Your search keyword '"Wenning, G"' showing total 17 results

1. Multiple System Atrophy

Author

Wenning, G. K. and Fanciulli, Alessandra

Subjects

Parkinson's Disease, a-synuclein, Multiple System atrophy

Published

2014

2. EFNS/MDS-ES recommendations for the diagnosis of Parkinson's disease

Author

Berardelli, Alfredo, Wenning, G. K., Antonini, A., Berg, D., Bloem, B. R., Bonifati, V., Brooks, D., Burn, D. J., Colosimo, Carlo, Fanciulli, Alessandra, Ferreira, J., Gasser, T., Grandas, F., Kanovsky, F., Kostic, V., Kulisewsky, J., Oertel, W., Poewe, W., Reese, J. P., Relja, M., Ruzicka, E., Shapira, A., Schrag, A., Seppi, K., Taba, P., Vidalhet, M., Clinical Genetics, and Schapira, Anthony

Subjects

Pathology, medicine.medical_specialty, Pediatrics, Parkinson's disease, Movement disorders, neurological disorders, parkinson's disease, movement disorders, 03 medical and health sciences, 0302 clinical medicine, Neuroimaging, Spect imaging, medicine, 030304 developmental biology, Genetic testing, 0303 health sciences, medicine.diagnostic_test, Essential tremor, business.industry, Parkinsonism, Diagnosis, medicine.disease, 3. Good health, Human Movement & Fatigue [DCN MP - Plasticity and memory NCEBP 10], Neurology, Neurology (clinical), Differential diagnosis, medicine.symptom, business, 030217 neurology & neurosurgery, Neurological disorders

Abstract

Item does not contain fulltext BACKGROUND: A Task Force was convened by the EFNS/MDS-ES Scientist Panel on Parkinson's disease (PD) and other movement disorders to systemically review relevant publications on the diagnosis of PD. METHODS: Following the EFNS instruction for the preparation of neurological diagnostic guidelines, recommendation levels have been generated for diagnostic criteria and investigations. RESULTS: For the clinical diagnosis, we recommend the use of the Queen Square Brain Bank criteria (Level B). Genetic testing for specific mutations is recommended on an individual basis (Level B), taking into account specific features (i.e. family history and age of onset). We recommend olfactory testing to differentiate PD from other parkinsonian disorders including recessive forms (Level A). Screening for pre-motor PD with olfactory testing requires additional tests due to limited specificity. Drug challenge tests are not recommended for the diagnosis in de novo parkinsonian patients. There is an insufficient evidence to support their role in the differential diagnosis between PD and other parkinsonian syndromes. We recommend an assessment of cognition and a screening for REM sleep behaviour disorder, psychotic manifestations and severe depression in the initial evaluation of suspected PD cases (Level A). Transcranial sonography is recommended for the differentiation of PD from atypical and secondary parkinsonian disorders (Level A), for the early diagnosis of PD and in the detection of subjects at risk for PD (Level A), although the technique is so far not universally used and requires some expertise. Because specificity of TCS for the development of PD is limited, TCS should be used in conjunction with other screening tests. Conventional magnetic resonance imaging and diffusion-weighted imaging at 1.5 T are recommended as neuroimaging tools that can support a diagnosis of multiple system atrophy (MSA) or progressive supranuclear palsy versus PD on the basis of regional atrophy and signal change as well as diffusivity patterns (Level A). DaTscan SPECT is registered in Europe and the United States for the differential diagnosis between degenerative parkinsonisms and essential tremor (Level A). More specifically, DaTscan is indicated in the presence of significant diagnostic uncertainty such as parkinsonism associated with neuroleptic exposure and atypical tremor manifestations such as isolated unilateral postural tremor. Studies of [(123) I]MIBG/SPECT cardiac uptake may be used to identify patients with PD versus controls and MSA patients (Level A). All other SPECT imaging studies do not fulfil registration standards and cannot be recommended for routine clinical use. At the moment, no conclusion can be drawn as to diagnostic efficacy of autonomic function tests, neurophysiological tests and positron emission tomography imaging in PD. CONCLUSIONS: The diagnosis of PD is still largely based on the correct identification of its clinical features. Selected investigations (genetic, olfactory, and neuroimaging studies) have an ancillary role in confirming the diagnosis, and some of them could be possibly used in the near future to identify subjects in a pre-symptomatic phase of the disease. 19 p.

Published

2013

3. Orthostatic hypotension and attention in Parkinson’s disease with and without dementia.

Author

Peralta, C., Stampfer-Kountchev, M., Karner, E., Köllensperger, M., Geser, F., Wolf, E., Seppi, K., Benke, T., Poewe, W., and Wenning, G. K.

Subjects

ORTHOSTATIC hypotension, PARKINSON'S disease, DEMENTIA, BLOOD pressure, NEUROPSYCHOLOGICAL tests, ATTENTION

Abstract

To compare frequency and degree of orthostatic hypotension (OH) in Parkinson’s disease (PD) and Parkinson’s disease with dementia (PDD) and its effect on attention and word fluency, blood pressure (BP) and heart rate changes during tilt were determined in 10 PD and 8 PDD patients. Attention and word fluency were evaluated in supine and tilted position using standard neuropsychological tests. OH defined as systolic BP (SBP) drop of ≥20 mmHg and/or diastolic BP (DBP) drop of ≥10 mmHg was present in 5 PDD patients and in 2 PD patients. SBP drop was significantly greater in PDD than in PD patients ( P < 0.05). Whereas word fluency was unaffected by tilt in both patient groups, attention as assessed with the Test of Everyday Attention (TEA) deteriorated significantly in the PDD group, correlating with blood pressure response (ΔSBP and TEA-2, r = 0.828, P < 0.05; ΔDBP and TEA-2, r = 0.828, P < 0.05). We conclude that OH is frequent in PDD and should be addressed therapeutically since it may exacerbate attentional dysfunction. [ABSTRACT FROM AUTHOR]

Published

2007

4. How to diagnose MSA early: the role of magnetic resonance imaging.

Author

Seppi, K., Schocke, M. F. H., Wenning, G. K., and Poewe, W.

Subjects

RESEARCH, MAGNETIC resonance imaging, PROTON magnetic resonance spectroscopy, DIAGNOSTIC imaging, PARKINSON'S disease, PARKINSON'S disease diagnosis, DIGITAL diagnostic imaging

Abstract

The clinical differentiation between Parkinson’s disease (PD) and multiple system atrophy (MSA) remains a challenge for each neurologist. The use of different magnetic resonance imaging (MRI) techniques including conventional MRI, proton magnetic resonance spectroscopy (MRS), diffusion-weighted imaging (DWI), magnetization transfer imaging (MTI) and MR volumetry (MRV) offer the potential for objective criteria in the differential diagnosis of neurodegenerative parkinsonism. The aim of this article is to review the role of different MRI techniques in the differential diagnosis of PD and MSA. [ABSTRACT FROM AUTHOR]

Published

2005

5. Management of multiple system atrophy: state of the art.

Author

Colosimo, C., Tiple, D., and Wenning, G. K.

Subjects

RESEARCH, NEURODEGENERATION, ETIOLOGY of diseases, PATIENTS, PARKINSON'S disease, ORTHOSTATIC hypotension, AUTONOMIC nervous system diseases, DOPA

Abstract

Multiple system atrophy (MSA) is a sporadic neurodegenerative disease of undetermined aetiology presenting with parkinsonian, autonomic, cerebellar, and pyramidal signs. Despite the lack of any effective therapy to reverse MSA, some of the symptoms may be improved with adequate symptomatic therapies. Medical treatment is largely aimed at mitigating the parkinsonian and autonomic features. The therapeutic results of levodopa therapy in cases of MSA are difficult to interpret because of their variability. Nevertheless, the simple statement that patients with MSA do not respond to levodopa is false. Clinical and pathologically proven series document levodopa efficacy in about 40-60% of patients with MSA and predominant parkinsonian features. Other antiparkinsonian compounds (dopamine agonists, amantadine) may also be employed, but they are not more effective than levodopa. Orthostatic hypotension (OH) can be suspected from the patient s history and subsequently documented in the clinic by measuring lying and standing blood pressure. The diagnosis ideally should be confirmed with additional laboratory tests to determine the cause and evaluate the functional deficit, so as to aid treatment. A number of pharmacological agents with different mechanisms of action have been used in MSA to reduce OH when this is symptomatic. OH can also be alleviated by avoiding aggravating factors, such as the effects of food, micturition, exposure to a warm environment, and physiological diurnal changes, and by using other non-pharmacological strategies. The treatment of the very common genitourinary symptoms (incontinence, retention, impotence) should also be considered in order to improve the quality of life of these patients. [ABSTRACT FROM AUTHOR]

Published

2005

6. Parkinsonism following striatal infarcts: incidence in a prospective stroke unit cohort.

Author

Peralta, C., Werner, P., Holl, B., Kiechl, S., Willeit, J., Seppi, K., Wenning, G., and Poewe, W.

Subjects

PARKINSON'S disease, BRAIN diseases, BASAL ganglia, CEREBROVASCULAR disease, BLOOD circulation disorders, BRAIN blood-vessels

Abstract

A number of case reports have highlighted the occurrence of parkinsonism following strategic infarcts affecting the basal ganglia but the prevalence of parkinsonism after striatal infarcts (SI) has not been assessed. Therefore, we evaluated the clinical features and prevalence of parkinsonism in a large series of patients admitted to the Stroke-Unit of the Department of Neurology Innsbruck. Cerebral scans were retrospectively screened for SI, defined as a lesion larger than 1.5?cm involving the basal ganglia and the internal capsule. Out of 622 patients, 27 met the criteria for SI (4.3%) and 11 patients were available for follow-up. All patients presented contralateral motor weakness. Bilateral akinetic-rigid parkinsonism was found in only one patient whose [123I]ß-CIT-SPECT showed a decrease of the ligand uptake following the limits of the vascular lesion. Overall, parkinsonism does not appear to be a frequent consequence of striatal infarcts. Multiple lacunar subcortical infarcts interrupting thalamocortical drive may be more critical for the development of vascular parkinsonism. [ABSTRACT FROM AUTHOR]

Published

2004

7. Impact of coexistent Alzheimer pathology on the natural history of Parkinson's disease.

Author

Jellinger, K. A., Seppi, K., Wenning, G. K., and Poewe, W.

Subjects

PARKINSON'S disease, DEMENTIA, ALZHEIMER'S disease, BRAIN diseases, PATHOLOGY, NATURAL history

Abstract

Summary.Objective: To assess the impact of coexisting Alzheimer (AD) pathology on the natural history of Parkinson's disease (PD). Background: AD changes are frequently present in brains of demented PD patients. Assessing the relative contribution of AD pathology to the natural history of PD is difficult and the impact of both AD and cortical Lewy body (LB) pathologies on cognitive dysfunction is still under discussion. From clinical experience, dementia in PD patients, mainly related to AD pathology, is associated with a poor outcome, but the impact of AD pathology on the natural history of PD has not been studied systematically. Material and methods: In 200 consecutive autopsy cases of PD (sex (m/f) ratio 1 : 1.1), age at death 58–98 (mean 77.0 ± 9.5) years, from a specialized Austrian brain bank, retrospectively assessed major initial clinical symptoms (tremor, akinesia), moderate/severe dementia, and duration of illness were correlated with associated AD pathologies using CERAD, Braak and NIA-Reagan criteria. Mann-Whitney U-test, Cox-regression were used for statistical analysis. Results: While gender had no influence on the clinical motor symptoms and outcome, tremor dominant type had a significantly better outcome than akinetic forms (p = 0.022), even after adjustment with age at onset and associated AD pathology (CERAD and Braak criteria). Patients with late onset showed significantly shorter duration of illness irrespective of dementia. Moderate to severe dementia, reported in 33% of the sample, was significantly correlated with AD pathology (all 3 criteria) that showed significantly negative correlation with survival: between CERAD 0-A vs. B and C there was a significant difference of odd ratios (p < 0.001), as was between Braak stages 0–2, 3–4.5, and 5, but not between Braak stages 3–4 and 5. Conclusions: The present data confirm previous studies suggesting better outcome of tremor-dominant than akinetic-rigid type of PD, significantly worse outcome in PD with late onset and dementia that is significantly correlated with coexistent neuritic Alzheimer pathology, particularly when using the CERAD and NIA-R criteria for the diagnosis of AD. Further studies are needed to elucidate the relative impact of cortical LB and AD pathologies on the natural history of PD. [ABSTRACT FROM AUTHOR]

Published

2002

8. A novel grading scale for striatonigral degeneration (multiple system atrophy).

Author

Wenning, G. K., Seppi, K., Tison, F., and Jellinger, K.

Subjects

OLIVOPONTOCEREBELLAR atrophies, CEREBELLUM degeneration, PARKINSON'S disease, BRAIN diseases, NEUROLOGICAL disorders, DOPAMINE, NEUROTRANSMITTERS

Abstract

Summary. Striatonigral degeneration (SND) is commonly thought to represent the neuropathological substrate of L-Dopa unresponsive parkinsonism in patients with multiple system atrophy (MSA). Other neuropathological hallmarks of MSA include olivopontocerebellar atrophy (OPCA) and preganglionic sympathetic spinal cord lesions. Clinicopathological evaluation of MSA patients recruited into ongoing natural history studies or neuroprotective intervention trials will require standardized grading of MSA pathology. Based on 25 autopsy cases of MSA, we propose a novel SND grading scale which allows semiquantitative assessment of lesion severity based on neuronal loss, astrogliosis and presence of α-synuclein positive glial cytoplasmic inclusions (GCIs) in substantia nigra, putamen, caudate nucleus, and globus pallidus. SND grade I is defined as degeneration of the substantia nigra pars compacta (SNC) with relative preservation of the striatum except for minimal gliosis and GCIs in the posterior putamen ("minimal change MSA"). SND grade II is characterized by neuronal loss, astrogliosis and presence of GCIs in SNC and posterior/dorsolateral putamen. Caudate nucleus and external globus pallidus may exhibit slight gliosis. Striatal pathology is severe and extends to anterior ventromedial subregions in SND grade III. There is neuronal loss in caudate nucleus and globus pallidus. GCIs are more abundant in grade II than grade III SNC and putamen. Preliminary clinicopathologic correlation studies suggest milder parkinsonian disability and better initial L-Dopa responsiveness in SND grade I and II cases compared to grade III cases. Prospective clinicopathologic studies are required to validate the proposed SND grading scale and may result in further subdivisions, particularly of SND grade III. [ABSTRACT FROM AUTHOR]

Published

2002

9. Botulinum toxin treatment in atypical parkinsonian disorders associated with disabling focal dystonia.

Author

Müller, J., Wenning, G. K., Wissel, J., Seppi, K., and Poewe, W.

Subjects

BOTULINUM toxin, NEUROTOXIC agents, CLOSTRIDIUM botulinum, BACTERIAL toxins, PARKINSON'S disease, EXTRAPYRAMIDAL disorders, BRAIN diseases

Abstract

We investigated the efficacy of botulinum toxin A (BtxA) therapy in patients with atypical parkinsonian disorders (APD) exhibiting different types of disabling focal dystonia unresponsive to oral drug therapy. Eight patients with functionally disabling focal dystonia out of a series of 60 consecutive patients with APDs regularly treated at our outpatient movement disorders clinic were included. Patients were diagnosed according to established criteria and had disabling limb dystonia (n=4) or craniocervical dystonia (n=4) unresponsive to oral pharmacological treatment. Localization and dose of BtxA injections was determined individually based on clinical examination as well as EMG in patients with limb dystonia. BtxA reduced dystonic symptoms in all patients; only one developed a transient local side-effect. BtxA was particularly effective in the long-term treatment (up to 50 months) of blepharospasm associated with progressive supranuclear palsy (PSP). BtxA also alleviated PSP-associated retrocollis and orofacial dystonia with lower lip retraction associated with PSP and multiple system atrophy. BtxA treatment of limb dystonia in corticobasal degeneration (CBD) temporarily improved hand and arm function in early disease stages while treatment in advanced stages reduced pain, facilitated hygiene and prevented secondary contractures. Limb dystonia was also alleviated by BtxA therapy in one patient with neuronal multisystem degeneration of undetermined cause. The results suggest that BtxA therapy may represent an effective means of alleviating disabling focal dystonia in different APDs. Particularly in early stage APD with disabling limb dystonia local BtxA injections may result in functional improvement. [ABSTRACT FROM AUTHOR]

Published

2002

10. What clinical features are most useful to distinguish definite multiple system atrophy from Parkinson's disease?

Author

Wenning, G. K., Ben-Shlomo, Y., Hughes, A., Daniel, S. E., Lees, A., and Quinn, N. P.

Published

2000

11. Natural history and survival of 14 patients with corticobasal degeneration confirmed at postmortem examination.

Author

Wenning, G. K., Litvan, I., Jankovic, J., Granata, R., Mangone, C. A., McKee, A., Poewe, W., Jellinger, K., Chaudhuri, K. Ray, D'Olhaberriague, L., Pearce, R. K. B., Ray Chaudhuri, K, and Pearce, R K

Subjects

COGNITION disorders diagnosis, AUTOPSY, BASAL ganglia, CEREBRAL cortex, COGNITION disorders, COMPARATIVE studies, NEUROPSYCHOLOGICAL tests, RESEARCH methodology, MEDICAL cooperation, PARKINSON'S disease, RESEARCH, SURVIVAL, EVALUATION research, RETROSPECTIVE studies, SEVERITY of illness index, DISEASE complications

Abstract

Objective: To analyse the natural history and survival of corticobasal degeneration by investigating the clinical features of 14 cases confirmed by postmortem examination.Methods: Patients with definite corticobasal degeneration were selected from the research and clinical files of seven tertiary medical centres in Austria, the United Kingdom, and the United States. Clinical features were analysed in detail.Results: The sample consisted of eight female and six male patients; mean age at symptom onset was 63 (SD 7.7) years, and mean disease duration was 7.9 (SD 2.6) years. The most commonly reported symptom at onset included asymmetric limb clumsiness with or without rigidity (50%) or tremor (21%). At the first neurological visit, on average 3.0 (SD 1.9) years after symptom onset, the most often encountered extrapyramidal features included unilateral limb rigidity (79%) or bradykinesia (71%), postural imbalance (45%), and unilateral limb dystonia (43%). Ideomotor apraxia (64%), and to a lesser extent cortical dementia (36%), were the most common cortical signs present at the first visit. During the course of the disease, virtually all patients developed asymmetric or unilateral akinetic rigid parkinsonism and a gait disorder. No patient had a dramatic response to levodopa therapy. Median survival time after onset of symptoms was 7.9 (SD 0.7) (range, 2.5-12.5) years, and, after the first clinic visit, 4.9 (SD 0.7) (range, 0.8-10) years. Early bilateral bradykinesia, frontal syndrome, or two out of tremor, rigidity, and bradykinesia, predicted a shorter survival.Conclusion: The results confirm that unilateral parkinsonism unresponsive to levodopa and limb ideomotor apraxia are the clinical hallmarks of corticobasal degeneration, and only a minority of patients with corticobasal degeneration present with dementia. The study also suggests that a focal cognitive and extrapyramidal motor syndrome is indicative of corticobasal degeneration. Survival in corticobasal degeneration was shortened by the early presence of (more) widespread parkinsonian features or frontal lobe syndrome. [ABSTRACT FROM AUTHOR]

Published

1998

12. Clinicopathological study of 35 cases of multiple system atrophy.

Author

Wenning, G K, Ben-Shlomo, Y, Magalhães, M, Daniel, S E, and Quinn, N P

Subjects

AGE factors in disease, BRAIN, COMPARATIVE studies, RESEARCH methodology, MEDICAL cooperation, NEURODEGENERATION, PARKINSON'S disease, RESEARCH, RESEARCH funding, EVALUATION research

Abstract

The clinical and pathological features of 35 cases with multiple system atrophy collected in the United Kingdom Parkinson's Disease Society Brain Bank (UKPDSBB) between 1985 and 1992 have been analysed. The median age of onset was 55 (range 33.3-75.8) years and median survival was 7.3 (range 2.1-11.5) years. Parkinsonism, usually asymmetric, occurred in all, and autonomic failure in all but one case. Cerebellar signs were noted in 34% and pyramidal features in 54% of the cases. Glial cytoplasmic inclusions were found in all cases with adequate fixation. Lewy bodies were detected in three cases. The substantia nigra was (usually severely) depleted of cells in all cases. With two exceptions the putamen was atrophic; the caudate and pallidum were less commonly and less severely affected. Overall nigrostriatal cell loss correlated with severity of disease at the time of death. The latest, but not the best, recorded levodopa response tended to be inversely related to the degree of putaminal degeneration. The olivopontocerebellar system was involved in 88% of the cases, the cerebellar vermis usually being more severely affected than the hemispheres. The presence of associated cerebellar pathology was, however, unrelated to the presence of cerebellar signs in life. [ABSTRACT FROM AUTHOR]

Published

1995

13. Placebo-controlled trial of riluzole in multiple system atrophy.

Author

Seppi, K., Peralta, C., Diem-Zangerl, A., Puschban, Z., Mueller, J., Poewe, W., and Wenning, G. K.

Subjects

DISEASES, PLACEBOS, PARKINSON'S disease, DRUGS, CLINICAL trials

Abstract

We performed a placebo-controlled cross-over trial of riluzole (100 mg b.i.d.) in 10 patients with probable multiple system atrophy (MSA) administering riluzole and placebo for 4 weeks each with a 4-week washout period. Outcome measures evaluated short-term anti-Parkinsonian effects using the Unified Parkinson's Disease Rating Scale (UPDRS) subscales (UPDRS-II, activities of daily living; UPDRS-III, motor examination; sum of UPDRS-II and -III) before and at the end of each treatment phase. Delta values were calculated by subtracting the UPDRS scores measured at the end of each treatment arm from those before onset of each medication phase. Riluzole was generally well tolerated. There were no significant anti-Parkinsonian effects of riluzole comparing the UPDRS delta values for both treatment arms using the Wilcoxon signed-rank test. It is unlikely that riluzole treatment could have clinically meaningful anti-Parkinsonian effects in MSA. A trial assessing the disease-modifying potential of riluzole in MSA is underway. [ABSTRACT FROM AUTHOR]

Published

2006

14. Dysautonomia in Movement Disorders

Author

Wenning, G. K. and Fanciulli, Alessandra

Subjects

Orthostatic hypotension, parkinson's disease, multiple system atrophy

15. No association of GBA mutations and multiple system atrophy.

Author

Srulijes, K., Hauser, A. ‐K., Guella, I., Asselta, R., Brockmann, K., Schulte, C., Soldà, G., Cilia, R., Maetzler, W., Schols, L., Wenning, G. K., Poewe, W., Barone, P., Wüllner, U., Oertel, W., Berg, D., Goldwurm, S., and Gasser, T.

Subjects

GENETIC mutation, ATROPHY

Abstract

A letter to the editor is presented in response to the article "No association of GBA mutations and multiple system atrophy" is presented.

Published

2013

16. Incidental Lewy body disease.

Author

Ben-Shlomo, Y and Wenning, G

Subjects

*DISEASE susceptibility, *ECOLOGY, *PARKINSON'S disease

Published

1994

17. Multiple system atrophy: sporadic or familial?

Author

Wenning, G K, Wagner, S, Daniel, S, and Quinn, N P

Subjects

*CENTRAL nervous system diseases, *COMPARATIVE studies, *RESEARCH methodology, *MEDICAL cooperation, *NEURODEGENERATION, *PARKINSON'S disease, *RESEARCH, *EVALUATION research

Published

1993