Paper

Screening of newborn infants for cholestatic hepatobiliary disease with tandem mass spectrometryCommentary: What is tandem mass spectrometry?

BMJ 1999; 319 doi: 10.1136/bmj.319.7208.471 (Published 21 August 1999)
Cite this as: BMJ 1999;319:471
  1. Imran Mushtaq, research fellowa,
  2. Stuart Logan, senior lecturer in epidemiologyb,
  3. Michael Morris, chemist (mass spectrometry applications)c,
  4. Andrew W Johnson, senior lecturer in biochemistrya,
  5. Angie M Wade, lecturer in medical statisticsb,
  6. Deirdre Kelly, consultant paediatric hepatologistd,
  7. Peter T Clayton, professor of paediatric metabolic disease and hepatologya (P.Clayton{at}ich.ucl.ac.uk)
  1. a Biochemistry Unit, Institute of Child Health, University College London, London WC1N 1EH
  2. b Epidemiology and Biostatistics Unit, Institute of Child Health
  3. c Micromass UK Limited, Wythenshawe, Manchester M23 9LZ
  4. d Liver Unit, Birmingham Children's Hospital, Ladywood Middleway, Ladywood, Birmingham B16 8ET
  1. Correspondence to: P T Clayton
  • Accepted 12 May 1999

Abstract

Objective: To assess the feasibility of screening for cholestatic hepatobiliary disease and extrahepatic biliary atresia by using tandem mass spectrometry to measure conjugated bile acids in dried blood spots obtained from newborn infants at 7-10 days of age for the Guthrie test.

Setting: Three tertiary referral clinics and regional neonatal screening laboratories.

Design: Unused blood spots from the Guthrie test were retrieved for infants presenting with cholestatic hepatobiliary disease and from the two cards stored on either side of each card from an index child. Concentrations of conjugated bile acids measured by tandem mass spectrometry in the two groups were compared.

Main outcome measures: Concentrations of glycodihydroxycholanoates, glycotrihydroxycholanoates, taurodihydroxycholanoates, and taurotrihydroxycholanoates. Receiver operator curves were plotted to determine which parameter (or combination of parameters) would best predict the cases of cholestatic hepatobiliary disease and extrahepatic biliary atresia. The sensitivity and specificity at a selection of cut off values for each bile acid species and for total bile acid concentrations for the detection of the two conditions were calculated.

Results: 218 children with cholestatic hepatobiliary disease were eligible for inclusion in the study. Two children without a final diagnosis and five who presented at <14 days of age were excluded. Usable blood spots were obtained from 177 index children and 708 comparison children. Mean concentrations of all four bile acid species were significantly raised in children with cholestatic hepatobiliary disease and extrahepatic biliary atresia compared with the unaffected children (P<0.0001). Of 177 children with cholestatic hepatobiliary disease, 104 (59%) had a total bile acid concentration >33 μmol/l (97.5th centile value for comparison group). Of the 61 with extrahepatic biliary atresia, 47 (77%) had total bile acid concentrations >33 μmol/l Taurotrihydroxycholanoate and total bile acid concentrations were the best predictors of both conditions. For all cholestatic hepatobiliary disease, a cut off level of total bile acid concentration of 30 μmol/l gave a sensitivity of 62% and a specificity of 96%, while the corresponding values for extrahepatic biliary atresia were 79% and 96%.

Conclusion: Most children who present with extrahepatic biliary atresia and other forms of cholestatic hepatobiliary disease have significantly raised concentrations of conjugated bile acids as measured by tandem mass spectrometry at the time when samples are taken for the Guthrie test. Unfortunately the separation between the concentrations in these infants and those in the general population is not sufficient to make mass screening for cholestatic hepatobiliary disease a feasible option with this method alone.

Key messages

  • The prognosis of cholestatic hepatobiliary disease in infancy, in particular biliary atresia, is improved by early detection

  • Infants destined to present with cholestatic jaundice in the first few months of life have raised concentrations of bile acids in the blood spots obtained at 7-10 days for current neonatal screening programmes

  • Tandem mass spectrometry can be used to detect this marker of neonatal cholestasis

  • Unfortunately there is too much overlap between bile acid concentrations in infants with cholestasis and those in control infants for this to be used as a single screening test for cholestatic hepatobiliary disease in general and biliary atresia

  • Tandem mass spectrometry is a powerful tool for neonatal screening but every potential application must be carefully assessed

Footnotes

  • Funding Children's Liver Disease Foundation; Mr David Drake, consultant paediatric surgeon (personal donation); EPSRC (Link scheme).

  • Competing interests None declared.

  • Accepted 12 May 1999

Commentary: What is tandem mass spectrometry?

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