Faculty Bibliography
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61
PPP2R5D Genetic Mutations and Early-Onset Parkinsonism [Letter]
PMID: 33098144
ISSN: 1531-8249
CID: 4734472
Neurologic Manifestations of Systemic Disease: Movement Disorders [Review]
ISI:000608049000003
ISSN: 1092-8480
CID: 4773982
Looking "Cherry Red Spot Myoclonus" in the Eyes: Clinical Phenotype, Treatment Response, and Eye Movements in Sialidosis Type 1
Sialidosis type 1 is a rare lysosomal storage disorder caused by mutations of the neuraminidase gene. Specific features suggesting this condition include myoclonus, ataxia and macular cherry-red spots. However, phenotypic variability exists. Here, we present detailed clinical and video description of three patients with this rare condition. We also provide an in-depth characterization of eye movement abnormalities, as an additional tool to investigate pathophysiological mechanisms and to facilitate diagnosis. In our patients, despite phenotypic differences, eye movement deficits largely localized to the cerebellum.
PMCID:8681143
PMID: 34992946
ISSN: 2160-8288
CID: 5107412
Alcohol-Responsive Hyperkinetic Movement Disorders-a Mechanistic Hypothesis
Patients with essential tremor, vocal tremor, torticollis, myoclonus-dystonia and posthypoxic myoclonus often benefit in a surprisingly rapid and robust manner from ingestion of a modest amount of alcohol (ethanol). Despite considerable investigation, the mechanism of ethanol's ability to produce this effect remains a mystery. In this paper, we review the pharmacology of ethanol and its analogue GHB (or sodium oxybate), summarize the published literature of alcohol-responsive hyperkinetic movement disorders, and demonstrate videos of patients we have treated over the last fifteen years with either an ethanol challenge or with chronic sodium oxybate therapy. We then propose a novel explanation for this phenomenon-namely, that ingestion of
PMCID:7597582
PMID: 33178485
ISSN: 2160-8288
CID: 4684342
RBD and autonomic dysfunction in newly diagnosed Parkinson's disease patients [Meeting Abstract]
Objective: To determine whether newly diagnosed Parkinson's disease (PD) patients with REM sleep behavior disorder (RBD) are more likely to have symptoms of autonomic dysfunction.
Background(s): RBD is highly associated with development of asynucleinopathies but only 51% of PD patients have RBD1,2. We addressed whether PD with and without RBD have different clinical phenotypes and progression.
Method(s): Hypothesis driven analysis of 295 early stage PD patients within 2 years from diagnosis on no PD medications from the Parkinson's Progressive Marker Initiative (PPMI) cohort were obtained. Genetic, SWEED and prodromal subgroups were excluded from analysis. RBDSQ equal or greater than 1 for item 6 (q6) was used to identify patients with RBD as this cutoff has greater sensitivity and specificity for identifying true RBD in PD3,4 Results: Subjects from baseline visit were divided in RBD+ (RBDSQ q6>1, n=128) and RBD- (RBDSQ q6<1, n=167). We considered SCOPA subscores (gastrointestinal(GI), urinary(UR), thermoregulation(THERM), cardiovascular(CV), pupillomotor(PM), sex(SEX)), sense of smell (UPSIT), anxiety (STAIT-trait), depression (GDS), motor (updrs-part3) and cognitive function (MOCA), UPDRS total score. Shapiro-Wilk and Mann-Whitney test for non-parametric data were used for the analyses. SCOPA sub-scores for the majority of the autonomic symptoms (GI, THERM, CV, PM) but not UR and SEX, were significantly higher in the REM+ cohort (p=<0.005). The other traits did not show statistically significant differences. Statistical significance between the two groups for GI, THERM, CV remained consistent using other thresholds for differentiating REM+ vs REM- groups (RBDSQ total score greater than 5 or combined RBDSQ total score and q6).
Conclusion(s): Our hypothesis driven analyses show that early stage PD patients with RBD have greater prevalence of autonomic symptoms, without worse UPDRS motor scores. This suggests that brainstem and peripheral autonomic symptoms cluster together, but are not associated with more diffuse involvement of motor systems and cognitive impairment at this early stage of PD. Prior analyses of PPMI data have identified a "diffuse/ malignant" subtype associated with higher UPDRS motor score, RBDSQ score, autonomic symptoms (SCOPA-AUT) and worse cognitive impairment5.6. These differences might be accounted by our more stringent criteria for RBD or our statistical approach using specific hypothesis versus cluster driven analyses
Background(s): RBD is highly associated with development of asynucleinopathies but only 51% of PD patients have RBD1,2. We addressed whether PD with and without RBD have different clinical phenotypes and progression.
Method(s): Hypothesis driven analysis of 295 early stage PD patients within 2 years from diagnosis on no PD medications from the Parkinson's Progressive Marker Initiative (PPMI) cohort were obtained. Genetic, SWEED and prodromal subgroups were excluded from analysis. RBDSQ equal or greater than 1 for item 6 (q6) was used to identify patients with RBD as this cutoff has greater sensitivity and specificity for identifying true RBD in PD3,4 Results: Subjects from baseline visit were divided in RBD+ (RBDSQ q6>1, n=128) and RBD- (RBDSQ q6<1, n=167). We considered SCOPA subscores (gastrointestinal(GI), urinary(UR), thermoregulation(THERM), cardiovascular(CV), pupillomotor(PM), sex(SEX)), sense of smell (UPSIT), anxiety (STAIT-trait), depression (GDS), motor (updrs-part3) and cognitive function (MOCA), UPDRS total score. Shapiro-Wilk and Mann-Whitney test for non-parametric data were used for the analyses. SCOPA sub-scores for the majority of the autonomic symptoms (GI, THERM, CV, PM) but not UR and SEX, were significantly higher in the REM+ cohort (p=<0.005). The other traits did not show statistically significant differences. Statistical significance between the two groups for GI, THERM, CV remained consistent using other thresholds for differentiating REM+ vs REM- groups (RBDSQ total score greater than 5 or combined RBDSQ total score and q6).
Conclusion(s): Our hypothesis driven analyses show that early stage PD patients with RBD have greater prevalence of autonomic symptoms, without worse UPDRS motor scores. This suggests that brainstem and peripheral autonomic symptoms cluster together, but are not associated with more diffuse involvement of motor systems and cognitive impairment at this early stage of PD. Prior analyses of PPMI data have identified a "diffuse/ malignant" subtype associated with higher UPDRS motor score, RBDSQ score, autonomic symptoms (SCOPA-AUT) and worse cognitive impairment5.6. These differences might be accounted by our more stringent criteria for RBD or our statistical approach using specific hypothesis versus cluster driven analyses
EMBASE:633837161
ISSN: 1531-8257
CID: 4756922
GBA and ATP13A mutation and PD: clinical phenotype and pathogenic implications [Meeting Abstract]
ISI:000536058007138
ISSN: 0028-3878
CID: 4561722
Looking "cherry red spot myoclonus" in the eyes [Meeting Abstract]
ISI:000536058002129
ISSN: 0028-3878
CID: 4561232
Ataxia Telangiectasia (Louis-Bar Syndrome)
Treasure Island (FL): StatPearls Publishing; 2019
pp. -
ISBN:
CID: 4194652
Early-onset pathologically proven multiple system atrophy with LRRK2 G2019S mutation [Letter]
PMCID:6642007
PMID: 31077434
ISSN: 1531-8257
CID: 4028652
Case Report: Hemiparkinsonism in a Patient With Multiple Sclerosis [Case Report]
ORIGINAL:0013418
ISSN: 1540-1367
CID: 3896432
