily dose. CONCLUSION: This case series demonstrates the clinical efficacy of utilizing low frequency (60 Hz) STN stimulation early in the DBS programming course in more advanced PD patients with levodopa responsive gait disturbance and freezing of gait. Activation of a broader stimulation field likely contributed to both axial and segmental symptom improvement while possibly aiding in the reduction of dyskinesia.
PMID: 25833008
ISSN: 1525-1403
CID: 2698032

Pseudobulbar laughter as a levodopa off phenomenon exacerbated by subthalamic deep brain stimulation

Chattha, P K; Greene, P E; Ramdhani, Ritesh A
Pseudobulbar affect is a common symptom in neurodegenerative diseases and can also result from lesions in cortical, subcortical and brainstem regions. In Parkinson's disease (PD), pseudobulbar affect (PBA) can occur as a wearing off phenomenon, manifested usually as crying without emotionality. In addition, subthalamic (STN) deep brain stimulation (DBS) has been reported to induce PBA in PD patients with no prior history of such episodes. We present a case of inappropriate laughter lacking mirth as a levodopa OFF phenomenon in a patient with PD, whose laughter also worsened with STN-DBS in his non-medicated state. Levodopa ameliorated his PBA both with and without stimulation. The case demonstrates pseudobulbar laughter as a levodopa OFF phenomenon that is also exacerbated by STN-DBS.
PMCID:4711012
PMID: 26788349
ISSN: 2054-7072
CID: 2698012

What's special about task in dystonia? A voxel-based morphometry and diffusion weighted imaging study

Ramdhani, Ritesh A; Kumar, Veena; Velickovic, Miodrag; Frucht, Steven J; Tagliati, Michele; Simonyan, Kristina
Numerous brain imaging studies have demonstrated structural changes in the basal ganglia, thalamus, sensorimotor cortex, and cerebellum across different forms of primary dystonia. However, our understanding of brain abnormalities contributing to the clinically well-described phenomenon of task specificity in dystonia remained limited. We used high-resolution magnetic resonance imaging (MRI) with voxel-based morphometry and diffusion weighted imaging with tract-based spatial statistics of fractional anisotropy to examine gray and white matter organization in two task-specific dystonia forms, writer's cramp and laryngeal dystonia, and two non-task-specific dystonia forms, cervical dystonia and blepharospasm. A direct comparison between both dystonia forms indicated that characteristic gray matter volumetric changes in task-specific dystonia involve the brain regions responsible for sensorimotor control during writing and speaking, such as primary somatosensory cortex, middle frontal gyrus, superior/inferior temporal gyrus, middle/posterior cingulate cortex, and occipital cortex as well as the striatum and cerebellum (lobules VI-VIIa). These gray matter changes were accompanied by white matter abnormalities in the premotor cortex, middle/inferior frontal gyrus, genu of the corpus callosum, anterior limb/genu of the internal capsule, and putamen. Conversely, gray matter volumetric changes in the non-task-specific group were limited to the left cerebellum (lobule VIIa) only, whereas white matter alterations were found to underlie the primary sensorimotor cortex, inferior parietal lobule, and middle cingulate gyrus. Distinct microstructural patterns in task-specific and non-task-specific dystonias may represent neuroimaging markers and provide evidence that these two dystonia subclasses likely follow divergent pathophysiological mechanisms precipitated by different triggers.
PMCID:4139455
PMID: 24925463
ISSN: 1531-8257
CID: 2698042

Isolated chorea associated with LGI1 antibody [Meeting Abstract]

Ramdhani, RA; Frucht, SJ
ISI:000337693401132
ISSN: 1531-8257
CID: 2785752

Isolated Chorea Associated with LGI1 Antibody

Ramdhani, Ritesh A; Frucht, Steven J
BACKGROUND: Leucine-rich glioma inactivated 1 (LGI1) antibody produces a syndrome of limbic encephalitis, hyponatremia, and facio-brachial dystonic seizures that is non-paraneoplastic and responsive to corticosteroids. Parkinsonism, tremor, and generalized chorea are rare manifestations of LGI1, but, when present, commonly accompany other signs of limbic encephalitis. CASE REPORT: We present a case of LGI1-related isolated chorea in a 53-year-old Japanese male. His chorea responded to high-dose steroids, suggesting a potential role for this synaptic antibody in triggering chorea. DISCUSSION: This case highlights a new treatable etiology of chorea.
PMCID:3889335
PMID: 24459615
ISSN: 2160-8288
CID: 2698062

Movement disorders emergencies

Chapter by: Ramdhani, Ritesh A; Frucht, Steven J
in: MOVEMENT DISORDERS IN NEUROLOGIC AND SYSTEMIC DISEASE by Poewe, W; Jankovic, J [Eds]
CAMBRIDGE : CAMBRIDGE UNIV PRESS, 2014
pp. 419-441
ISBN:
CID: 2698092

Reply to: Hemichorea Associated with CASPR2 Antibody [Letter]

Ramdhani, Ritesh A; Frucht, Steven J
This letter was written in reply to this letter to the editor: Vynogradova I, Savitski V, Heckmann JG. Hemichorea associated with CASPR2 antibody. Tremor Other Hyperkinet Mov. 2014; 4. doi: 10.7916/D8VM49C5. The above letter to the editor was written in response to this article: Ramdhani RA, Frucht SJ. Isolated Chorea Associated with LGI1 Antibody. Tremor Other Hyperkinet Mov. 2014; 4. doi: 10.7916/D8MG7MFC.
PMCID:4039211
PMID: 24918026
ISSN: 2160-8288
CID: 2698052

Morphometric changes in task- and non-task-specific focal dystonias: A comparative analysis [Meeting Abstract]

Ramdhani, RA; Choy, M; Velickovic, M; Frucht, SJ; Tagliati, M; Simonyan, K
ISI:000320940500031
ISSN: 0885-3185
CID: 2785742

Primary dystonia: conceptualizing the disorder through a structural brain imaging lens

Ramdhani, Ritesh A; Simonyan, Kristina
BACKGROUND: Dystonia is a hyperkinetic movement disorder characterized by involuntary, repetitive twisting movements. The anatomical structures and pathways implicated in its pathogenesis and their relationships to the neurophysiological paradigms of abnormal surround inhibition, maladaptive plasticity, and impaired sensorimotor integration remain unclear. OBJECTIVE: We review the use of high-resolution structural brain imaging using voxel-based morphometry (VBM) and diffusion tensor imaging (DTI) techniques for evaluating brain changes in primary torsion dystonia and their relationships to the pathophysiology of this disorder. METHODS: A PubMed search was conducted to identify relevant literature. RESULTS: VBM and DTI studies produced somewhat conflicting results across different forms of primary dystonia and reported increases, decreases, or both in gray matter volume and white matter integrity. However, despite the discrepancies, these studies are consistent in revealing brain abnormalities in dystonia that extend beyond the basal ganglia and involve the sensorimotor cortex and cerebellum. DISCUSSION: Although limited to date, structural magnetic resonance imaging (MRI) studies combined with functional brain imaging and neurophysiological modalities begin to establish structural-functional relationships at different levels of the abnormal basal ganglia, cortical, and cerebellar networks and provide clues into the pathophysiological mechanisms that underlie primary dystonia. Cross-disciplinary studies are needed for further investigations of the interplay between structural-functional brain abnormalities and environmental and genetic risk factors in dystonia patients.
PMCID:3629863
PMID: 23610744
ISSN: 2160-8288
CID: 2698072