Clinical Guideline. Change History Date Change details, since approval Approved by
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1 Clinical Guideline 1. The detection of alcohol misusers attending hospital 2. The management of alcohol withdrawal syndrome (AWS) 3. The management of Wernicke s Encephalopathy (WE) Document Detail Document Type Guidelines 1. The detection of alcohol misusers attending hospital; Document name 2. The management of alcohol withdrawal syndrome; 3. The management of Wernicke s Encephalopathy. Document location GTi Clinical Guidance Database Version 2.0 Effective from 15 June 2010 Review date 15 June 2012 Owner General Medicine Author Carl Holvey Senior Psychiatric Liaison Pharmacist Nicola Torrens Senior Admissions Pharmacist Approved by, date Drug & Therapeutics Committee, May 2010 Superseded documents Related documents Keywords Alcohol withdrawal, Wernicke s, Encephalopathy, AWS, alcohol misusers, chlordiazepoxide, Relevant external law, regulation, standards Change History Date Change details, since approval Approved by DTC Reference 10052a Review by June 2012
2 CONTENTS Chapter 1 Summary and Algorithms 1.1 Management Algorithm for the alcohol withdrawal syndrome 1.2 Management in unusual circumstances Page The Alcohol Withdrawal Syndrome (AWS) 2.1 Symptoms of alcohol withdrawal 2.2 Risk factors for progression to severe withdrawal 2.3 Detection of alcohol misuse Alcohol use disorders identification test (AUDIT) The CAGE questionnaire 2.4 Medical management of alcohol withdrawal The first 24 hours Days Difficult to control Patients Management of Alcohol Withdrawal related seizures Patients who are difficult to assess using CIWA-Ar Elderly Patients Pregnant Patients Wernicke s encephalopathy (WE) 3.1 Treatment 3.2 Prophylaxis 3.3 Oral B-vitamin absorption in alcohol misusers Appendix 4.1 Trust Referral Services & Community Services 4.2 Alcohol use disorders identification test (AUDIT) tool 4.3 Clinical Institute Withdrawal Assessment of Alcohol Scale, Revised (CIWA-Ar) 4.4 Alcohol withdrawal nursing observation chart 4.5 Patient information References and Authors 17 DTC Reference 10052a Page 1 of 17 Review by June2012
3 Management algorithm for the alcohol withdrawal syndrome All patients admitted to hospital should be asked about their alcohol intake. Symptoms and Signs (Non-specific and absence does not exclude withdrawal) Anxiety/Agitation/Irritability Nausea/Vomiting/Diarrhoea Convulsions Tremor of hands, tongue, eyelids Insomnia Hallucinations Sweating Fever with or without infection Delirium Tachycardia Hypertension Prescribe chlordiazepoxide 25 to 50mg every 2 hours as required on the PRN side & Pabrinex One/Two pairs TDS (See right) Nursing observations and administration of chlordiazepoxide is every 2 hours for 24hours starting at the first signs of withdrawal. Dose is dependent on CIWA-Ar score. If CIWA-Ar scale 0 to 9 or patient asleep no treatment necessary If CIWA-Ar score 10 to 14 give 25mg If CIWA-Ar score 15 or above give 50mg After initial 24-hour assessment period "PRN" should be discontinued and a standard 5-day reducing regimen should be prescribed based on the baseline dose of chlordiazepoxide Vitamin Supplementation Parental Pabrinex is prescribed to treat or avoid Wernike s Encepalopathy (WE) Indication Regimen Length of course Known/suspected chronic alcohol misuser One pair of Pabrinex IVHP ampoules IV TDS At least one day Any Patient displaying symptoms of WE* TWO pairs of Pabrinex IVHP ampoules IV TDS 3-7 day *Ataxia, hypothermia and hypotension, confusion, ophthalmoplegia or nystagmus, memory disturbances, coma or unconsciousness. The classic triad only occurs in 10% of patients. Administration of Pabrinex IVHP: Each pair of ampoules to be diluted in 50ml to 100ml 0.9% sodium chloride or 5% w/v glucose. Infuse over 30 minutes. Small risk of anaphylaxis. Facilities to manage anaphylaxis must be available. Oral vitamin supplementation & discharge Thiamine 100mg TDS and Vitamin B Co Strong 2 OD should be continued for 2 weeks (up to 6 weeks) Chlordiazepoxide should NOT be prescribed on discharge. Day 1 total PRN Day 2 (mg) Day 3 (mg) Day 4 (mg) Day 5* (mg ) dose 8am 12pm 6pm 10pm 8am 12pm 6pm 10pm 8am 12pm 6pm 10pm 8am 12pm 6pm 10pm 300mg mg mg mg mg mg mg mg mg mg mg mg *A longer detox may be required if at Day 5 the patient is on a total daily chlordiazepoxide dose of 40mg or larger. Further information -In liver impairment, a shorter acting benzodiazepine may be indicated (1mg lorazepam=25mg chlordiazepoxide) -oral benzodiazepines should be given on presentation of seizures. -A fixed dose chlordiazepoxide withdrawal regimen should be prescribed in patients where it s difficult to rate their alcohol withdrawal. See full guideline for: -Difficult to control patients -Delirious patients -Psychotic patients -Alcohol-induced seizures DTC Reference 10052a Page 2 of 17 Review by June2012
4 1.2 Management in Unusual Circumstances Options that may be considered in difficult to control patients Discuss with the medical team and sometimes it may be necessary to consult with Psychiatric Liaison Services. Only give >300mg of chlordiazepoxide per day after medical review. Switching to IV diazepam IV diazepam emulsion may be administered as a bolus by peripheral or central route. Administer the undiluted emulsion at a rate of 1ml per minute (5mg per minute). A dose of 10mg every minutes may be given until symptoms subside or the patient is markedly sedated. Usual maximum dose is 30mg in 24 hours. Monitor for symptoms of withdrawal and sedation. For patients with liver failure, IV lorazepam 1mg to 2mg every 5 minutes should be used until the patient is awake but calm. In elderly patients consider using half the recommended adult dose. Monitor ECG, blood pressure, pulse oximetry, respiratory rate and temperature when giving high dose benzodiazepines. Consider extending the PRN dosing beyond 24 hours in patients with delirium tremens. Consider using a longer withdrawal regimen if unable to stabilise after 24 hours Consider an antipsychotic Usually haloperidol (consider lower doses in the elderly) PO/IM 5mg tds (Maximum 15mg IM or 30mg PO in 24 hours) Refer the patient to the appropriate psychiatric team who may consider the addition of an antipsychotic to control agitation. Poor English, Confused, Delirious or Psychotic Patients For these patients the CIWA-Ar scale is inappropriate as the patient will not be able to score on anxiety, orientation and clouding of sensorium, tactile, auditory and visual disturbances. It may be more appropriate to assess physical symptoms objectively and use a FIXED reduction regime immediately. Start at Day 2 of the 5 day withdrawal scale If using a FIXED reducing regime, it may be necessary to use prn Chlordiazepoxide on top of the fixed regime in the first 24 hours to prevent breakthrough withdrawal symptoms. If the prn doses are utilised a review of the fixed regimen doses are needed after 24 hours. The doses will need to be increased to take into account the prn utilisation. Elderly patients To minimise adverse effects associated with benzodiazepines (e.g. over sedation, confusion and ataxia) in the elderly it is important to bear in mind the start low and go-slow rule. In general it is recommended that half the dose of the benzodiazepine is used. Patients with liver failure The metabolism of chlordiazepoxide is impaired in liver disease. But it may be used cautiously in mild to moderate impairment (reduce the dose by 50%). For patients with severe or acute liver impairment, lorazepam may be used as an alternative as its metabolism is not impaired in liver disease. Pregnant patients As in any patient who may be pregnant or is pregnant, each case is dealt with on an individual basis. It is important to bear in mind the risk of seizure against the risk of foetal exposure to chlordiazepoxide. It is essential the obstetric team is informed if the patient presents during late pregnancy or in labour. The Psychiatric Liaison services can be contacted for advice; please see page 17 for contact details. Long term regular use of chlordiazepoxide should be avoided. DTC Reference 10052a Page 3 of 17 Review by June2012
5 2 The Alcohol Withdrawal Syndrome (AWS) 2.1 Symptoms of alcohol withdrawal 34 : Common Features Less-common Hand tremor Sweating, flushing Arrhythmias Minor hallucinations Tachycardia Hypertension Insomnia Convulsions Paraesthesiae Anxiety, agitation, Nausea, vomiting, Hepatic dysfunction confusion, disorientation anorexia, diarrhoea Suicidal ideation 40% of individuals will develop an acute withdrawal syndrome upon stopping or significantly curtailing alcohol intake. The risk of withdrawal is not directly related to intake. 24,35 Symptoms are seen within hours (typically 6 to 8) of the last drink and may develop before the blood alcohol level has fallen to zero. Symptoms outlined below may vary in severity, commonly peaking at 10 to 30 hours and usually subsiding by 40 to 50 hours. 1,12,24,34 Alcohol related seizures This includes epileptiform seizures (normally grand mal) that usually occur within 12 to 48 hours of alcohol cessation and may develop before the blood alcohol level has fallen to zero. 12 Fits are rare beyond 48 hours following alcohol cessation. 24 Delirium tremens (DTs) DTs occurs in about 5% of patients undergoing alcohol withdrawal but accounts for the highest morbidity and mortality. Untreated, DTs is fatal in 15-20% of patients whilst early detection and prompt initiation of treatment usually prevents onset. 4 Appropriate management reduces mortality to around 1%. 1 Onset of DTs is 2 to 5 days (most commonly at 2 to 3 days) following cessation and represents a medical emergency. 1,8,24,36,37 If untreated, death may result from respiratory and cardiovascular collapse or cardiac arrhythmias. Patients most at risk are those with a high fever (>104 F/39.9 C), tachycardia, dehydration and an associated illness (e.g. pneumonia or pancreatitis), general debility or where the diagnosis is delayed. 12 Characteristic symptoms of DTs 8,12,24,34,35,36 o Severe tremor o Clouding of consciousness o Delusions o Confusion and disorientation o Tachycardia>100/min o Agitation, violent behaviour o Delirium o Fever, with or without infection: temperature > 101 F/38.3 C o Severe hallucinations, often evoke extreme fear (mainly visual, may be tactile or auditory) 2.2 Risk factors for progression to severe withdrawal There is a risk of progression to severe withdrawal symptoms and delirium tremens if the patient with mild symptoms also has associated risk factors: 8,29&35 o Fever o High levels of anxiety o Tachycardia o Hypoglycaemia o Poor physical health o Insomnia o Sweating o Hypomagnesaemia o Hypocalcaemia o Other psychiatric disorders o Concomitant use of other psychotropic drugs o Hypokalaemia (with respiratory alkalosis) o High alcohol intake, > 15 units per day in a person of normal build o Previous history of severe withdrawal, seizures and/or DTs DTC Reference 10052a Page 4 of 17 Review by June2012
6 2.3 The detection of alcohol misuse All patients presenting to A&E or admitted to general medical or surgical wards should be asked about alcohol intake. None of the available laboratory markers are sufficiently sensitive or specific to be used as the sole means of detecting alcohol misuse The AUDIT (Alcohol Use Disorders Identification Test) questionnaire is the most appropriate means of identification of alcohol misusers in general hospitals (See appendix 4.2). The minimum score (for non-drinkers) is zero and the maximum possible score is 40. A score of 8 or more indicates a strong likelihood of hazardous or harmful alcohol consumption The CAGE questionnaire The CAGE questionnaire is a very brief assessment, which will only pick up the most severe alcohol misuse. CAGE is an acronym for four questions: 1) Have you ever felt you ought to CUT down on your drinking? 2) Have people ever ANNOYED you by asking you about your drinking? 3) Have you every felt bad or GUILTY about your drinking? 4) Have you ever had a drink first thing in the morning (EYE-OPENER) to steady your nerves or get rid of a hangover? A positive answer to 2 questions suggests alcohol dependence DTC Reference 10052a Page 5 of 17 Review by June2012
7 2.4 Medical Management 1st choice benzodiazepine: Oral administration of chlordiazepoxide Chlordiazepoxide has a lower potential for abuse than diazepam. 4,29 Intravenous diazepam or lorazepam has a more rapid onset of effect so may be preferred where urgent control is required. Formulary preparations Chlordiazepoxide Lorazepam Diazepam Capsules 5mg & 10mg Tablets 1mg & Injection 4mg/ml Tablets 2mg, 5mg, 10mg, oral solution 2mg/5ml, 5mg/5ml, injection (emulsion) 5mg/ml Patients with liver failure Chlordiazepoxide may be used cautiously in liver impairment; reduce the required dose by 50% of the normal dose. Lorazepam may be used in severe or acute liver impairment, its metabolism is not impaired in liver disease. Lorazepam has a shorter half-life than chlordiazepoxide which may increase the seizure risk. 29 Equivalent benzodiazepine doses (approximate) 31 Diazepam 10 mg = chlordiazepoxide 25mg = lorazepam 1mg The first 24 hours Give a stat dose of chlordiazepoxide 25mg to 50mg based on the severity of clinical signs and symptoms. If withdrawal symptoms are mild, an initial dose may not be required. Subsequent doses during the first 24-hours are administered with a frequency and dosage that depends upon the observations of alcohol withdrawal status rated by the ward staff using the CIWA-Ar scale (see appendix 3). If CIWA-Ar scale is 0 to 9: If CIWA-Ar scale is 10 to 14: If CIWA-Ar scale is 15 or above: no treatment is necessary 25mg should be administered 50mg should be administered Prescribe chlordiazepoxide on the As required section as written below: Drug Chlordiazepoxide Date Dose 25-50mg Every 2 hours Valid period 24 Hours only Route PO Doctor's Signature Additional Information If CIWA-Ar give 25mg If CIWA-Ar 15 or above give 50mg BEFORE GIVING ABOVE 300MG IN 24HOURS SEEK MEDICAL REVIEW Pharmacy DTC Reference 10052a Page 6 of 17 Review by June2012
8 Observations should be carried out every 2 hours Each set of observations consists of: - applying the alcohol withdrawal scale (CIWA-Ar) - taking BP - taking pulse - monitoring respiratory rate If the patient is asleep they should not be woken up to be scored for observations. However, it should be recorded that they were asleep. This is also to determine the amount of chlordiazepoxide that should be administered. The cumulative chlordiazepoxide dose administered during the initial 24-hour period assessed is called the baseline dose, and this is used to calculate the subsequent reducing regime. In complicated patients (e.g. DTs) consider increasing the 2 hourly observation and PRN dosing beyond the first 24 hours. Contact prescriber if patient is tachycardic or hypertensive. Frequency of observations may need to be altered in discussion with the medical team Days 2 to 6 Chlordiazepoxide five-day reducing regimen (days 2 to 5) After the initial 24-hour assessment period patients should be given chlordiazepoxide using a fixed reducing regimen. Ideally no chlordiazepoxide should be prescribed on a PRN basis after the initial 24 hours. Chlordiazepoxide is given in divided doses, usually four times a day. The dose is reduced by approximately 20% of the initial 24-hour dose per day. The following table indicate the form that this reducing dose should take according to the total dosage of chlordiazepoxide in the first 24 hours. These figures are estimates based on the tablet or capsule strength available. Observations should be carried out twice daily Observations (not including CIWA-Ar) may be carried out more frequently if any complications are seen. DTC Reference 10052a Page 7 of 17 Review by June2012
9 Day 1 total PRN Chlordiazepoxide 5-day reducing regimen Day 2 (mg) Day 3 (mg) Day 4 (mg) Day 5* (mg ) dose 8am 12pm 6pm 10pm 8am 12pm 6pm 10pm 8am 12pm 6pm 10pm 8am 12pm 6pm 10pm 300mg mg mg mg mg mg mg mg mg mg mg mg *If on Day 5 the patient is on a total daily chlordiazepoxide dose of 40mg or larger consider a longer reducing regimen by following the chart Difficult to control patients Consider increasing daily chlordiazepoxide dose above 300mg per day after medical review. Consider referral to the psychiatric liaison team for advice. Consider parenteral benzodiazepines. IV diazepam emulsion may be administered as a bolus by peripheral or central route. A dose of 10mg every minutes may be given until symptoms subside or the patient is markedly sedated. Usual maximum dosage is 30mg in 24 hours. Administer the undiluted emulsion at a rate of 1ml per minute (5mg per minute). Monitor for symptoms of withdrawal and sedation. Use of flumazenil in patients receiving benzodiazepines for management of alcohol withdrawal symptoms must be discussed with the Clinical Toxicology Team. For patients with liver failure, IV lorazepam 1mg to 2mg every 5 minutes should be used until the patient is awake but calm. 38 In the elderly, in general only half the benzodiazepine dose is recommended. Monitor ECG, blood pressure, respiratory rate pulse oximetry and temperature when giving high dose benzodiazepines. Consider antipsychotic Refer the patient to the appropriate psychiatric team who may consider the addition of an antipsychotic such as haloperidol or olanzapine to control agitation. e.g. Haloperidol po/im 2.5-5mg tds (Maximum 15mg IM or 30mg po in 24 hours), an ECG should be taken if haloperidol is given, the QTc should be <440ms in men and <470ms in females. All antipsychotics have the additional risk of lowering the seizure threshold, which is a particular concern in alcohol withdrawal. DTC Reference 10052a Page 8 of 17 Review by June2012
10 2.4.4 Management of Alcohol Withdrawal related seizures Prophylactic treatment of seizures in patients with a prior history of withdrawal seizures should be managed with diazepam 20mg or chlordiazepoxide 50mg administered orally upon presentation, followed by a further 2 doses at 1 hour intervals. 1 It may be suitable to then use CIWA-Ar scale along with a flexible 24 hour chlordiazepoxide regimen. Frequency of observations may need to be altered in discussion with the medical team. If status epilepticus occurs, usually this is managed with: IV Diazepam 2mg/min. Maximum mg. IV Lorazepam 2mg/min. Maximum 4-8 mg. There is little evidence to support the use of antiepileptics in the prophylaxis or treatment of alcohol withdrawal-induced seizures Patients who are difficult to assess using the CIWA-Ar score Prescribe a Fixed Schedule Reducing Regimen Start at Day 2 of the 5 day Withdrawal Scale These include patients who are delirious, confused, cannot speak English or are unable to communicate effectively. For these patients the CIWA-Ar scale is inappropriate as the patient will not be able to score on anxiety, orientation and clouding of sensorium, tactile, auditory and visual disturbances. If a score is inappropriate it is difficult to give the correct dose of Chlordiazepoxide. Therefore, it is recommended to put the patient on a Fixed Schedule Reducing Regimen. It may be necessary to chart PRN Chlordiazepoxide for the first 24 hours in case of breakthrough symptoms. If the PRN doses are utilised a review of the fixed regimen doses are needed after 24 hours. The doses will need to be increased to take into account the PRN utilisation Elderly Patients To minimise adverse effects associated with benzodiazepines (e.g. over sedation, confusion and ataxia) in the elderly it is important to bear in mind the start low and go-slow rule. In general it is recommended that half the dose of the benzodiazepine is used Pregnant Patients As in any patient who may be pregnant or is pregnant, each case is dealt with on an individual basis. It is important to bear in mind the risk of seizure against the risk of foetal exposure to chlordiazepoxide. It is essential the obstetric team is informed if the patient presents during late pregnancy or in labour. The Psychiatric Liaison services can be contacted for advice please see page 17 for contact details. Long term regular use of chlordiazepoxide should be avoided. DTC Reference 10052a Page 9 of 17 Review by June2012
11 3 Wernicke s encephalopathy (WE) Inappropriately managed WE 22 is the primary contributory cause of death in 17% of affected patients and results in permanent brain damage in 85% of survivors. Post-mortem analysis has demonstrated that WE may occur in as many as 12.5% of chronic alcohol misusers, although WE or Korsakoff s psychosis has historically been diagnosed during life in only 5-20% of patients. 2,13,14 The classically described triad of signs acute confusion (82%), ataxia (23%) and ophthalmoplegia (29%) actually occurs in only 10% of patients. 14 As a result the triad cannot be used as the basis of a diagnosis. 3.1 Treatment Wernicke s encephalopathy is reversible in the early stages with rapid restoration of CNS B-vitamins (in particular thiamine) and treatment should be initiated immediately a diagnosis is suspected. 6,24,39 The diagnosis should be based on the presence of any one or more of the following signs in the absence of another more probable explanation of these features. 4,6,7,24 Acute confusion Decreased consciousness level including unconsciousness or coma Memory disturbance Ataxia/unsteadiness Ophthalmoplegia (eye muscle paralysis causing squint or double vision) Nystagmus (involuntary rhythmic oscillation of one or both eyes) Unexplained hypotension with hypothermia. Treatment of Wernicke s encephalopathy Pabrinex IVHP 2 pairs of ampoules three times daily for 3 to 7 days Treatment should be continued after 3 days until no further improvement is seen. Pabrinex can be given intramuscularly in very exceptional circumstances each pair has a volume of 7mL. It is extremely painful and the risk of haematoma is significant. Under these circumstances it may only be possible to give ONE pair (7mL) IM at a time and this dose repeated as often as the patient will tolerate. Consider reverting to intravenous therapy as soon as possible. DTC Reference 10052a Page 10 of 17 Review by June2012
12 3.2 Prophylaxis All patients undergoing alcohol withdrawal should be treated prophylactically for WE. This includes anyone admitted for other reasons who are subsequently found to require detoxification, 7 as well as those with a known/suspected history of alcohol misuse. 4,6,10,24,29&40 Prophylaxis against Wernicke s encephalopathy Pabrinex IVHP 1 pair of ampoules three times a day for 1 day Administration Each pair of ampoules should be diluted in 50ml to 100ml sodium chloride 0.9% or glucose 5% and infused over 30 minutes. Pabrinex can be given intramuscularly in very exceptional circumstances each pair has a volume of 7mL. It is extremely painful and the risk of haematoma is significant. Under these circumstances it may only be possible to give ONE pair (7mL) IM at a time and this dose repeated as often as the patient will tolerate. Consider reverting to intravenous therapy as soon as possible. Safety of parenteral B-vitamins Parenteral thiamine administration is associated with a very small risk of anaphylaxis (5 cases per 1 million IV ampoules). As a result the Committee on the Safety of Medicines (CSM) advises that 3 : use be restricted to patients in whom parenteral treatment is essential. (parenteral treatment is considered essential for all patients in alcohol withdrawal) intravenous injections be administered slowly facilities for treating anaphylaxis be available 3.3 Oral B-vitamin absorption in alcohol misusers Absorption of oral thiamine is limited and not sufficient to treat WE. Absorption of thiamine appears to be independently affected by both alcohol and malnutrition. Absorption is reduced by around 70% in abstemious malnourished alcohol misusers. Absorption is reduced further in the presence of alcohol. 6 An inadequate diet combined with reduced absorption frequently results in insufficient thiamine to meet daily requirements with a consequent depletion of body stores. Thiamine 100mg three times a day plus oral vitamin B compound strong 2 tablets once a day should be considered after parenteral administration of B vitamins for 14 days or until review by the GP. Thiamine 100mg TDS and Vitamin B compound strong 2 Tablets OD Continue at discharge for 14 days and then GP to review. Oral should be continued for at least 6 weeks DTC Reference 10052a Page 11 of 17 Review by June2012
13 Appendix 4.1, Referring Patients Who to refer? Refer patients with the following presentation to the appropriate psychiatric team at the earliest opportunity: - Patients with co-morbid psychiatric complications - Patients experiencing complications on withdrawal e.g. hallucinations - Patients who have recently self harmed - Behaviourally disturbed patients with delirium tremens - Alcohol dependence in pregnancy can be referred directly to the community drug and alcohol team (CDAT) at Blackfriars Road. Which team to refer to on Medical and Surgical Wards? General liaison psychiatry team, bleep 0123 (24 hours) or extension 83486/ (normal working hours) Addictions Liaison nurse, bleep 0497 (normal working hours) Specialist Psychiatric Pharmacist, bleep 2436 (normal working hours) Older adults (> 65yo) liaison psychiatry team, Bleep 0449 or extension (normal working hours), or refer on epr. Accident and Emergency or CDU, (24 hours) A+E liaison psychiatry team, Bleep 0482 or extension 82152/ Neuropsychiatry Team, for patients with lasting cognitive deficits after acute withdrawal is complete. Fax referral request to (normal working hours) Local Community contacts Contact the community team as early as possible after the patient s admission. The community team will only accept patients who are residents in their catchment area. Blackfriars Road CDAT (North Southwark Patients) 151 Blackfriars Road SE1 8EL. Tel: (Mon Fri (except Tues) pm; Tues pm then 4.00pm pm late clinic till 7.00pm late clinic appointments only). Lewisham Community Drug and Alcohol Service The Central Clinic 410, Lewisham High Street SE13 6LJ. Tel: (Mon, Wed and Thurs pm; Tues pm; Fri am & 12-5 pm). Maudsley Hospital Community Alcohol Service (covers Lambeth and South Southwark) Marina House, Denmark Hill, SE5 8AZ. Tel: (Southwark), (Lambeth). (Opening times: Mon, Wed, Thurs and Fri 9 12:30 then 2: pm; Tues 9 12:30 and 4-7pm; Sat 9-12:30pm limited service). SMART project (covers Lambeth/ Southwark and Lewisham) 9a Mitcham Lane, SW9 9NT. Tel (Opening times: Mon to Wed 10-5pm, Thurs 2-5pm, Friday 10 2pm) DTC Reference 10052a Page 12 of 17 Review by June2012
14 Appendix 4.2, AUDIT (Alcohol Use Disorders Identification Test) Circle the number that comes closest to the patient s answer How often do you have a drink containing alcohol? (0) NEVER (1) MONTHLY (2) TWO TO FOUR (3) TWO TO THREE OR LESS TIMES A MONTH TIMES A WEEK (4) FOUR OR MORE TIMES A WEEK How many drinks containing alcohol do you have on a typical day when you are drinking? (Code number of standard drinks = units) (0) 1 OR 2 (1) 3 OR 4 (2) 5 OR 6 (3) 7 TO 9 (4) 10 OR MORE How often do you have six or more drinks on one occasion? (1) LESS THAN (0) NEVER (2) MONTHLY (3) WEEKLY MONTHLY (4) DAILY OR ALMOST DAILY How often during the last year have you found that you were not able to stop drinking once you had started? (0) NEVER (1) LESS THAN MONTHLY (2) MONTHLY (3) WEEKLY (4) DAILY OR ALMOST DAILY How often during the last year have you failed to do what was normally expected from you because of drinking? (0) NEVER (1) LESS THAN MONTHLY (2) MONTHLY (3) WEEKLY (4) DAILY OR ALMOST DAILY How often during the last year have you needed a first drink in the morning to get yourself going after a heavy drinking session? (0) NEVER (1) LESS THAN MONTHLY (2) MONTHLY (3) WEEKLY (4) DAILY OR ALMOST DAILY How often during the last year have you had a feeling of guilt or remorse after drinking? (0) NEVER (1) LESS THAN MONTHLY (2) MONTHLY (3) WEEKLY (4) DAILY OR ALMOST DAILY How often during the last year have you been unable to remember what happened the night before because you had been drinking. (0) NEVER (1) LESS THAN MONTHLY (2) MONTHLY (3) WEEKLY Have you or someone else been injured as a result of your drinking? (0) NO (2) YES, BUT NOT IN THE LAST YEAR (4) YES, DURING THE LAST YEAR (4) DAILY OR ALMOST DAILY Has a relative or friend or a doctor or other health worker been concerned about your drinking or suggested you cut down? (0) NO (2) YES, BUT NOT IN THE LAST YEAR (4) YES, DURING THE LAST YEAR Cumulative score The minimum score (for non-drinkers) is zero and the maximum possible score is 40. A score of 8 or more indicates a strong likelihood of hazardous or harmful alcohol consumption. 41 DTC Reference 10052a Page 13 of 17 Review by June2012
15 Appendix 4.3, Clinical Institute Withdrawal Assessment of Alcohol Scale, Revised (CIWA-Ar) Using the descriptions below rate each withdrawal symptom then add the scores together. If CIWA-Ar result is between 10 to 14 give 25mg or if above 15 give 50mg of chlordiazepoxide. Nausea and Vomiting: Ask Do you feel sick to your stomach? Have you vomited? Observation 0 no nausea with no vomiting 1 mild nausea with no vomiting intermittent nausea with dry heaves constant nausea, frequent dry heaves and vomiting Tremor: Arms extended and fingers spread wide apart. Observation 0 no tremor 1 not visible, but can be felt fingertip to fingertip moderate, with patients arms extended severe, even with arms not extended Paroxysmal Sweats: Observation 0 no sweat visible 1 barely perceptible sweating, palms moist beads of sweat obvious on forehead drenching sweats Anxiety: Ask Do you feel nervous? Observation 0 no anxiety, at ease 1 mildly anxious moderately anxious or guarded, so anxiety is suggested equivalent to acute panic states as seen in severe delirium or acute schizophrenic states Agitation: Observation 0 normal activity 1 somewhat more than normal activity moderately fidgety and restless paces back and forth during interview, or thrashes about Tactile (touch) Disturbances: Ask Have you any itching, pins and needles sensations, any burning, any numbness, or do you feel bugs crawling on or under your skin? Observation 0 none 1 very mild itching, pins and needles, burning or numbness 2 mild itching, pins and needles, burning or numbness 3 moderate itching, pins and needles, burning or numbness 4 moderately severe hallucinations 5 severe hallucinations 6 extremely severe hallucinations 7 continuous hallucinations Auditory (hearing) Disturbances: Ask Are you more aware of sounds around you? Are they harsh? Do they frighten you? Are you hearing anything that is disturbing you? Are you hearing things you know are not there? Observation 0 not present 1 very mild harshness or ability to frighten 2 mild harshness or ability to frighten 3 moderate harshness or ability to frighten 4 moderately severe hallucinations 5 severe hallucinations 6 extremely severe hallucinations 7 continuous hallucinations Visual (sight) Disturbances: Ask Does the light appear to be too bright? Is it s colour different? Does it hurt your eyes? Are you seeing anything that s disturbing you? Are you seeing anything that you know is not there? Observation 0 not present 1 very mild sensitivity 2 mild sensitivity 3 moderate sensitivity 4 moderately severe hallucinations 5 severe hallucinations 6 extremely severe hallucinations 7 continuous hallucinations Headache, Fullness in Head: Ask Does your head feel different? Does it feel like there is a band around your head? Do not rate for dizziness or lightheadedness. Otherwise, rate severity. Observation 0 not present 1 very mild 2 mild 3 moderate 4 moderately severe 5 severe 6 very severe 7 extremely severe Orientation and Clouding of Sensorium: Ask "What day is this? Where are you? Who am I?" 0 orientated and can do serial additions 1 cannot do serial additions or is uncertain about date 2 disorientated for date by no more than 2 calendar days 3 disorientated for date by more than 2 calendar days 4 disorientated for place or person DTC Reference 10052a Page 14 of 17 Review by June2012
16 Appendix 4.4, Alcohol withdrawal nursing observation chart (based on CIWA-Ar scale) Begin using this chart at the first sign of withdrawal symptoms Name: (or affix label) Ward: Consultant: Sheet Number: Date: Time: 24hour clock (Hrs) Respiratory Rate: (breaths per minute) If below 10 inform medical team Nausea / Vomiting (0-7) Tremor (0-7) Sweats (0-7) Anxiety (0-7) Agitation (0-7) Tactile disturbances (0-7) Auditory disturbances (0-7) Visual Disturbances (0-7) Headache (0-7) Orientation (0-4) TOTAL SCORE (MAX 67) Dose given (mg) PLEASE SIGN DRUG CHART If CIWA-Ar scale is Give 25mg of chlordiazepoxide If CIWA-Ar scale 15 Give 50mg of chlordiazepoxide Nurses Signature Total Dose of chlordiazepoxide in 24 hours = Do not exceed maximum dose of 300mg in 24 hours. This acts as the baseline dose. Then proceed to calculate 5 day (or longer if required) reducing regimen. DTC Reference 10052a Page 15 of 17 Review by June2012
17 Appendix 4.5, Patient Information National Services Alcohol Concern visit This website has lots of useful information in their library and publication section as well as factsheets that could be given directly to patients. Drinkline Tel (Available: 24 hours 7 days a week) or visit Alcoholics Anonymous Tel (Available: 7 days a week 10am 10pm) or visit The London Drug and Alcohol Network visit The Tool find a service allows you to find a community alcohol centre that is local to the patients address. DTC Reference 10052a Page 16 of 17 Review by June2012
18 5. References 1. Adinoff B et al. Medical Toxicology 1988; 3: Blansjaar BA & Van Dijk JG. Alcohol & Alcoholism 1992; 27 (4): BNF No 55, March 2008; Pharmaceutical Press, Bedfordshire. 4. Chick J. Hospital Pharmacist 2000; 7: Cook CCH et al. B-Complex vitamins in the prophylaxis and treatment of Wernickes Korsakoffs Syndrome. British Journal of Hospital Medicine, 1997 (57) Cook CCH et al. Alcohol & Alcoholism 1998; 33 (4): Cook CCH. Alcohol & Alcoholism 2000; 35 (Suppl 1): Glen I et al. The management of alcohol withdrawal & delirium tremens: A good practice statement. CRAG/SCOTMEG Working Group on Mental Illness. Final report June Greenblatt DJ et al. Clinical Pharmacokinetics of anxiolytics and hypnotics in the elderly. Therapeutic considerations (Part I). Clinical Pharmacokinetics, 1991 Vol21(3), Corrigan, JD et al. [1995], J Head Trauma Rehabilitation, 10(3): Guirguis a, Kenna G. Treatment considerations for alcohol withdrawal syndrome, US Pharmacist. 12. Hall W & Zador D. Lancet 1997; 349: Harper C. Journal of Neurology, Neurosurgery and Psychiatry 1979; 42: Harper CG et al. Journal of Neurology, Neurosurgery and Psychiatry 1986; 49: Hillburn M et al. Seizures in alcohol dependent patients. Therapy in Practice. CNS Drugs 2003, 17(14); Korsten T, O Connor P. Management of Drug and Alcohol Withdrawal, The New England Journal of Medicine, May 1,2003; 348; Lange-Arschenfeldt et al, Symptom triggered vs standard chlormethiazole treatment of inpatient alcohol withdrawal, European Addiction Research; 9; Lingford-Hughes AR, Welch S, Nutt DJ. Evidence-based guidelines for the pharmacological management of substance misuse, addiction and co-morbidity: recommendations from the British Association for Psychopharmacology. J of Psychopharmacology 2004; 18(3): Martin PR et al. The role of thiamine deficiency in alcoholic brain disease. Alcoholic Research and Health 2003, 27(2). 20. Markowitz J et. Al. Oral nutritional supplementation for the alcoholic patient: a brief overview. Annals of Clinical Psychiatry 2000, 12(3). 21. Malcolm R. Alcohol withdrawal, relapse prevention. Psychiatric Annals; 3; McIntosh C et. Al. Parenteral Thiamine use in the Prevention and Treatment of Wernicke s Korsakoffs Syndrome, Psychiatric Bulletin 2005 (29); McKay G. Thiamine Treatment of Wernicke s Encephalopathy: Guidelines and Issues. 24. Morgan MY & Ritson B. Alcohol and Health Medical Council on Alcoholism, London. 25. Office for National Statistics (ONS) Living in Great Britain: results for the 1998 General Household Survey, the Stationary Office, London. 26. Pabrinex IVHP, Summary of Product Characteristics, April Reoux JP, Miller K, Routine hospital alcohol detox compared with symptom triggered management with CIWA-Ar. The American Journal on Addictions 9; Ritson B. ABC of alcohol. Treatment of alcohol related problems. BMJ 2005 Vol Royal College of Physicians (RCP). Alcohol can the NHS afford it? Royal College of Physicians of London Smith M. Pharmacological Management of Alcohol Withdrawal : A meta-analysis and evidence based practice guidance, 1997, 278 (2). 31. Taylor et al (2007) The South London and Maudsley NHS trust 2007, 9 th Edition Prescribing guidelines, Taylor & Francis, London 32. Thomson AD et al. Patterns of S-Thiamine hydrochloride absorption in the malnourished alcoholic patient. J Lab Clinical Medicine, July Thomson AD et al. The Royal College of Physicians report on alcohol; Guidelines for managing Wernickes Encephalopathy in the A & E department, Alcohol and Alcoholism (37); Wills S (2005) Drugs of abuse 2 nd edition, Pharmaceutical Press, London. 35. Drug and Therapeutics Bulletin, [1991], 29(18): Erwin WE, Williams DB, Speir WA. Delirium tremens. South Med J. 1998, 91(5): Rubino, FA. Neurologic complications of alcoholism. Psychiatry Clinical, North America, (1992) 15(2): Turner A et al [1989] J General Intern Medicine, 4: BMJ. Wernicke's encephalopathy. Br Med J 1979;2; Ferguson, R. K., Soryal, I. N. and Pentland, B. (2000) Wernicke Korsakoff syndrome in head injury: a missed insult. Alcohol and Alcoholism 35 (Suppl. 1), Saunders, J.B., Aasland, O.G., Babor, T.F., De La Fuente, J.R. and Grant, M., Development of the Alcohol Use disorders Identification Test (AUDIT): WHO Collaborative Project on Early Detection of Persons with Harmful Alcohol Consumption. II. Addiction 88, pp Main Authors Azizah Attard Senior Psychiatric Liaison Pharmacist St Thomas Hospital Nicola Torrens Senior Admissions Pharmacist St Thomas Hospital Carl Holvey Senior Psychiatric Liaison Pharmacist St Thomas Hospital Consulters of these guidelines Grainne D Ancona Principal Pharmacist Medicine Simon Paton Addiction Liaison Nurse - Addiction Services St Thomas Hospital Dr Mark Kinirons Consultant Physician St Thomas Hospital Dr Gopinath Ranjith Consultant Psychiatrist St Thomas Hospital DTC Reference 10052a Page 17 of 17 Review by June2012
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