K H Brandt scite author profile

SUMMARY Samples of serum, bile, and urine were collected simultaneously from patients with cholestasis of varying aetiology and from patients with cirrhosis; their bile acid composition was determined by gas/liquid chromatography and mass spectrometry In cholestasis, the patterns in all three body fluids differed consistently and strikingly. In serum, cholic acid was the major bile acid and most bile acids (> 93 %) were unsulphated, whereas, in urine, chenodeoxycholic was the major bile acid, and the majority of bile acids (> 60 %) were sulphated. Secondary bile acids were virtually absent in bile, serum, and urine. The total amount of bile acids excreted for 24 hours correlated highly with the concentration of serum bile acids; in patients with complete obstruction, urinary excretion averaged 71 6 mg/24 h. In cirrhotic patients, serum bile acids were less raised, and chenodeoxycholic acid was the predominant acid. In healthy controls, serum bile acids were consistently richer in chenodeoxycholic acid than biliary bile acids, and no bile acids were present in urine. No unusual monohydroxy bile acids were present in patients with primary biliary cirrhosis, but, in several patients, there was a considerable amount of hyocholic acid present in the urinary bile acids. The analyses of individual bile acids in serum and urine did not appear to provide helpful information in the differential diagnosis of cholestasis. Thus, in cholestasis, conjugation of chenodeoxycholic acid with sulphate becomes a major biochemical pathway, urine becomes a major route of bile acid excretion, and abnormal bile acids are formed.

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Detection and significance of anti-HBc in the blood bank; preliminary results of a controlled prospective study

Katchaki¹,

Siem²,

Brouwer

et al. 1980

Journal of Virological Methods

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Quantitative analysis of bile acids in serum and bile, using gas -liquid chromatography

Henegouwen

Ruben

Brandt

1974

Clinica Chimica Acta

110

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Low therapeutic value of D‐penicillamine in a short‐term prospective trial in primary biliary cirrhosis

Taal¹,

Schalm²,

Kate³

et al. 1983

Liver

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A small double-blind controlled trial to evaluate the short-term effects of D-penicillamine therapy was carried out in 24 patients with primary biliary cirrhosis (PBC). The daily dose of D-penicillamine was increased monthly by 250 mg until a total of 1 g daily was reached. Two out of 11 patients (18%) were withdrawn because of side-effects, as also were 4 out of 13 (31%) patients receiving the placebo. Transient improvement in symptoms was observed in 4of 11 patients on D-penicillamine, but also in 5 of 13 patients from the placebo group. The proportion of patients showing a fall in serum IgM, IgG and hepatic copper was significantly larger for the D-penicillamine group than for the placebo group. No improvement in liver tests was observed, but the progression of inflammatory periportal liver cell destruction (piecemeal necrosis) was retarded in patients on D-penicillamine @=0.02). Data analysis within the Dpenicillamine group showed that lowering the dose of D-penicillamine to 500 mg daily abolished the effect on the serum immunoglobulins and hepatic copper. The beneficial effect of D-penicillamine therapy appears to be small and doserelated; side effects should not prevent its use, provided the drug is introduced slowly.

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Is an Acute Disturbance in Hepatic Transport of Bile-Acids the Primary Cause of Cholestasis in Benign Recurrent Intrahepatic Cholestasis?

1974

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K H Brandt

Sulphated and unsulphated bile acids in serum, bile, and urine of patients with cholestasis.

Detection and significance of anti-HBc in the blood bank; preliminary results of a controlled prospective study

Quantitative analysis of bile acids in serum and bile, using gas -liquid chromatography

Low therapeutic value of D‐penicillamine in a short‐term prospective trial in primary biliary cirrhosis

Is an Acute Disturbance in Hepatic Transport of Bile-Acids the Primary Cause of Cholestasis in Benign Recurrent Intrahepatic Cholestasis?

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