R. Galvin scite author profile

Background: Although Wernicke encephalopathy (WE) is a preventable and treatable disease it still often remains undiagnosed during life. Objectives: To create practical guidelines for diagnosis, management and prevention of the disease. Methods: We searched MEDLINE, EMBASE, LILACS, Cochrane Library. Conclusions and recommendations: The clinical diagnosis of WE should take into account the different presentations of clinical signs between alcoholics and non alcoholics (Recommendation Level C); although prevalence is higher in alcoholics, WE should be suspected in all clinical conditions which could lead to thiamine deficiency (good practice point – GPP). The clinical diagnosis of WE in alcoholics requires two of the following four signs; (i) dietary deficiencies (ii) eye signs, (iii) cerebellar dysfunction, and (iv) either an altered mental state or mild memory impairment (Level B). Total thiamine in blood sample should be measured immediately before its administration (GPP). MRI should be used to support the diagnosis of acute WE both in alcoholics and non alcoholics (Level B). Thiamine is indicated for the treatment of suspected or manifest WE. It should be given, before any carbohydrate, 200 mg thrice daily, preferably intravenously (Level C). The overall safety of thiamine is very good (Level B). After bariatric surgery we recommend follow‐up of thiamine status for at least 6 months (Level B) and parenteral thiamine supplementation (GPP). Parenteral thiamine should be given to all at‐risk subjects admitted to the Emergency Room (GPP). Patients dying from symptoms suggesting WE should have an autopsy (GPP).

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EFNS guideline on the diagnosis and management of alcohol‐related seizures: report of an EFNS task force

Bråthen

Ben‐Menachem

Brodtkorb

et al. 2005

Euro J of Neurology

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Despite being a considerable problem in neurological practice and responsible for onethird of seizure-related admissions, there is little consensus as to the optimal investigation and management of alcohol-related seizures. The final literature search was undertaken in September 2004. Consensus recommendations are given graded according to the EFNS guidance regulations. To support the history taking, use of a structured questionnaire is recommended. When the drinking history is inconclusive, elevated values of carbohydrate-deficient transferrin and/or gammaglutamyl transferase can support a clinical suspicion. A first epileptic seizure should prompt neuroimaging (CT or MRI). Before starting any carbohydrate containing fluids or food, patients presenting with suspected alcohol overuse should be given prophylactic thiamine parenterally. After an alcohol withdrawal seizure (AWS), the patient should be observed in hospital for at least 24 h and the severity of withdrawal symptoms needs to be followed. For patients with no history of withdrawal seizures and mild to moderate withdrawal symptoms, routine seizure preventive treatment is not necessary. Generally, benzodiazepines are efficacious and safe for primary and secondary seizure prevention; diazepam or, if available, lorazepam, is recommended. The efficacy of other drugs is insufficiently documented. Concerning long-term recommendations for non-alcohol dependant patients with partial epilepsy and controlled seizures, small amounts of alcohol may be safe. Alcohol-related seizures require particular attention both in the diagnostic work-up and treatment. Benzodiazepines should be chosen for the treatment and prevention of recurrent AWS.

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One Europe, one neurologist?

Grisold

Galvin

Lisnic³

et al. 2007

Euro J of Neurology

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In recent years, there has been a major shift in emphasis within neurology from being a largely diagnostic discipline to one much more actively involved in treating disease. There have been major scientific advances leading to new and effective treatments. There is also a much greater awareness of the burden of neurological disease (Olesen J, Leonardi M. European Journal of Neurology 2003; 10: 471) and informed sufferers are requesting specific intervention. There is wide variation in the delivery of neurological services throughout Europe. This is reflected in manpower levels, the place of neurology related to other medical specialties and different mixes of hospital and private office practice. These differences have been thrown into sharper focus by the recent expansion of the European Union (EU). Initial training in neurology is given to undergraduate/pre-graduate students. Post-graduate education is delivered within a residency program leading to specialist qualification and certification. We now recognize that this is only the beginning of a life long program of continuous education and development (CME/CPD). National and international exchange programs facilitate the growth of knowledge and promote professional harmony and cooperation. The free migration of medical specialists has been an aspiration but remains limited by cultural, linguistic, personal, professional, political and economic factors. Two bodies, the European Board of Neurology (EBN-UEMS) http://www.uemsneuroboard.org (Union Europe´enne des Me´decins Spe´cialistes) and the European Federation of Neurological Societies (EFNS) http://www.efns.org are actively involved in harmonising and developing neurology at the European level.

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Diagnosis, Therapy and Prevention of Wernicke's Encephalopathy

Galvin

Bråthen

Ivashynka³

et al. 2011

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Non-traumatic brachial plexopathies, clinical, radiological and neurophysiological findings from a tertiary centre

Mullins¹,

O'Sullivan²,

Neligan³

et al. 2007

Clinical Neurology and Neurosurgery

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R. Galvin

EFNS guidelines for diagnosis, therapy and prevention of Wernicke encephalopathy

EFNS guideline on the diagnosis and management of alcohol‐related seizures: report of an EFNS task force

One Europe, one neurologist?

Diagnosis, Therapy and Prevention of Wernicke's Encephalopathy

Non-traumatic brachial plexopathies, clinical, radiological and neurophysiological findings from a tertiary centre

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