Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed

Background: Dubin-Johnson syndrome (DJS) presents during the neonatal period with a phenotype that overlaps with a broad list of causes of neonatal cholestasis (NC), which makes the identification of DJS challenging for clinicians. We conducted a case-controlled study to investigate the utility of...

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Main Authors: Abdulrahman Al-Hussaini, Ali Asery, Omar Alharbi
Format: Article
Language:English
Published: Wolters Kluwer Medknow Publications 2023-01-01
Series:The Saudi Journal of Gastroenterology
Subjects:
Online Access:http://www.saudijgastro.com/article.asp?issn=1319-3767;year=2023;volume=29;issue=3;spage=183;epage=190;aulast=
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author Abdulrahman Al-Hussaini
Ali Asery
Omar Alharbi
author_facet Abdulrahman Al-Hussaini
Ali Asery
Omar Alharbi
author_sort Abdulrahman Al-Hussaini
collection DOAJ
description Background: Dubin-Johnson syndrome (DJS) presents during the neonatal period with a phenotype that overlaps with a broad list of causes of neonatal cholestasis (NC), which makes the identification of DJS challenging for clinicians. We conducted a case-controlled study to investigate the utility of urinary coproporphyrins (UCP) I% as a potential diagnostic biomarker. Methods: We reviewed our database of 533 cases of NC and identified 28 neonates with disease-causing variants in ATP-binding cassette-subfamily C member 2 (ABCC2) gene “Cases” (Study period 2008–2019). Another 20 neonates with cholestasis due to non-DJS diagnoses were included as “controls.” Both groups underwent UCP analysis to measure CP isomer I percentage (%). Results: Serum alanine aminotransferase (ALT) levels were within the normal range in 26 patients (92%) and mildly elevated in 2 patients. ALT levels were significantly lower in neonates with DJS than in NC from other causes (P < 0.001). The use of normal serum ALT levels to predict DJS among neonates with cholestasis had a sensitivity of 93%, specificity 90%, positive predictive value (PPV) 34%, and negative predictive value (NPV) 99.5%. The median UCPI% was significantly higher in DJS patients [88%, interquartile range (IQR) 1–IQR3, 84.2%–92.7%] than in NC from other causes [67%, (IQR1–IQR3, 61%–71.5%; Confidence interval 0.18–0.28; P< 0.001)]. The use of UCPI% >80% to predict DJS had a sensitivity, specificity, PPV, and NPV of 100%. Conclusion: Based on the results from our study, we propose sequencing of the ABCC2 gene in neonates with normal ALT, presence of cholestasis and UCP1% >80%.
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spelling doaj.art-89382e729da044ccb0ec8a9011396db32023-07-23T16:14:07ZengWolters Kluwer Medknow PublicationsThe Saudi Journal of Gastroenterology1319-37671998-40492023-01-0129318319010.4103/sjg.sjg_480_22Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposedAbdulrahman Al-HussainiAli AseryOmar AlharbiBackground: Dubin-Johnson syndrome (DJS) presents during the neonatal period with a phenotype that overlaps with a broad list of causes of neonatal cholestasis (NC), which makes the identification of DJS challenging for clinicians. We conducted a case-controlled study to investigate the utility of urinary coproporphyrins (UCP) I% as a potential diagnostic biomarker. Methods: We reviewed our database of 533 cases of NC and identified 28 neonates with disease-causing variants in ATP-binding cassette-subfamily C member 2 (ABCC2) gene “Cases” (Study period 2008–2019). Another 20 neonates with cholestasis due to non-DJS diagnoses were included as “controls.” Both groups underwent UCP analysis to measure CP isomer I percentage (%). Results: Serum alanine aminotransferase (ALT) levels were within the normal range in 26 patients (92%) and mildly elevated in 2 patients. ALT levels were significantly lower in neonates with DJS than in NC from other causes (P < 0.001). The use of normal serum ALT levels to predict DJS among neonates with cholestasis had a sensitivity of 93%, specificity 90%, positive predictive value (PPV) 34%, and negative predictive value (NPV) 99.5%. The median UCPI% was significantly higher in DJS patients [88%, interquartile range (IQR) 1–IQR3, 84.2%–92.7%] than in NC from other causes [67%, (IQR1–IQR3, 61%–71.5%; Confidence interval 0.18–0.28; P< 0.001)]. The use of UCPI% >80% to predict DJS had a sensitivity, specificity, PPV, and NPV of 100%. Conclusion: Based on the results from our study, we propose sequencing of the ABCC2 gene in neonates with normal ALT, presence of cholestasis and UCP1% >80%.http://www.saudijgastro.com/article.asp?issn=1319-3767;year=2023;volume=29;issue=3;spage=183;epage=190;aulast=abcc2genedubin-johnson syndromeneonatal cholestasissaudi arabiaurinary coproporphyrins
spellingShingle Abdulrahman Al-Hussaini
Ali Asery
Omar Alharbi
Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed
The Saudi Journal of Gastroenterology
abcc2gene
dubin-johnson syndrome
neonatal cholestasis
saudi arabia
urinary coproporphyrins
title Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed
title_full Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed
title_fullStr Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed
title_full_unstemmed Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed
title_short Urinary coproporphyrins as a diagnostic biomarker of Dubin-Johnson syndrome in neonates: A diagnostic pathway is proposed
title_sort urinary coproporphyrins as a diagnostic biomarker of dubin johnson syndrome in neonates a diagnostic pathway is proposed
topic abcc2gene
dubin-johnson syndrome
neonatal cholestasis
saudi arabia
urinary coproporphyrins
url http://www.saudijgastro.com/article.asp?issn=1319-3767;year=2023;volume=29;issue=3;spage=183;epage=190;aulast=
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AT aliasery urinarycoproporphyrinsasadiagnosticbiomarkerofdubinjohnsonsyndromeinneonatesadiagnosticpathwayisproposed
AT omaralharbi urinarycoproporphyrinsasadiagnosticbiomarkerofdubinjohnsonsyndromeinneonatesadiagnosticpathwayisproposed