Gas chromatography-mass spectrometry exhaled breath analysis for phenotyping interstitial lung disease- an exploratory study

Iris G. van der Sar; Iris A. Simons; Roxanne F.G. van Duren; Esther J. Nossent; Marlies S. Wijsenbeek; Jan Willem Duitman; Arlette E. Odink; Lilian J. Meijboom; Catharina C. Moor; Paul Brinkman

doi:10.1088/1752-7163/ae2ef4

Gas chromatography-mass spectrometry exhaled breath analysis for phenotyping interstitial lung disease- an exploratory study

Iris G. van der Sar
, Iris A. Simons
, Roxanne F.G. van Duren
, Esther J. Nossent
, Marlies S. Wijsenbeek
, Jan Willem Duitman
, Arlette E. Odink
, Lilian J. Meijboom
, Catharina C. Moor
, Paul Brinkman

Amsterdam UMC
University of Amsterdam
Erasmus University Rotterdam

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Interstitial lung disease (ILD) encompasses pulmonary disorders characterised by varying degrees of inflammation and/or fibrosis. The presence and extent of these pulmonary abnormalities on (high-resolution) computed tomography (CT) have consequences for diagnosis and treatment; however, inter-observer assessment varies. Analysis of exhaled volatile organic compounds (VOCs) through gas chromatography-mass spectrometry (GC-MS) offers a noninvasive approach to biomarker discovery and pathophysiology understanding. Our study aims to explore the ability of GC-MS-driven exhaled breath analysis to differentiate ILD patients with predominant fibrotic, inflammatory, or a combination of fibrotic and inflammatory pulmonary abnormalities in a training and an external validation cohort. In a multicentre cross-sectional study, patients diagnosed with ILD were recruited. After central review of chest CT scans by independent radiologists, patients were categorised as fibrotic, inflammatory or mixed phenotype group based on the percentage of chest CT scan abnormalities. Breath samples were collected and analysed via GC-MS. Significantly different VOC fragments between groups were selected and used to differentiate groups in the training cohort with sparse partial least squares discriminant analysis. Analyses were validated with patients from an external cohort. 53 patients were included, 21 patients in the fibrotic, 14 in the inflammatory and 18 in the mixed phenotype group. Area under the curve (AUCs) for discrimination between groups ranged from 0.89-1.00 in training cohorts. An attempt to confirm these findings in our external validation cohort resulted in AUCs of 0.63-0.84. Re-evaluation of the training model led to an AUC of 0.78-0.83. This study shows that GC-MS driven exhaled breath analysis towards differentiation of ILD phenotypes is challenging. Current findings emphasise the importance of predefined validation steps during the process of biomarker discovery.

Original language	English
Article number	016005
Journal	JOURNAL OF BREATH RESEARCH
Volume	20
Issue number	1
DOIs	https://doi.org/10.1088/1752-7163/ae2ef4
Publication status	Published - 1 Mar 2026

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van_der_Sar_2026_J._Breath_Res._20_016005Final published version, 840 KBLicence: CC BY

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van der Sar, I. G., Simons, I. A., van Duren, R. F. G., Nossent, E. J., Wijsenbeek, M. S., Duitman, J. W., Odink, A. E., Meijboom, L. J., Moor, C. C., & Brinkman, P. (2026). Gas chromatography-mass spectrometry exhaled breath analysis for phenotyping interstitial lung disease- an exploratory study. JOURNAL OF BREATH RESEARCH, 20(1), Article 016005. https://doi.org/10.1088/1752-7163/ae2ef4

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title = "Gas chromatography-mass spectrometry exhaled breath analysis for phenotyping interstitial lung disease- an exploratory study",

abstract = "Interstitial lung disease (ILD) encompasses pulmonary disorders characterised by varying degrees of inflammation and/or fibrosis. The presence and extent of these pulmonary abnormalities on (high-resolution) computed tomography (CT) have consequences for diagnosis and treatment; however, inter-observer assessment varies. Analysis of exhaled volatile organic compounds (VOCs) through gas chromatography-mass spectrometry (GC-MS) offers a noninvasive approach to biomarker discovery and pathophysiology understanding. Our study aims to explore the ability of GC-MS-driven exhaled breath analysis to differentiate ILD patients with predominant fibrotic, inflammatory, or a combination of fibrotic and inflammatory pulmonary abnormalities in a training and an external validation cohort. In a multicentre cross-sectional study, patients diagnosed with ILD were recruited. After central review of chest CT scans by independent radiologists, patients were categorised as fibrotic, inflammatory or mixed phenotype group based on the percentage of chest CT scan abnormalities. Breath samples were collected and analysed via GC-MS. Significantly different VOC fragments between groups were selected and used to differentiate groups in the training cohort with sparse partial least squares discriminant analysis. Analyses were validated with patients from an external cohort. 53 patients were included, 21 patients in the fibrotic, 14 in the inflammatory and 18 in the mixed phenotype group. Area under the curve (AUCs) for discrimination between groups ranged from 0.89-1.00 in training cohorts. An attempt to confirm these findings in our external validation cohort resulted in AUCs of 0.63-0.84. Re-evaluation of the training model led to an AUC of 0.78-0.83. This study shows that GC-MS driven exhaled breath analysis towards differentiation of ILD phenotypes is challenging. Current findings emphasise the importance of predefined validation steps during the process of biomarker discovery.",

author = "\{van der Sar\}, \{Iris G.\} and Simons, \{Iris A.\} and \{van Duren\}, \{Roxanne F.G.\} and Nossent, \{Esther J.\} and Wijsenbeek, \{Marlies S.\} and Duitman, \{Jan Willem\} and Odink, \{Arlette E.\} and Meijboom, \{Lilian J.\} and Moor, \{Catharina C.\} and Paul Brinkman",

note = "Publisher Copyright: Creative Commons Attribution license.",

year = "2026",

month = mar,

day = "1",

doi = "10.1088/1752-7163/ae2ef4",

language = "English",

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T1 - Gas chromatography-mass spectrometry exhaled breath analysis for phenotyping interstitial lung disease- an exploratory study

AU - van der Sar, Iris G.

AU - Simons, Iris A.

AU - van Duren, Roxanne F.G.

AU - Nossent, Esther J.

AU - Wijsenbeek, Marlies S.

AU - Duitman, Jan Willem

AU - Odink, Arlette E.

AU - Meijboom, Lilian J.

AU - Moor, Catharina C.

AU - Brinkman, Paul

N1 - Publisher Copyright: Creative Commons Attribution license.

PY - 2026/3/1

Y1 - 2026/3/1

N2 - Interstitial lung disease (ILD) encompasses pulmonary disorders characterised by varying degrees of inflammation and/or fibrosis. The presence and extent of these pulmonary abnormalities on (high-resolution) computed tomography (CT) have consequences for diagnosis and treatment; however, inter-observer assessment varies. Analysis of exhaled volatile organic compounds (VOCs) through gas chromatography-mass spectrometry (GC-MS) offers a noninvasive approach to biomarker discovery and pathophysiology understanding. Our study aims to explore the ability of GC-MS-driven exhaled breath analysis to differentiate ILD patients with predominant fibrotic, inflammatory, or a combination of fibrotic and inflammatory pulmonary abnormalities in a training and an external validation cohort. In a multicentre cross-sectional study, patients diagnosed with ILD were recruited. After central review of chest CT scans by independent radiologists, patients were categorised as fibrotic, inflammatory or mixed phenotype group based on the percentage of chest CT scan abnormalities. Breath samples were collected and analysed via GC-MS. Significantly different VOC fragments between groups were selected and used to differentiate groups in the training cohort with sparse partial least squares discriminant analysis. Analyses were validated with patients from an external cohort. 53 patients were included, 21 patients in the fibrotic, 14 in the inflammatory and 18 in the mixed phenotype group. Area under the curve (AUCs) for discrimination between groups ranged from 0.89-1.00 in training cohorts. An attempt to confirm these findings in our external validation cohort resulted in AUCs of 0.63-0.84. Re-evaluation of the training model led to an AUC of 0.78-0.83. This study shows that GC-MS driven exhaled breath analysis towards differentiation of ILD phenotypes is challenging. Current findings emphasise the importance of predefined validation steps during the process of biomarker discovery.

AB - Interstitial lung disease (ILD) encompasses pulmonary disorders characterised by varying degrees of inflammation and/or fibrosis. The presence and extent of these pulmonary abnormalities on (high-resolution) computed tomography (CT) have consequences for diagnosis and treatment; however, inter-observer assessment varies. Analysis of exhaled volatile organic compounds (VOCs) through gas chromatography-mass spectrometry (GC-MS) offers a noninvasive approach to biomarker discovery and pathophysiology understanding. Our study aims to explore the ability of GC-MS-driven exhaled breath analysis to differentiate ILD patients with predominant fibrotic, inflammatory, or a combination of fibrotic and inflammatory pulmonary abnormalities in a training and an external validation cohort. In a multicentre cross-sectional study, patients diagnosed with ILD were recruited. After central review of chest CT scans by independent radiologists, patients were categorised as fibrotic, inflammatory or mixed phenotype group based on the percentage of chest CT scan abnormalities. Breath samples were collected and analysed via GC-MS. Significantly different VOC fragments between groups were selected and used to differentiate groups in the training cohort with sparse partial least squares discriminant analysis. Analyses were validated with patients from an external cohort. 53 patients were included, 21 patients in the fibrotic, 14 in the inflammatory and 18 in the mixed phenotype group. Area under the curve (AUCs) for discrimination between groups ranged from 0.89-1.00 in training cohorts. An attempt to confirm these findings in our external validation cohort resulted in AUCs of 0.63-0.84. Re-evaluation of the training model led to an AUC of 0.78-0.83. This study shows that GC-MS driven exhaled breath analysis towards differentiation of ILD phenotypes is challenging. Current findings emphasise the importance of predefined validation steps during the process of biomarker discovery.

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DO - 10.1088/1752-7163/ae2ef4

M3 - Article

C2 - 41411683

AN - SCOPUS:105027185721

SN - 1752-7155

VL - 20

JO - JOURNAL OF BREATH RESEARCH

JF - JOURNAL OF BREATH RESEARCH

IS - 1

M1 - 016005

ER -

Gas chromatography-mass spectrometry exhaled breath analysis for phenotyping interstitial lung disease- an exploratory study

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