Pharmacology in Liver Disease. Sandeep Whitehead Advanced Clinical Pharmacist Hepatology and Liver Transplant

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Pharmacology in Liver Disease Sandeep Whitehead Advanced Clinical Pharmacist Hepatology and Liver Transplant

Objectives Outline the drug management for patients with: Ascites Spontaneous Bacterial Peritonitis (SBP) Encephalopathy Bleeding varices Hepatorenal syndrome Pruritus Alcohol withdrawal Describe the factors which need to be considered when selecting drugs and dosage regimens in chronic liver disease.

Ascites Treatment aim- mobilisation of intra-abdominal fluid No added salt diet (80mmol/day) Diuretics Fluid restriction to 1.5-2L/day (if serum sodium <130mmol/l) 90% of patients can be managed as above Paracentesis TIPSS (transjugular intrahepatic portosystemic shunt)

Drug Choices - Diuretics Aldosterone antagonist: Spironolactone 100-400mg od Increased aldosterone due to activation & reduced degradation by liver Plus/minus Loop diuretic: Frusemide (40-160mg od) Bumetanide (1-4mg od )

Diuretics - side effects Hyperkalaemia (spironolactone) Hypokalaemia (loop diuretics) Hyponatraemia (stop if Na <120mmol/L) Nephrotoxicity Gynaecomastia (Spironolactone) Encephalopathy (electrolyte disturbances)

Monitoring Daily weight aim to lose 0.5kg/day or 1-2kg/day if peripheral oedema Dose titrate every 3-5 days U&Es Renal function (creatinine, urea) Na, K

Spontaneous Bacterial Peritonitis Start antibiotics whilst awaiting the results of culture of ascitic fluid eg. Piperacillin Tazobactam IV 4.8g 8 hourly (some centres use Cefuroxime, Ciprofloxacin) Treat for 5 days- when clinically improved Long term prophylaxis Previous episodes of SBP Ascitic protein <10g/l =Co-trimoxazole 960mg OD

Encephalopathy Treatment aim: to improve cognitive function Events precipitating hepatic encephalopathy: Infection Bleeding e.g. GI Electrolyte imbalance Constipation Drugs Acute liver failure Porto-systemic shunts

Treatment Identify & treat precipitating factors Remove causative drugs: Sedating e.g. benzodiazepines Constipating e.g. opioids Diuretics electrolyte imbalance

Treatment Lactulose 10-50ml bd-tds Laxative effect Broken down in gut leading to acidification of colonic contents and a reduction in absorption of nitrogenous waste Side effects of lactulose Flatulence Abdominal pain Diarrhoea Enemas If NBM

Antibiotics for Encephalopathy Rifaximin 550mg BD broad antimicrobial spectrum against most of the Grampositive and negative, aerobic and anaerobic bacteria, including ammonia producing species reducing the production of ammonia and other compounds that are believed to be important to the pathogenesis of hepatic encephalopathy. Side effects Nausea Anaemia Ascites Peripheral Oedema

Monitoring Stool chart Aim to produce 2-3 loose stools a day Temperature if infection Cognitive improvement Number connection tests Serial sevens

Bleeding Varices Aims of Treatment Resuscitate (blood/ffp/colloids) Control bleeding (medical & endoscopic treatment) Prevent complications Prevent re-bleeding Stop bleeding Drug therapy: Terlipressin, Octreotide Plus 1 of: Sclerotherapy Endoscopic Oesophageal Banding Adhesives e.g. Histoacryl glue for gastric varices TIPSS (transjugular intrahepatic portosystemic shunt)

Octreotide & Terlipressin Reduce portal pressure by causing splanchic vasoconstriction Reduce re-bleeding rates Terlipressin (reduced mortality) 1-2mg IV bolus 4-6 hourly (usually 2mg qds) Octreotide (unlicensed use) Continuous IV infusion - 50mcg/hour Usually discontinued 2 days after bleeding stopped (terlipressin licensed for 72 hrs)

Terlipressin side effects Abdominal cramps Headache Increased blood pressure

Monitoring: Terlipressin/ Octreotide Bleeding Blood Pressure Length of treatment course

Antibiotics in Variceal Bleed Reduce bacteraemia: SBP Reduce short term mortality Local policy Piperacillin-Tazobactam 4.5g IV for 48 hours

Prevention of recurrent variceal bleeding Non-selective beta-blockers e.g. Propranolol or Nadolol Reduce portal pressure by decreasing splanchnic blood flow and the hyperdynamic circulation associated with cirrhosis Starting dose: propranolol 20-40mg bd up to 80mg bd Reduce mortality

Beta blocker side effects Bronchospasm (CI in asthma) Bradycardia Hypotension Peripheral vasoconstriction Fatigue Impotence

Beta blocker monitoring BP - Aim for >100mmHg systolic (some patients may tolerate lower) Heart rate Aim of treatment is to reduce HR to 25% less than baseline (above 55bpm)- this is the maximum tolerated dose)

Hepatorenal Syndrome (HRS) Renal impairment associated with liver disease Low arterial pressure, reduced renal perfusion Aim to increase renal perfusion and renal function Vasoconstrictors constrict splanchic bed and increase renal perfusion Poor prognosis

Treatment of HRS Terlipressin IV used most frequently Unlicensed use Range of doses in studies from 0.5mg bd to 2mg 6 times a day In practice, St James s liver unit use 1mg qds In combination with 20% HAS **Remove any nephrotoxic medications

Pruritus in liver disease Cause? Subjective; varies from patient to patient Can be all over body, in eyes, ears etc or isolated areas Often worse at night and when hot Can be debilitating Can be indication for liver transplant Efficacy of treatment can be monitored by visual analogue scale

Pruritis Treatment options Topical preparations E.g. menthol 1% in aqueous cream Do not apply on broken skin Short term, immediate relief May not be useful for patients with generalised all over itch Antihistamines non-sedating (e.g. cetirizine)-? ineffective sedating (e.g.chlorpheniramine) Sedating drugs can be useful at night to aid sleep

Cholestyramine (Questran ) Anion exchange resin; forms insoluble complexes with bile acids in the intestine and excreted in faeces (prevents their absorption). Initiate at 4g od or bd May take 48hours to take effect Reduces absorption of other drugs - give other drugs 1 hour before or 4-6 hours after colestyramine Can mix in drinks / incorporate into recipes

Cholestyramine side effects Not absorbed therefore no systemic side effects: Unpleasant taste Constipation Occasionally, diarrhoea Nausea & vomiting Can cause depletion of fat soluble vitamins long term

Ursodeoxycholic acid Naturally occurring bile acid; displaces toxic bile acids from enterohepatic pool, protects cells from toxic bile acids and stimulates bile excretion. displacement theory Dose: 10-15mg/kg/day Can be given in divided doses or single dose Can take up to 2 weeks to take effect May worsen itch!

Other options for Pruritis Rifampicin / Phenobarbitone Induce hepatic enzymes Not licensed for this indication Rifampicin 150mg bd, increase to 300mg bd Takes 48 to 72 hours to work Interacts with lots of drugs (not ideal post transplant) Colours urine red

Ondansetron Not licensed for this indication 5HT3 antagonist Inhibits perception of itch Anecdotal reports suggest IV has been effective (within 1 hour) If effective after stat IV dose, give oral 4mg bd increasing to 8mg bd

Opioid antagonists; Work quickly but patients become tolerant, therefore regular dose increases necessary Naloxone continuous infusion Naltrexone orally 25-50mg daily Serotonin Selective Reuptake Inhibitors eg Sertraline Gabapentin

Alcohol Withdrawal Anxiety, tremor, sweating, nausea, tachycardia, hypertension, hallucinations Chlordiazepoxide (regular and prn) Initially chlordiazepoxide ~20-30mg qds + 5-10 mg prn A maximum daily dose of 120mg Reducing course over ~ 7 days

Wernicke s encphalopathy Vitamin B deficiency Thiamine -100mg tds Vitamin B Co. strong- 2 tabs tds High risk Pabrinex IV 1 pair Daily for 3-5 days Anaphylaxis risk give over >10mins Treatment (1 or more signs present) Pabrinex IV 2 pairs tds for 2 days followed by 1 pair twice a day until improvement ceases

How to determine a patient s liver function and how it effects drug handling There isn t a book that gives dosing of drugs in liver impairment No way of measuring directly the liver s ability to metabolise drugs Effects of liver impairment on the way drugs are handled in the body not consistent & predictable Limited published information available (which maybe misleading e.g. from manufacturers)

References Drugs and the Liver A guide to drug handling in liver dysfunction Edited by Penny North-Lewis Paediactric Liver Pharmacist, SJUH

Need to consider lots of factors.. LFTs Clotting function Signs Diagnosis Other investigations e.g. biopsy, ultrasound The drug

Drug handling in particular patient Liver Test Results The patient Drug Characteristics e.g. how drug is handled in body and side effects Signs of Liver Disease

The drug Absorption Distribution Metabolism Elimination Side Effect profile Hepatotoxicity

Absorption of drugs Absorption of some drugs may be affected by oedema in ascites (e.g. frusemide?- less absorption in gut wall) Fat soluble drugs have reduced absorption in cholestasis (e.g. fat soluble vitamins) The effect of fat soluble drugs may be increased in Cachetic patients

Distribution Fat soluble drugs are not affected by ascites Water soluble drugs will distribute into ascitic fluid which may lead to lower serum concentration and reduce efficacy May need to increase dose

Distribution Reduced albumin levels If highly protein bound drugn (ie binds to albumin); Increased free drug available= toxic E.g phenytoin (90%), warfarin (99%) **May need to reduce dose

Metabolism Reduced number of hepatocytes may lead to reduced metabolism of drugs (to active/ inactive form) Reduced hepatic flow in portal hypertension/ cirrhosis leads to increased systemic availability (reduced first pass metabolism)

Elimination Accumulation may occur in cholestatic patients if the drug undergoes biliary excretion a problem if active/toxic metabolites are produced alternative routes of elimination? e.g. kidneys

Side Effect Profile Drugs with the following side effects may need to be avoided/used with caution; Sedation Constipation Coagulopathy Effects on electrolytes Effects on fluid balance Renal toxicity GI ulceration

Drugs to avoid/use cautiously NSAIDs/ Anticoagulants In cirrhotics risk of varices/bleeding abnormalities Sedatives In cirrhotics/encephalopathics sedatives mask/precipitate encephalopathy. Constipating drugs Risk of encephalopathy with constipation Diuretics Electrolyte imbalance can precipitate encephalopathy Sodium containing drugs e.g. IV or effervescent preparations May worsen ascites

Important Points to Consider Avoid or use certain drugs cautiously Avoid hepatotoxic drugs if possible Use therapeutic levels, where possible Monitor for efficacy eg BP, HR Monitor for toxicity Check renal function Use the smallest effective dose at the greatest interval and titrate according to response Take Care: not to under dose!

Drug Choice in liver disease Analgesics Paracetamol normal doses Opiates small doses, titrate slowly care with constipation/sedation (encephalopathy) Antidepressants SSRI s e.g Fluoxetine, venlafaxine over older sedating drugs e.g. amitriptyline (tricyclic antidepressant) Anti-emetics Ondasetron Benzodiazepines Short acting

Any Questions?