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Multicenter Study
. 2022 Nov;163(5):1407-1422.
doi: 10.1053/j.gastro.2022.07.047. Epub 2022 Jul 21.

Independent Validation and Assay Standardization of Improved Metabolic Biomarker Signature to Differentiate Pancreatic Ductal Adenocarcinoma From Chronic Pancreatitis

Ujjwal M Mahajan  1 Bettina Oehrle  1 Simon Sirtl  1 Ahmed Alnatsha  1 Elisabetta Goni  1 Ivonne Regel  1 Georg Beyer  1 Marlies Vornhülz  1 Jakob Vielhauer  1 Ansgar Chromik  2 Markus Bahra  3 Fritz Klein  4 Waldemar Uhl  5 Tim Fahlbusch  5 Marius Distler  6 Jürgen Weitz  6 Robert Grützmann  7 Christian Pilarsky  7 Frank Ulrich Weiss  8 M Gordian Adam  9 John P Neoptolemos  10 Holger Kalthoff  11 Roland Rad  12 Nicole Christiansen  13 Bianca Bethan  14 Beate Kamlage  14 Markus M Lerch  15 Julia Mayerle  16
Affiliations
Multicenter Study

Independent Validation and Assay Standardization of Improved Metabolic Biomarker Signature to Differentiate Pancreatic Ductal Adenocarcinoma From Chronic Pancreatitis

Ujjwal M Mahajan et al. Gastroenterology. 2022 Nov.

Abstract

Background & aims: Pancreatic ductal adenocarcinoma cancer (PDAC) is a highly lethal malignancy requiring efficient detection when the primary tumor is still resectable. We previously developed the MxPancreasScore comprising 9 analytes and serum carbohydrate antigen 19-9 (CA19-9), achieving an accuracy of 90.6%. The necessity for 5 different analytical platforms and multiple analytical runs, however, hindered clinical applicability. We therefore aimed to develop a simpler single-analytical run, single-platform diagnostic signature.

Methods: We evaluated 941 patients (PDAC, 356; chronic pancreatitis [CP], 304; nonpancreatic disease, 281) in 3 multicenter independent tests, and identification (ID) and validation cohort 1 (VD1) and 2 (VD2) were evaluated. Targeted quantitative plasma metabolite analysis was performed on a liquid chromatography-tandem mass spectrometry platform. A machine learning-aided algorithm identified an improved (i-Metabolic) and minimalistic metabolic (m-Metabolic) signatures, and compared them for performance.

Results: The i-Metabolic Signature, (12 analytes plus CA19-9) distinguished PDAC from CP with area under the curve (95% confidence interval) of 97.2% (97.1%-97.3%), 93.5% (93.4%-93.7%), and 92.2% (92.1%-92.3%) in the ID, VD1, and VD2 cohorts, respectively. In the VD2 cohort, the m-Metabolic signature (4 analytes plus CA19-9) discriminated PDAC from CP with a sensitivity of 77.3% and specificity of 89.6%, with an overall accuracy of 82.4%. For the subset of 45 patients with PDAC with resectable stages IA-IIB tumors, the sensitivity, specificity, and accuracy were 73.2%, 89.6%, and 82.7%, respectively; for those with detectable CA19-9 >2 U/mL, 81.6%, 88.7%, and 84.5%, respectively; and for those with CA19-9 <37 U/mL, 39.7%, 94.1%, and 76.3%, respectively.

Conclusions: The single-platform, single-run, m-Metabolic signature of just 4 metabolites used in combination with serum CA19-9 levels is an innovative accurate diagnostic tool for PDAC at the time of clinical presentation, warranting further large-scale evaluation.

Keywords: CA19-9; Chronic Pancreatitis; Diagnostic Signature; Metabolic Signature; Pancreatic Cancer.

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