Connective Tissue-Activating Peptide III: A Novel Blood Biomarker for Early Lung Cancer Detection

Author:

Yee John1,Sadar Marianne D.1,Sin Don D.1,Kuzyk Michael1,Xing Li1,Kondra Jennifer1,McWilliams Annette1,Man S.F. Paul1,Lam Stephen1

Affiliation:

1. From the Division of Thoracic Surgery, Vancouver General Hospital, the University of British Columbia; Genome Science Centre and the Cancer Imaging Department, British Columbia Cancer Agency & the University of British Columbia; The James Hogg iCapture Centre & the Heart and Lung Institute at St Paul's Hospital; and the Department of Medicine, Respiratory Division, University of British Columbia, Vancouver, British Columbia, Canada.

Abstract

PurposeThere are no reliable blood biomarkers to detect early lung cancer. We used a novel strategy that allows discovery of differentially present proteins against a complex and variable background.MethodsMass spectrometry analyses of paired pulmonary venous-radial arterial blood from 16 lung cancer patients were applied to identify plasma proteins potentially derived from the tumor microenvironment. Two differentially expressed proteins were confirmed in 64 paired venous-arterial blood samples using an immunoassay. Twenty-eight pre- and postsurgical resection peripheral blood samples and two independent, blinded sets of plasma from 149 participants in a lung cancer screening study (49 lung cancers and 100 controls) and 266 participants from the National Heart Lung and Blood Institute Lung Health Study (45 lung cancer and 221 matched controls) determined the accuracy of the two protein markers to detect subclinical lung cancer.ResultsConnective tissue-activating peptide III (CTAP III)/ neutrophil activating protein-2 (NAP-2) and haptoglobin were identified to be significantly higher in venous than in arterial blood. CTAP III/NAP-2 levels decreased after tumor resection (P = .01). In two independent population cohorts, CTAP III/NAP-2 was significantly associated with lung cancer and improved the accuracy of a lung cancer risk prediction model that included age, smoking, lung function (FEV1), and an interaction term between FEV1and CTAP III/NAP-2 (area under the curve, 0.84; 95% CI, 0.77 to 0.91) compared to CAPIII/NAP-2 alone.ConclusionWe identified CTAP III/NAP-2 as a novel biomarker to detect preclinical lung cancer. The study underscores the importance of applying blood biomarkers as part of a multimodal lung cancer risk prediction model instead of as stand-alone tests.

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

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