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MLAB 2401: Clinical Chemistry Keri Brophy-Martinez

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Jendrassik-Grof Advantages Not affected by pH changes Maintains optical sensitivity at low bilirubin concentrations ... product of bilirubin metabolism ... – PowerPoint PPT presentation

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Title: MLAB 2401: Clinical Chemistry Keri Brophy-Martinez


1
MLAB 2401 Clinical ChemistryKeri Brophy-Martinez
  • Assessment of Liver Function

2
Liver Panel
  • Albumin
  • Bilirubin, total
  • Bilirubin, direct
  • AST/SGOT
  • ALT/SGPT
  • Alkaline Phosphatase

3
History of Bilirubin Analysis
  • Ehrlich(1883)
  • Described the reaction of bilirubin with
    diazotized sulfanilic acid DIAZO REACTION
  • Malloy and Evelyn (1937)
  • Diazo reaction with 50 methanol as an
    accelerator
  • Jendrassik and Grof ( 1938)
  • Diazo reaction with caffeine-benzoate-acetate as
    accelerator
  • Increased sensitivity

4
Measured vs. Calculated
  • Measured Analytes
  • Total Bilirubin
  • Conjugated bilirubin (DIRECT)
  • Calculated Analytes
  • Unconjugated bilirubin (INDIRECT)

5
Fractions Their Characteristics
  • Conjugated/Direct
  • Polar
  • Water-soluble
  • Found in plasma, unbound or free
  • Reacts with diazotized sulfanilic acid without an
    accelerator
  • Unconjugated/Indirect
  • Nonpolar
  • Water-insoluble
  • Found in plasma, bound to albumin
  • Reacts with diazotized sulfanilic acid with an
    accelerator
  • Delta
  • Conjugated bilirubin bound to albumin
  • Observed in hepatic obstructions

6
Specimen Collection and Storage
  • Serum or plasma preferred
  • Temperature sensitive
  • Fasting sample preferred
  • Lipemia increases bilirubin concentrations
  • No hemolysis
  • Hemolysis decreases the reaction of bilirubin
    with the diazo reagent
  • Light sensitive
  • Bilirubin levels decrease by 30-50 per hour.

7
Methods of Bilirubin Analysis
  • Jendrassik-Grof
  • Measures Total and Conjugated bilirubin
  • Principle
  • Bilirubin pigments in serum react with a diazo
    reagent which results in the production of
    azobilirubin( a purple product). Measured at 540
    nm.
  • Caffeine -benzoate accerlerates the coupling of
    bilirubin with the diazo reagent.
  • Ascorbic acid stops the reaction.
  • Alkaline tartrate converts the purple
    azobilirubin to a blue azobilirubin.
  • This product is measured spectrophotometrically _at_
    600 nm.

8
Jendrassik-Grof
  • Advantages
  • Not affected by pH changes
  • Maintains optical sensitivity at low bilirubin
    concentrations
  • Insensitive to high protein concentrations
  • Jendrassik-Grof Animation
  • http//webcls.utmb.edu/lo/publicdl.asp?616404F6782
    E84851260BFF8F344F92903AF

9
Reference Ranges for Bilirubin
10
Urine Bilirubin
  • Presence indicates conjugated hyperbilirubinemia
  • Detected using urine dipsticks
  • Have a diazo reagent imbedded in the strip
  • Follows the Ehrlich principle
  • (Chemstrip/Multistix)
  • Fresh urine should be used
  • Avoid light and oxidation

11
Urobilinogen
  • End product of bilirubin metabolism
  • Majority excreted in feces, some reabsorbed and
    returned to the liver
  • Increased
  • Hemolytic disease
  • Defective liver-cell function
  • Decreased
  • Biliary obstruction
  • Carcinoma

12
Determination of Urobilinogen
  • Ehrlichs reaction
  • Ehrlichs reagentp-dimethyl aminobenzaldehyde
  • Urobilinogen Ehrlichs reagent Red color
  • Performed on fresh urine
  • Reference Range
  • 0.1-1.0 Ehrlich units in two hours

13
Enzymes
  • Liver damage results in the release of enzymes
    into the circulation
  • Differentiate between functional or mechanical
    causes of disease
  • Significant enzymes
  • AST
  • ALT
  • ALP
  • GGT
  • 5 nucleotidase
  • LDH

14
Enzymes
  • Aminotransferases
  • ALT and AST rise rapidly in most diseases of the
    liver and stay elevated for up to 2-6 weeks
  • Highest levels seen with hepatitis, hepatic
    ischemia and drug/toxin-induced necrosis
  • Phosphatases
  • ALP differentiates hepatobiliary disease from
    bone disease
  • 5-Nucleotidase is elevated in hepatobiliary
    disease

15
Enzymes
  • GGT elevated in biliary obstruction and in
    chronic alcoholism
  • LDH/LD serves as a nonspecific marker of cellular
    injury

16
Enzymes Points to Remember
  • Elevated Liver enzymes are as easy as ABC
  • Alcoholism
  • Biliary Obstruction
  • Cirrhosis

17
Misc. Liver Function Tests
  • Prothrombin time
  • Elevated in liver disease
  • Ammonia
  • Elevated in liver disease
  • Glucose/Galactose Tolerance
  • Assess the livers ability to metabolize
    carbohydrates

18
Disease States
Condition AST ALT ALP GGT Albumin
Alcoholic hepatits I I NI III N
Acute Hepatitis III II I I N
Biliary Obstruction NI NI I I I
Cirrhosis NI NI NI NI D
Reyes Syndrome I I N
I Increased N Normal
19
Hepatitis A Markers
  • Performed by serological antibodies
  • IgM indicates acute infection and can persist for
    3-6 months
  • IgG appears shortly after IgM, and confers
    lifelong immunity.

20
Hepatitis B Markers
  • HBsAG Hepatitis B Surface Antigen
  • Detected prior to onset of symptoms
  • HBcAG Hepatitis B Core Antigen
  • Found in an acute infection
  • HBeAg Hepatitis B Envelope Antigen
  • Found in acute and chronic infections

21
Hepatitis B Virus
22
Hepatitis C Testing
  • Two methods currently used
  • Anti-HCV detection by EIA (Screen)
  • A positive test indicates exposure to HCV, it can
    not determine a current infection versus a past
    infection
  • Quantitative nucleic acid PCR for HCV RNA
    (Confirmatory)

23
References
  • Bishop, M., Fody, E., Schoeff, l. (2010).
    Clinical Chemistry Techniques, principles,
    Correlations. Baltimore Wolters Kluwer
    Lippincott Williams Wilkins.
  • http//www.abbottdiagnostics.co.uk/About_Us/UK/hep
    atitis_antigen.cfm
  • http//depts.washington.edu/labweb/Divisions/Viro/
    Hepatitis_sero.htm
  • http//tmp.kiwix.org4201/A/Hepatitis_B.html
  • Sunheimer, R., Graves, L. (2010). Clinical
    Laboratory Chemistry. Upper Saddle River Pearson
    .
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