NEW APPROACH TO QUANTITATION OF VARIOUS SOURCES OF BILIRUBIN IN MAN

  • 1 January 1976
    • journal article
    • research article
    • Vol. 87 (5), 767-780
Abstract
Studies of the early labeling of fecal bile pigment have been widely interpreted as indicating that 10-20% of total bile pigment production in normal man is derived from the processes which give rise to the early labeled pigment peak (ELP). This conclusion is based on a very small number of studies with inherent experimental and analytic limitations. A new experimental approach was employed. Plasma bilirubin turnover (BRT), total red blood cell volume (TRCV) and red cell survival were measured in 26 normal volunteers and 35 patients with various hepatic and/or hematologic disorders. The quantity of bilirubin derived from red blood cell degradation (BRRBC) was calculated from TRCV and the mean red cell life-span and the difference between BRT and BRRBC, designated excess bilirubin synthesis (EBS), was considered to represent the quantity of bilirubin derived from the processes responsible for ELP. In normal volunteer subjects, EBS averaged 1.0 mg/kg per day, and accounted for 25% of daily bilirubin turnover. Results derived by this approach exceeded the range estimated from analysis of early labeled peak data. Further analysis of the data in terms of a simple model of bilirubin sources was compatible with the hypothesis that EBS consists of an essentially constant component, averaging 0.8 mg/kg per day, presumably derived principally from the liver, and a 2nd component which varies with the erythropoietic rate. In normal man the liver may contribute the major fraction of EBS.

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