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Transcript 
Evaluation of Liver Function tests in Primary Care
Abid Suddle
Institute of Liver Studies, KCH
Liver Function tests
• Markers of hepatocellular damage
• Cholestasis
• Liver synthetic function
Markers of Hepatocellular damage
Transaminases
• AST‐ liver, heart skeletal muscle, kidneys, brain, RBCs
• In liver 20% activity is cytosolic and 80% mitochondrial
• Clearance performed by sinusoidal cells, half‐life 17hrs
• ALT – more specific to liver, v.low concentrations in kidney and skeletal muscles. • In liver totally cytosolic.
• Half‐life 47hrs
Markers of Cholestasis
• ALP – liver and bone (placenta, kidneys, intestines )
• Hepatic ALP present on surface of bile duct epithelia and accumulating bile salts increase its release from cell surface. • ALP isoenzymes, 5‐NT or gamma GT may be necessary to evaluate the origin of ALP
• Gamma‐GT – hepatocytes and biliary epithelial cells, pancreas, renal tubules and intestine
• Very sensitive but Non‐specific
• Confirm hepatic source for a raised ALP
• Alcohol
Markers of liver synthetic function
Bilirubin, Albumin and PT (INR)
• Useful indicators of liver synthetic function
• In primary care when associated with liver enzyme abnormalities should raise concern
• Thrombocytopaenia is a sensitive indicator of liver fibrosis
Patterns of liver enzyme alteration
• Hepatic vs cholestatic
• Magnitude of enzyme alteration (ALT >10x vs minor abnormalities)
• Rate of change
• Nature of the course of the abnormality (mild fluctuation vs progressive increase)
COMMON CAUSES OF ABNORMAL LFTS IN THE UK
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Transient mild abnormalities Drugs – eg Statins
Alcohol excess
Viral hepatitis
Non‐Alcoholic Fatty Liver Disease (NAFLD)
Investigation of Abnormal LFTs
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PRINCIPLES
2.5% of population have raised LFTs
Normal LFTs do not exclude liver disease
Interpret LFTs in clinical context
Take a careful history for risk factors, drugs, alcohol, comorbidity, autoimmunity
Physical examination for liver disease
Chase likely diagnosis rather than follow algorithm unless there are no clues If mild abnormalities and no risk factors or suggestion of serious liver disease , repeat LFTs after an interval (with lifestyle modification) Synthetic impairment/ signs of decompensation
URGENT evaluation
Acute hepatitis (ALT>10xULN)
• Viral
• Drugs/ Toxic
• Ischemia
• Autoimmune
Investigation of acute hepatitis
• Urgent evaluation especially if jaundiced/ synthetic impairment
• Evaluation RFs viral hepatitis, drug exposure
• Discontinue potential candidate drugs
• Hep A IgM, HBV cIgM + SAg, HCV IgG, HEV IgM
• Ultrsound
Acute alcoholic hepatitis
Spectrum: abnormal LFTs → ACLF
History: malaise, abdo pain anorexia
Examination: PSCLD, Hepatomegaly
Investigations: AST never >10xULN; AST:ALT>2; Bilirubin, PT
• Urgent evaluation if jaundiced
• Steroids/ DF
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ALT/AST 2‐5x ULN
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Transient
Drug effect
Chronic viral hepatitis
Alcohol
NAFLD
Autoimmune
Metabolic liver disease
Common medication •
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Statins
NSAIDs
Antibiotics
Antituberculosis drugs
Herbal remedies
Alternative medications NAFLD
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Hepatic manifestation of metabolic syndrome
Therefore risk factors
ALT, AST 2‐4x ULN
GGT
Fat on USS
Chronic viral hepatitis
• Hepatitis B
Ethnic group, Risks for BBV
HBSAg
• Hepatitis C Blood product transfusion before 1992
IDU
HCV Ab, RNA, genotype
Autoimmune
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Female sex
Young
Previous/ family history AI disease
Elevated globulin/ serum IgG
Positive AAs: ANA, SMA, anti‐LKM
Metabolic liver disease
• Haemochromatosis
Arthralgia, DM
Elevated serum ferritin and TFS genetics
• Wilsons
Young, undiagnosed liver disease
Psychaitric/ Neurologic symptoms
Caeruloplasmin
Cholestasis
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Transient
Drugs
Biliary Obstruction
PBC
PSC
Infiltration
Biliary obstruction
• Gallstones
• Cancer head of pancreas
• Cholangiocacinoma
• Ultrasound CT
Medications  elevation of bilirubin
and ALP
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Anabolic steroid
Allopurinol
Amoxicillin‐clavuronic acid
Captopril
Carbamazepine
Chlorpropamide
Cyproheptadine
Diltiazem
Erythromycin
Estrogens
Floxuridine
Flucloxacillin
Fluphenazine
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Gold salts
Imipramine
Indinavir
Iprindole
Nevirapine
Methytestosterone
Methylenedioxymethamphetamine
Oxaprozin
Pizotyline
Quinidine
Tolbutamide
TPN
Trimethoprim‐sulfamethoxazole
PBC
• Female predominant
• Elevated cholestatic enzymes, no biliary
obstruction, pruritis, xanthelasma
• AMA positive, IgM
PSC
• Young, IBD
• ANCA
• Secondary care evaluation
Diagnostic approach in elevated serum alkaline phosphatase
elevated ALP
History and PE
normal bilirubin, ALT, AST
GGT or 5’nucleotidase
positive
negative
not hepatobiliary
U/S
review medication
AMA
abnormal liver chemistries
yes
Cholangiography
CT
no
AMA
negative
no duct dilatation
liver biopsy
U/S
observation
> 6 months
as elevated ALT evaluation, liver
biopsy, ERCP
γ‐glutamyltransferase (GGT)
• Sensitive but not specific
• increase
– alcohol – drug • anticonvulsant (CBZ, phenytoin, and barbiturate), OC
– almost all type of liver diseases Important points
• Investigate abnormalities in light of clinical context
• Abnormalities associated with synthetic impairment or signs of decompensation require emergent evaluation
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