cover image European Journal of Neurology

European Journal of Neurology

2017 - Volume 24
Issue 5 | May 2017
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Original Paper

Background and purpose

X‐linked dystonia‐parkinsonism (XDP) is an inherited neurodegenerative adult‐onset movement disorder associated with striatal atrophy. As the dopaminergic system has not yet been systemically studied in this basal ganglia model disease, it is unclear whether nigrostriatal dysfunction contributes to parkinsonism in XDP.

Methods

Pre‐ and post‐synaptic dopaminergic function was assessed in XDP. A total of 10 jod‐benzamide (IBZM) single‐photon emission computed tomography (SPECT) images were obtained for nine patients aged 42.3 ± 9.5 years (SD; range 30–52) and one asymptomatic mutation carrier (38 years), and four ioflupane (FP‐CIT) SPECT images were obtained for four patients, aged 41.5 ± 11.6 years (range 30–52 years). Structural magnetic resonance imaging was also performed for all mutation carriers and 10 matched healthy controls.

Results

All patients were men who suffered from severe, disabling segmental or generalized dystonia and had varying degrees of parkinsonism. IBZM SPECT images were pathological in 8/9 symptomatic patients with distinct reduced post‐synaptic tracer uptake in the caudate nucleus and putamen, and unremarkable in the asymptomatic mutation carrier. Longer disease duration was correlated with lower IBZM binding ratios. All subjects exhibited slightly reduced FP‐CIT uptake values compared to controls for each analyzed region (−37% to −41%) which may be linked to basal ganglia volume loss. Visual inspection revealed physiological FP‐CIT uptake in 1/4 patients.

Conclusions

This nuclear imaging study provides evidence that the functional decline of post‐synaptic dopaminergic neurotransmission is related to disease duration and ongoing neurodegeneration. Given the severe striatal cell loss which could be verified with post‐synaptic nuclear imaging, both parkinsonism and dystonia in XDP are probably mainly due to striatal dysfunction.

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Authors:
N. Brüggemann, R. L. Rosales, J. L. Waugh, A. J. Blood, A. Domingo, M. Heldmann, R. D. Jamora, A. Münchau, T. F. Münte, L. V. Lee, I. Buchmann and C. Klein
Article first published online:
25 Feb 2017 | DOI: 10.1111/ene.13256

Original Article

Background and purpose

Data on mortality in patients with epilepsy have been available since the 1800s. They consistently show a 2−3‐fold increase compared to the general population. Despite major advances in diagnostic tools and treatment options, there is no evidence for a decrease in premature deaths. The temporal trend of mortality in a hospital‐based epilepsy cohort over three decades was assessed.

Methods

A hospital‐based incidence cohort was recruited from a specialized epilepsy outpatient clinic at Innsbruck Medical University between 1980 and 2007, divided by decade into three cohorts and followed for 5 years after initial epilepsy diagnosis. Deaths and their primary causes were determined using probabilistic record linkage with the Austrian death registry. Age‐, sex‐ and period‐adjusted standardized mortality rates (SMRs) were computed in relation to the general population of the same area and grouped according to time of diagnosis.

Results

In all, 122 deaths in 4549.9 person‐years (1954.5 women, 2595.2 men) were identified. The overall SMR was 2.2 [95% confidence interval (CI) 1.8–2.6] and decreased from 3.0 (95% CI 2.1–4.3) in 1980–1989, to 2.7 (95% CI 2.0–3.5) in 1990–1999 and to 1.4 (95% CI 1.0–2.0) in 2000–2007.

Conclusions

This study indicates a decrease in mortality in newly diagnosed epilepsy patients over the last three decades. This may be due to advances in diagnosis and treatment over the past three decades, including early identification of drug resistance, introduction of new anti‐epileptic drugs and establishment of a comprehensive epilepsy surgery programme in this region.

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Authors:
C. A. Granbichler, W. Oberaigner, G. Kuchukhidze, J.‐P. Ndayisaba, A. Ndayisaba, A. Taylor, G. Bauer, G. Luef and E. Trinka
Article first published online:
27 Feb 2017 | DOI: 10.1111/ene.13267

Original Article

Background and purpose

Few studies have examined why some patients with dementia stop attending medical consultations. We conducted a retrospective study to investigate factors associated with discontinuous clinic attendance.

Methods

Participants were 988 patients with dementia from university hospital (UH) clinics and affiliated local hospital (LH) clinics. We compared continuous and discontinuous attenders on cognitive and affective functions and activities of daily living (ADL), and also compared UH and LH patients (UH: continuous, = 176; discontinuous, = 207; LH: continuous, = 418; discontinuous, = 187).

Results

The total annual rate of discontinuation was 8.0%, and the mean period of attendance before discontinuation was 2.2 ± 2.4 years (UH, 2.8 ± 3.0; LH, 1.5 ± 1.3, < 0.01). Scores for the Mini‐Mental State Examination, Hasegawa Dementia Scale – Revised, Geriatric Depression Scale, apathy scale, Abe's behavioral and psychological symptoms of dementia (BPSD) score, and ADL were significantly worse in the discontinuous group than the continuous group for both UH and LH patients ( < 0.01). The best predictor of discontinuation was ADL decline (UH and LH) and Abe's BPSD score (UH). The most common reason for discontinuation was returning to the family doctor (39.1% for UH), and cessation of hospital attendance at their own discretion (35.3% for LH).

Conclusions

We identified the main reasons for discontinuation of attendance as returning to the family doctor and cessation of hospital attendance at their own discretion. The best predictors of discontinuation were ADL decline and worsening BPSD. There were significant differences in discontinuation between UH and LH patients with dementia.

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Authors:
N. Hishikawa, Y. Fukui, Y. Nakano, R. Morihara, M. Takemoto, K. Sato, T. Yamashita, Y. Ohta and K. Abe
Article first published online:
01 Mar 2017 | DOI: 10.1111/ene.13268

Original Article

Background and purpose

Atypical Parkinsonian disorders (APD) frequently overlap in clinical presentations, making the differential diagnosis challenging in the early stages. The present study aimed to evaluate the accuracy of the [F]fluoro‐deoxy‐glucose positron emission tomography Statistical Parametric Mapping (SPM) optimized procedure in supporting the early and differential diagnosis of APD.

Methods

Seventy patients with possible APD were retrospectively included from a large clinical cohort. The included patients underwent [F]fluoro‐deoxy‐glucose positron emission tomography within 3 months of the first clinical assessment and a diagnostic follow‐up. An optimized SPM voxel‐wise procedure was used to produce t‐maps of brain hypometabolism in single subjects, which were classified by experts blinded to any clinical information. We compared the accuracy of both the first clinical diagnosis and the SPM t‐map classifications with the diagnosis at follow‐up as the reference standard.

Results

At first diagnosis 60% of patients were classified as possible APD (progressive supranuclear palsy, corticobasal degeneration, dementia with Lewy bodies, multiple system atrophy) and about 40% as APD with uncertain diagnosis, providing 52% sensitivity, 97% specificity and 86% accuracy with respect to the reference standard. SPM t‐map classification showed 98% sensitivity, 99% specificity and 99% accuracy, and a significant agreement with the diagnosis at follow‐up ( < 0.001).

Conclusions

The SPM t‐map classification at entry predicted the second diagnosis at follow‐up. This indicates its significantly superior role for an early identification of APD subtypes, particularly in cases of uncertain diagnosis. The use of a metabolic biomarker at entry in the instrumental work‐up of APD may shorten the diagnostic time, producing benefits for treatment options and support to the patients.

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Authors:
S. P. Caminiti, P. Alongi, L. Majno, M. A. Volontè, C. Cerami, L. Gianolli, G. Comi and D. Perani
Article first published online:
28 Feb 2017 | DOI: 10.1111/ene.13269

Original Article

Background and purpose

Although there is growing and convincing evidence that socially deprived patients are at higher risk of stroke and worse outcomes, it remains controversial whether or not they suffer more severe stroke. This study aimed to evaluate the influence of social deprivation on initial clinical severity in patients with stroke.

Methods

A total of 1536 consecutive patients with an acute first‐ever stroke (both ischaemic stroke and intracerebral hemorrhage) were prospectively enrolled from six French study centers. Stroke severity on admission was measured by the National Institutes of Health Stroke Scale score. Social deprivation was assessed at the individual level by the Evaluation de la Précarité et des Inégalités de santé dans les Centres d'Examen de Santé (EPICES) score, a validated multidimensional questionnaire, and several additional single socioeconomic indicators. Polytomous logistic regression analyses were performed to evaluate the association between social deprivation and stroke severity.

Results

In univariate analysis, the EPICES score ( = 0.039) and level of education ( = 0.018) were the only two socioeconomic variables associated with stroke severity. Multivariate analysis of the association between EPICES and National Institutes of Health Stroke Scale scores showed that more deprived patients presented a significantly higher risk of both mild and moderate/severe stroke (odds ratio for mild versus minor stroke, 1.39; 95% confidence interval, 1.06–1.84; odds ratio for moderate/severe versus minor stroke, 1.44; 95% confidence interval, 1.09–1.92). A non‐significant trend towards a higher risk of both mild and moderate/severe stroke in less educated patients was observed.

Conclusions

Social deprivation was associated with a more severe clinical presentation in patients with stroke. These findings may contribute to the worse outcome after stroke in deprived patients, and underline the need for strategies to reduce social inequalities for stroke.

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Authors:
Y. Béjot, A. Guilloteau, J. Joux, A. Lannuzel, E. Mimeau, C. Mislin‐Tritsch, I. Fournel and C. Bonithon‐Kopp
Article first published online:
25 Feb 2017 | DOI: 10.1111/ene.13271

Original Article

Background and purpose

Significant effects on clinical/neuroradiological disease activity have been reported in patients with relapsing–remitting multiple sclerosis treated with delayed‐release dimethyl fumarate (DMF) in phase III DEFINE/CONFIRM trials. We conducted a analysis of integrated data from DEFINE/CONFIRM to evaluate the effect of DMF on achieving no evidence of disease activity (NEDA) in patients with relapsing–remitting multiple sclerosis.

Methods

The analysis included patients randomized to DMF 240 mg twice daily, placebo or glatiramer acetate (CONFIRM only) for ≤2 years. A time‐to‐event method was used to estimate the percentage of patients achieving NEDA. Clinical NEDA (no relapses/no 12‐week confirmed disability progression) was analysed in the intention‐to‐treat (ITT) population. Neuroradiological (no new/newly enlarging T2 hyperintense lesions/no gadolinium‐enhancing lesions) and overall NEDA (clinical and neuroradiological NEDA) were analysed in the magnetic resonance imaging (MRI) cohort.

Results

The ITT and MRI populations comprised 1540 and 692 patients, respectively. The percentage of patients with clinical NEDA (ITT population) and neuroradiological NEDA (MRI cohort) was higher with DMF versus placebo over 2 years [clinical NEDA: 38.9% relative reduction; hazard ratio (HR), 0.61; 95% confidence interval (CI), 0.52‐0.72; < 0.0001; neuroradiological NEDA: 40.0% relative reduction; HR, 0.60; 95% CI, 0.49–0.73; < 0.0001]. The percentage of patients achieving overall NEDA (MRI cohort) was also higher with DMF (26%) versus placebo (12%) over 2 years, with a relative risk reduction of 42.7% (HR, 0.57; 95% CI, 0.48–0.69; < 0.0001).

Conclusions

A significantly higher percentage of patients treated with DMF achieved NEDA status over 2 years compared with placebo.

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Authors:
E. Havrdova, G. Giovannoni, R. Gold, R. J. Fox, L. Kappos, J. Theodore Phillips, M. Okwuokenye and J. L. Marantz
Article first published online:
22 Mar 2017 | DOI: 10.1111/ene.13272

Short Communication

Background and purpose

Portugal has been identified as one of the countries with a high prevalence of LRRK2‐G2019S, considered to be the most frequent known cause of familial and sporadic Parkinson's disease (PD). The aim of this study was to evaluate the prevalence of PD in Portugal using a door‐to‐door methodology.

Methods

A cross‐sectional study was conducted in the Portuguese community‐dwelling population; that is, elderly people living in the community on their own, aged ≥50 years and resident in mainland Portugal, in two phases: (i) a questionnaire was applied to screen potential cases of PD; and (ii) screened cases were evaluated by an expert in PD to confirm diagnosis.

Results

The adjusted prevalence of PD for the Portuguese community‐dwelling population aged ≥50 years was 0.24%. The estimated total number of cases of PD for the Portuguese population is 180/100 000 inhabitants.

Conclusions

The results of this study show that a geographical region with a high frequency of a causal mutation for PD does not automatically imply a high prevalence of patients with PD.

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Authors:
J. J. Ferreira, N. Gonçalves, A. Valadas, C. Januário, M. R. Silva, L. Nogueira, J. L. M. Vieira and A. B. Lima
Article first published online:
02 Mar 2017 | DOI: 10.1111/ene.13273

Original Article

Background and purpose

Improved biomarkers are needed to facilitate clinical decision‐making and as surrogate endpoints in clinical trials in multiple sclerosis (MS). We assessed whether neurodegenerative and neuroinflammatory markers in cerebrospinal fluid (CSF) at initial sampling could predict disease activity during 2 years of follow‐up in patients with clinically isolated syndrome (CIS) and relapsing–remitting MS.

Methods

Using multiplex bead array and enzyme‐linked immunosorbent assay, CXCL1, CXCL8, CXCL10, CXCL13, CCL20, CCL22, neurofilament light chain (NFL), neurofilament heavy chain, glial fibrillary acidic protein, chitinase‐3‐like‐1, matrix metalloproteinase‐9 and osteopontin were analysed in CSF from 41 patients with CIS or relapsing–remitting MS and 22 healthy controls. Disease activity (relapses, magnetic resonance imaging activity or disability worsening) in patients was recorded during 2 years of follow‐up in this prospective longitudinal cohort study.

Results

In a logistic regression analysis model, NFL in CSF at baseline emerged as the best predictive marker, correctly classifying 93% of patients who showed evidence of disease activity during 2 years of follow‐up and 67% of patients who did not, with an overall proportion of 85% (33 of 39 patients) correctly classified. Combining NFL with either neurofilament heavy chain or osteopontin resulted in 87% overall correctly classified patients, whereas combining NFL with a chemokine did not improve results.

Conclusions

This study demonstrates the potential prognostic value of NFL in baseline CSF in CIS and relapsing–remitting MS and supports its use as a predictive biomarker of disease activity.

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Authors:
I. Håkansson, A. Tisell, P. Cassel, K. Blennow, H. Zetterberg, P. Lundberg, C. Dahle, M. Vrethem and J. Ernerudh
Article first published online:
06 Mar 2017 | DOI: 10.1111/ene.13274

CME Article

Background and purpose

Up to 50% of ischaemic strokes in young adults are classified as cryptogenic despite extensive work‐up. We sought to evaluate the prevalence of non‐obstructive carotid atherosclerosis (NOCA) and its association with patent foramen ovale (PFO) in young adults with cryptogenic stroke (CS).

Methods

Patients aged 18–54 years, consecutively treated for first‐ever CS in an academic stroke service, were included. NOCA was assessed using carotid ultrasound examination and was defined as carotid plaque with <50% stenosis. PFO was diagnosed with transesophageal echocardiography.

Results

A total of 164 patients [mean age (SD) = 43.7 (8.5) years; 104 men] were included. A PFO was found in 79/164 (48.2%) patients. NOCA was demonstrated in 41/164 (25%) patients. NOCA was more common in patients without PFO [37.6% vs. 11.4%, < 0.001; adjusted odds ratio (95% confidence interval), 0.24 (0.10–0.56)]. Older age ( = 0.046) and subcortical location of cerebral infarct ( = 0.015) were also associated with the absence of PFO, whereas hypertension, diabetes and smoking were not.

Conclusions

This study demonstrates that NOCA is common in young adults with CS. NOCA is negatively associated with PFO. Detecting NOCA is an important component of stroke investigation in young adults.

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Authors:
A. Jaffre, B. Guidolin, J.‐B. Ruidavets, N. Nasr and V. Larrue
Article first published online:
15 Mar 2017 | DOI: 10.1111/ene.13275

Original Article

Background and purpose

Recent studies have suggested a possible excess risk of skin neoplasms in patients with myotonic dystrophy (DM). Risk factors related to this observation have not been defined.

Method

Information regarding personal history of skin tumors, pigmentation phenotype, and skin reaction to sun exposure were collected from 266 DM patients who were enrolled in the US National Institutes of Health National Registry of Myotonic Dystrophy and Facioscapulohumeral Muscular Dystrophy Patients and Family Members.

Results

Seventy‐seven subjects reported having skin tumors that were either benign ( = 31), malignant ( = 32) or both ( = 14). Female gender [odds ratio (OR) = 2.27, 95% confidence interval (CI) 1.02–5.05, = 0.04], older age (OR = 1.10, 95% CI 1.05–1.16, < 0.001) and DM1 subtype (OR = 3.42, 95% CI 1.27–9.26, = 0.02) were associated with a malignant skin tumor. The associations between malignant skin tumors and known risk factors [light eye color (OR = 1.62, 95% CI 0.78–3.39, = 0.20), light skin complexion (OR = 1.31, 95% CI 0.63–2.73, = 0.48) and moderate/extensive face freckles (OR = 1.47, 95% CI 0.50–4.34, = 0.49)] were modest. Strong, but not statistically significant, associations were noted with sunburn reactions when exposed to sunlight (OR = 4.28, 95% CI 0.91–19.95, = 0.06, and OR = 2.19, 95% CI 0.67–7.09, = 0.19, for sunburn with and without blistering, respectively).

Conclusions

Although our study was limited by small sample size, the risk factors for malignant skin tumors in DM strongly resemble the general population. It is recommended that DM patients adhere to sun exposure protective behavior.

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Authors:
S. M. Gadalla, J. E. Hilbert, W. B. Martens, S. Givens, R. T. Moxley and M. H. Greene
Article first published online:
20 Mar 2017 | DOI: 10.1111/ene.13276

Letter to the Editor

Response to Xia .

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Authors:
J. Hoogmoed
Article first published online:
17 Apr 2017 | DOI: 10.1111/ene.13277

Original Article

Background and purpose

The incidence, underlying physiopathology, features and association with lesion topography of visual hallucinations in acute stroke have scarcely been investigated.

Methods

Patients with a diagnosis of acute stroke (ischaemic or haemorrhagic) in any vascular territory, admitted within 24 h after the onset of symptoms, were consecutively included in the study. Patients with a previous history of psychosis or cognitive impairment were excluded. They and/or their caregivers answered a structured hallucination and sleep questionnaire at admission, within the first 15 days and at the clinical follow‐up 3–6 months after discharge. Lesion location (IMAIOS online atlas) and leukoaraiosis (Wahlund scale) were determined by magnetic resonance imaging or computed tomography scan. Subsets of patients also underwent a neuropsychological evaluation ( = 50) and an electroencephalogram ( = 33) before discharge.

Results

In all, 77 patients with a mean age of 71 ± 12 years were included of whom 57.1% were men. The incidence of visual hallucinations was 16.7%. These hallucinations were mostly complex, in black and white and self‐limited. The appearance of hallucinations was not influenced by age, sex, neuropsychological performance during admission or modified Rankin scale score at discharge. Visual hallucinations were associated with occipital cortex lesions ( = 0.04), and with sleep disturbances during and before admission ( = 0.041 and = 0.03 respectively).

Conclusions

Visual hallucinations are relatively frequent in patients with acute stroke and they are self‐limited. Patients with occipital lesions and sleep disturbances are more likely to suffer them.

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Authors:
E. Morenas‐Rodríguez, P. Camps‐Renom, A. Pérez‐Cordón, A. Horta‐Barba, M. Simón‐Talero, E. Cortés‐Vicente, D. Guisado‐Alonso, E. Vilaplana, C. García‐Sánchez, A. Gironell, C. Roig, R. Delgado‐Mederos and J. Martí‐Fàbregas
Article first published online:
22 Mar 2017 | DOI: 10.1111/ene.13278

Original Article

Background and purpose

Hereditary spastic paraplegia is a clinically and genetically heterogeneous group of rare, inherited disorders causing an upper motor neuron syndrome with (complex) or without (pure) additional neurological symptoms. Mutations in the gene have already been associated with recessive and dominant forms of hereditary spastic paraplegia (SPG30) in a few cases.

Methods

All family members included in the study were examined neurologically. Whole‐exome sequencing was used in affected individuals to identify the responsible candidate gene. Conventional Sanger sequencing was conducted to validate familial segregation.

Results

A family of Macedonian origin with two affected siblings, one with slowly progressive and the other one with a more complex and rapidly progressing hereditary spastic paraplegia is reported. In both affected individuals, two novel pathogenic mutations outside the motor domain of the gene were found (NM_001244008.1:c.2909G>A, p.Arg970His and c.1214dup, p.Asn405Lysfs*40) that segregate with the disease within the family establishing the diagnosis of autosomal recessive SPG30.

Conclusions

This report provides the first evidence that mutations outside the motor domain of the gene can cause (recessive) SPG30 and extends the genotype−phenotype association for ‐related diseases.

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Authors:
M. Krenn, G. Zulehner, C. Hotzy, J. Rath, E. Stogmann, M. Wagner, T. B. Haack, T. M. Strom, A. Zimprich and F. Zimprich
Article first published online:
22 Mar 2017 | DOI: 10.1111/ene.13279

Original Article

Background and purpose

Atrial fibrillation (AF) and significant carotid artery stenosis (CAS) often coexist in patients with acute stroke but whether CAS affects the stroke recurrence rate in anticoagulated AF patients is largely unknown. The effect of concomitant CAS on both short‐ and long‐term prognosis after stroke in patients with AF was evaluated.

Methods

The multicentre, retrospective FibStroke registry included AF patients with an ischaemic stroke or transient ischaemic attack (TIA) during 2003–2012. In this sub‐study, 165 AF patients with ischaemic stroke or TIA with significant (>50%) CAS (CAS group) and 734 AF patients without CAS (non‐CAS group) were identified. The median follow‐up time after an index event was 3.5 (interquartile range 3.9) years. Long‐term stroke recurrence rate, 30‐day mortality, CHADS‐VASc score, other risk factors and the use and intensity of anticoagulation were assessed.

Results

The recurrence rate of ischaemic stroke (21.2% vs. 12.7%, = 0.005, 8.1 vs. 3.6 events per100 follow‐up years) was significantly higher in CAS patients compared to the non‐CAS group despite similar anticoagulation/antithrombotic therapy. CAS patients had higher mean CHADS‐VASc scores than non‐CAS patients (4.3 vs. 3.3, < 0.001). However, in a multivariate analysis CAS was shown to be an independent risk factor for stroke recurrence (hazard ratio 2.02, 95% confidence interval 1.37–3.01, = 0.001). The 30‐day all‐cause mortality was significantly higher in CAS patients (7.9% vs. 1.9%, < 0.001) and CAS was an independent risk factor also for 30‐day mortality (odds ratio 3.34, 95% confidence interval 1.51–7.38, = 0.003).

Conclusions

In patients with AF, concomitant CAS was an independent risk factor for both long‐term stroke recurrence and 30‐day mortality.

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Authors:
H. Lehtola, K. E. J. Airaksinen, P. Hartikainen, J. E. K. Hartikainen, A. Palomäki, I. Nuotio, A. Ylitalo, T. Kiviniemi and P. Mustonen
Article first published online:
20 Mar 2017 | DOI: 10.1111/ene.13280

Editorial

Abstract

Click to view the accompanying paper in this issue.

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Authors:
R. Lanzillo
Article first published online:
22 Mar 2017 | DOI: 10.1111/ene.13283

Letter to the Editor

Sleep disorders require a comprehensive evaluation and confirmation with polysomnography in patients with multiple sclerosis

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Authors:
T. Ekiz and A. C. Pazarli
Article first published online:
17 Apr 2017 | DOI: 10.1111/ene.13284

Short Communication

Background and purpose

Performance on gambling tasks in Parkinson's disease (PD) is of particular interest, as pathological gambling is often associated with dopamine replacement therapy in these patients. We aimed to evaluate the effects of transcranial direct current stimulation (tDCS) over the right dorsolateral prefrontal cortex (DLPFC) in modulating gambling behaviour in PD.

Methods

We assessed the effects of cathodal tDCS over the right DLPFC during the Iowa Gambling Task in 20 patients with PD, compared with sham stimulation. We then conducted a second experimental design, assessing the effects of anodal tDCS over the right DLPFC.

Results

We observed that cathodal tDCS over the right DLPFC increased Iowa Gambling Task scores compared with sham stimulation. In the second experimental design, we did not find significant differences between anodal and sham tDCS.

Conclusions

Cathodal tDCS over the right DLPFC possibly reduces the pathological overdrive in frontostriatal networks in patients with PD on dopaminergic medication, thus modulating impulsive and risky decision‐making.

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Authors:
A. Benussi, A. Alberici, V. Cantoni, R. Manenti, M. Brambilla, V. Dell'Era, S. Gazzina, M. Manes, V. Cristillo, A. Padovani, M. Cotelli and B. Borroni
Article first published online:
15 Mar 2017 | DOI: 10.1111/ene.13286

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Article first published online:
17 Apr 2017 | DOI: 10.1111/ene.13305