Mr Ricky Gellissen Imperial College Healthcare NHS Trust, London, UK

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Mr Ricky Gellissen Imperial College Healthcare NHS Trust, London, UK Ms Sally Bufton University Hospital Birmingham NHS Foundation Trust, Queen Elizabeth Hospital, Birmingham

Mrs Janet Catt Royal Free London NHS Trust, UK

Mrs Janet Catt Royal Free London NHS Trust, UK Speaker Name COMPETING INTEREST OF FINANCIAL VALUE > 1,000: Statement Janet Catt Date

Janet Catt MSc RN Lead Nurse Specialist Practic

Liver blood tests monitoring cirrhosis HIV/HCV coinfection patients

Liver disease is currently one of the leading causes of morbidity and mortality among HIV infected patients in Western countries. HIV/HCV coinfected patients have a 3-fold greater risk of progression to cirrhosis or decompensated liver disease than HCV mono infected patients (Graham et al 2001) The accelerated rate is magnified in patients with low CD4 cell counts Cirrhotic patients should be carefully assessed by an expert in advanced liver disease for signs of liver decompensation.

Blood tests help build a picture of how the liver is functioning.. However, don t also forget to assess your patient individually. There may be another explanation ie, holidays abroad to high risk countries Tattoo Drugs, including Chinese herbal remedies recent unprotected sexual intercourse alcohol

Liver function tests easily measured as part of routine blood test analysis Detect the presence of liver disease Gauge the extent of known liver damage Follow response to treatment Rarely suggest a specific diagnosis but can categorise as to whether there is damage or destruction directly to liver cells (hepatocellular) or impaired transport of bile (cholestatic) They can further direct evaluation of the patient

ALT / AST : Are liver enzymes in liver cells, when injury to liver cells occurs these are released into blood causing amounts in blood to increase ALT mainly found in the liver AST low specificity for liver found also in heart and other muscles in the body.

Both will be raised in recent liver injury does not tell anything about residual function capacity If there is reversal of AST:ALT ratio, and in the context of viral hepatitis this is a very good clue that there is advanced liver disease (but can also occur with Alcohol/NASH) If levels are decreasing: Liver cells are so damaged that there are no more cells to damage Improving, and no further damage

Enzyme found mainly in the liver Alcohol makes GGT elevated Can be associated with cholestasis If Alkaline Phosphatase (ALP) is elevated check GGT. If normal = not associated with liver If raised = most probably liver related disease

Indicated in: 1) Cholestasis - Bile cannot flow from liver to the duodenum. a) bile acids stimulate AFP (b) Duct obstruction or damage prevents bile acid excretion into duodenum so ALP levels in serum rise significantly 2) Pregnancy 3) Bone disease (bone growth) ie Pagets disease, prostate and breast cancer

Albumin: synthesised in liver, a reliable marker of chronic liver injury if decreased. Albumin has a 20 day half life, which means takes a longer time for Albumin to decrease, so usually a marker of chronic disease

True test of liver function, reflects the liver s ability to take up, process and secrete bilirubin into bile. (Red blood cells are removed from circulation by the SPLEEN RBC live 120 days and can travel of a total of 300 miles within our body) Remaining urobilinogen reabsorbed into circulation (bile and urine) Haem is broken down into Bilirubin Uncong bili (yellow pigment), water insoluble, bound to blood protein (Albumin) travels to liver some converted by gut bacteria into urobilinogen, then stercobilinogen Bilirubin Converted in liver to conj bilirubin by glucuronyl transferase and becomes water soluble Secreted into the intestines to be excreted out of the body conj bili put into fluid Bile, which is formed in Liver and stored in Gallbladder

PT / INR The most sensitive test for liver disease. A simple measure of liver s capacity to synthesise clotting factors. The first indication that the liver is starting to fail. Requires so many proteins that are synthesised in the liver. If liver not processing, then takes longer for coagulation to occur. PT / INR will start to rise

Low platelets (thrombocytopenia) Enlarged spleen (on liver u/s) should not be able to palpate a healthy spleen splenomegaly Spleen filters blood (RBC/WBC and platelets) Cirrhosis cause pressure/congestion in portal vein system, and increases blood flow back to the spleen This causes cells to accumulate in the spleen, enlarging the spleen and depleting the platelet count. Remember to also monitor renal function

HIV/HCV co-infection patients with suggestions of advanced liver disease should always be referred to a Hepatologist for further investigation. Avoid drugs that may cause hepatoxicity and risk of decompensation discuss with specialist Pharmacist if unsure HCC surveillance: liver ultrasound + AFP every 6 months

THANK YOU Janet.Catt@nhs.net