Liver Function Tests PDF
Liver Function Tests PDF
Liver Function Tests PDF
&
Abstract:
Laboratory liver tests are broadly defined as tests useful in the evaluation and treatment of patients
with hepatic dysfunction. The liver carries out metabolism of carbohydrate, protein and fats. Some of
the enzymes and the end products of the metabolic pathway which are very sensitive for the
abnormality occurred may be considered as biochemical marker of liver dysfunction. Some of the
biochemical markers such as serum bilirubin, alanine amino transferase, aspartate amino transferase,
ratio of aminotransferases, alkaline phosphatase, gamma glutamyl transferase, 5 nucleotidase,
ceruloplasmin, -fetoprotein are considered in this article. An isolated or conjugated alteration of
biochemical markers of liver damage in patients can challenge the clinicians during the diagnosis of
disease related to liver directly or with some other organs. The term liver chemistry tests is a
frequently used but poorly defined phrase that encompasses the numerous serum chemistries that
can be assayed to assess hepatic function and/or injury.
Key words: Laboratory liver test, bilirubin, alanine amino transferase, aspartate amino transferase,
ratio of aminotransferases, alkaline phosphatase, gamma glutamyl transferase, 5 nucleotidase,
ceruloplasmin, -fetoprotein
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Serum Bilirubin
Bilirubin is the catabolic product of haemoglobin produced within the reticuloendothelial system,
released in unconjugated form which enters into the liver, converted to conjugated forms bilirubin
mono and diglucuronides by the enzyme UDP-glucuronyltransferase [1]. Normal serum total bilirubin
varies from 2 to 21mol/L. The indirect (unconjugated) bilirubin level is less than 12mol/L and direct
(conjugated) bilirubin less than 8mol/L [2]. The serum bilirubin levels more than 17mol/L suggest
liver diseases and levels above 24mol/L indicate abnormal laboratory liver tests [3, 4]. Jaundice
occurs when bilirubin becomes visible within the sclera, skin, and mucous membranes at a blood
concentration of around 40 mol/L [5]. The occurrence of unconjugated hyperbilirubinemia due to
over production of bilirubin, decreased hepatic uptake or conjugation or both. It is observed in
genetic defect of UDP-glucuronyltransferase causing Gilbert\'s syndrome, Crigler-Najjar syndrome and
reabsorption of large hematomas and ineffective erythropoiesis [6, 7]. In viral hepatitis,
hepatocellular damage, toxic or ischemic liver injury higher levels of serum conjugated bilirubin is
seen. Hyperbilirubinemia in acute viral hepatitis is directly proportional to the degree of histological
injury of hepatocytes and the longer course of the disease [3]. It has been observed that the
decrease of conjugated serum bilirubin is a bimodal fashion when the biliary obstruction is resolved
[8]. Parenchymal liver diseases or incomplete extrahepatic obstruction due to biliary canaliculi give
lower serum bilirubin value than those occur with malignant obstruction of common bile duct but the
level remains normal in infiltrative diseases like tumours and granuloma [9]. Raised Serum bilirubin
from 20.52 mol/L to 143.64mol/L in acute inflammation of appendix has been observed [10]. In
normal asymptomatic pregnant women total and free bilirubin concentrations were significantly lower
during all three trimesters and a decreased conjugated bilirubin was observed in the second and third
trimesters [11]. The recent study has shown that a high serum total bilirubin level may protect
neurologic damage due to stroke [12].
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elevated ALT levels and its specificity to hepatocellular diseases, the absolute peak of the ALT
elevation does not correlate with the extent of liver cell damage [13]. Viral hepatitis like A, B, C, D
and E may be responsible for a marked increase in aminotransferase levels. The increase in ALT
associated with hepatitis C infection tends to be more than that associated with hepatitis A or B [14].
Moreover in patients with acute hepatitis C serum ALT is measured periodically for about 1 to 2 years
[1]. Persistence of elevated ALT for more than six months after an occurrence of acute hepatitis is
used in the diagnosis of chronic hepatitis. Elevation in ALT levels are greater in persons with
nonalcoholic steatohepatitis than in those with uncomplicated hepatic steatosis [15]. In a recent study
the hepatic fat accumulation in childhood obesity and nonalcoholic fatty liver disease causes serum
ALT elevation. Moreover increased ALT level was associated with reduced insulin sensitivity,
adiponectin and glucose tolerance as well as increased free fatty acids and triglycerides [16].
Presence of Bright liver and elevated plasma ALT level was independently associated with increased
risk of the metabolic syndrome in adults [17]. ALT level is normally elevated during 2nd trimester in
asymptomatic normal pregnancy [11]. In one of the study, serum ALT levels in symptomatic pregnant
patients such as in hyperemesis gravidarum was 103.5U/L, in pre-eclampsia patients was 115U/L and
in haemolysis with low platelet count patients showed 149U/L. However in the same study ALT
rapidly drops more than 50% of the elevated values within 3 days indicating the improvement during
postpartum [4]. One of the recent study has shown that coffee and caffeine consumption reduces the
risk of elevated serum ALT activity in excessive alcohol consumption, viral hepatitis, iron overload,
overweight, and impaired glucose metabolism [18].
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AST/ALT ratio
The ratio of AST to ALT has more clinical utility than assessing individual elevated levels. A coenzyme
pyridoxal-5\'-phosphate deficiency may depress serum ALT activity and consequently increases the
AST/ALT ratio [21, 22]. The ratio increases in progressive liver functional impairment and found
81.3% sensitivity and 55.3% specificity in identifying cirrhotic patients [23]. Whereas mean ratio of
1.45 and 1.3 was found in alcoholic liver disease and post necrotic cirrhosis respectively [24]. The
ratio greater than 1.17 was found in one year survival among patients with cirrhosis of viral cause
with 87% sensitivity and 52% specificity [25]. An elevated ratio greater than 1 shows advanced liver
fibrosis and chronic hepatitis C infection [26]. However, an AST/ALT ratio greater than 2
characteristically is present in alcoholic hepatitis. A recent study differentiated nonalcoholic
steatohepatitis (NASH) from alcoholic liver disease showing AST/ALT ratio of 0.9 in NASH and 2.6 in
patients with alcoholic liver disease. A mean ratio of 1.4 was found in patients with cirrhosis related to
NASH [27]. Wilson\'s disease can cause the ratio to exceed 4.5 and similar such altered ratio is found
even in Hyperthyroidism [28, 29].
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and in such situations measurement of gamma glutamyl transferase assists as it is raised only in
cholestatic disorders and not in bone diseases [30].
5 Nucleotidase (NTP)
NTP is a glycoprotein generally disseminated throughout the tissues of the body localised in
cytoplasmic membrane catalyzing release of inorganic phosphate from nucleoside-5-phosphates. The
normal range established is 0 to 15U/L [1]. Raised levels of NTP activity were found in patients with
obstructive jaundice, parenchymal liver disease, hepatic metastases and bone disease [9]. NTP is
precise marker of early hepatic primary or secondary tumours. ALP levels also increased in
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conjugation with NTP showing intra or extra hepatic obstruction due to malignancy [39]. Elevation of
NTP is found in acute infective hepatitis and also in chronic hepatitis [40]. In acute hepatitis elevation
of NTP activity is more when compared with chronic hepatitis and it is attributed to shedding of
plasma membrane with ecto NTP activity due to cell damage, or leakage of bile containing high NTP
activity [41]. Serum NTP activity was slightly but significantly higher in the second and third
trimesters of pregnancy [11].
Ceruloplasmin
Ceruloplasmin is synthesized in the liver and is an acute phase protein. It binds with the copper and
serves as a major carrier for copper in the blood [1]. Normal plasma level of ceruloplasmin is 200 to
600mg/L [2]. The level is elevated in infections, rheumatoid arthritis, pregnancy, non Wilson liver
disease and obstructive jaundice. Low levels may also be seen in neonates, menkes disease,
kwashiorkor, marasmus, protein losing enteropathy, copper deficiency and aceruloplasminemia [3]. In
Wilson\'s disease ceruloplasmin level is depressed. Decreased rate of synthesis of the ceruloplasmin is
responsible for copper accumulation in liver because of copper transport defect in golgi apparatus,
since ATP7B is affected [30]. Serum ceruloplasmin levels were elevated in the chronic active liver
disease (CALD) but lowered in the Wilsons disease (WD). Hence it is the most reliable routine
chemical screening test to differentiate between CALD and WD [42].
-fetoprotein (AFP)
The AFP gene is highly activated in foetal liver but is significantly repressed shortly after birth. The
mechanisms that trigger AFP transcriptional repression in postpartum liver are not properly
understood. AFP is the major serum protein in the developing mammalian foetus produced at high
levels by the foetal liver and visceral endoderm of the yolk sac and at low levels by foetal gut and
kidney. AFP is required for female fertility during embryonic development by protecting the
developing female brain from prenatal exposure to estrogen [43]. In response to liver injury and
during the early stages of chemical hepatocarcinogenesis led to the conclusion that maturation arrest
of liver-determined tissue stem cells give rise to hepatocellular carcinomas [44]. The normal level of
AFP is 0 to 15g/L [2]. An AFP value above 400 - 500g/L has been considered to be diagnostic for
hepatocellular carcinoma (HCC) in patients with cirrhosis. A high AFP concentration 400g/L in HCC
patients is associated with greater tumour size, bilobar involvement, portal vein invasion and a lower
median survival rate [45]. Higher serum AFP levels independently predict a lower sustained virological
response (SVR) rate among patients with chronic hepatitis C [46]. There are three different AFP
variants, differing in their sugar chains (AFP-L1, AFP-L2, AFP-L3). AFP-L1, the non- Lens culinaris
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agglutinin (LCA) -bound fraction, is the main glycoform of AFP in the serum of patients with nonmalignant chronic liver disease. In contrast, Lens culinaris-reactive AFP, also known as AFP-L3, is the
main glycoform of AFP in the serum of HCC patients and it can be detected in approximately one third
of patients with small HCC (< 3 cm), when cut-off values of 10% to 15% are used [47]. AFP-L3 acts
as a marker for clearance of HCC after treatment. It is reported that an AFP-L3 level of 15% or more
is correlated with HCC- associated portal vein invasion [48]. Estimating the AFP-L3 / AFP ratio is
helpful in diagnosis and prognosis of HCC [49]. There is a direct association between secondtrimester maternal serum alpha-fetoprotein levels and the risk of sudden infant death syndrome
(SIDS), which may be mediated in part through impaired foetal growth and preterm birth [50].
Conclusion
Laboratory liver tests help to elucidate the alteration of markers which reflect the liver disease. The
assessment of enzyme abnormalities like, the predominant pattern of enzyme alteration, the
magnitude of enzyme alteration in the case of aminotransferases, isolated elevation or in conjugation
with some other parameter, the rate of change and the nature of the course of alteration or follow up
of 6 months to 1-2 years helps in the diagnosis of the disease. But a single laboratory liver test is of
little value in screening for liver disease as many serious liver diseases may be associated with normal
levels and abnormal levels might be found in asymptomatic healthy individuals. The pattern of
enzyme abnormality, interpreted in the context of the patients symptoms can aid in directing the
subsequent diagnosis.
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List of abbreviations
AFP: -fetoprotein
ALP: Alkaline phosphatase
ALT: Alanine amino transferase
AST: Aspartate amino transferase
CALD: Chronic active liver disease
GGT: Gamma Glutamyl Transferase
HCC: Hepatocellular carcinoma
LCA: Lens culinaris agglutinin
NAHS: Nonalcoholic steatohepatitis
NTP: 5 Nucleotidase
SIDS: Sudden infant death syndrome
SVR: Sustained virological response
UDP: Uridyne diphosphate
WD: Wilsons disease
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