Clinical development of a blood biomarker using apolipoprotein-A2 isoforms for early detection of pancreatic cancer

Author:

Kashiro Ayumi,Kobayashi Michimoto,Oh Takanori,Miyamoto Mitsuko,Atsumi Jun,Nagashima Kengo,Takeuchi Keiko,Nara Satoshi,Hijioka Susumu,Morizane Chigusa,Kikuchi Shojiro,Kato Shingo,Kato Ken,Ochiai Hiroki,Obata Daisuke,Shizume Yuya,Konishi Hiroshi,Nomura Yumiko,Matsuyama Kotone,Xie Cassie,Wong Christin,Huang Ying,Jung Giman,Srivastava Sudhir,Kutsumi Hiromu,Honda Kazufumi

Abstract

Abstract Background We have previously reported apolipoprotein A2-isoforms (apoA2-is) as candidate plasma biomarkers for early-stage pancreatic cancer. The aim of this study was the clinical development of apoA2-is. Methods We established a new enzyme-linked immunosorbent sandwich assay for apoA2-is under the Japanese medical device Quality Management System requirements and performed in vitro diagnostic tests with prespecified end points using 2732 plasma samples. The clinical equivalence and significance of apoA2-is were compared with CA19-9. Results The point estimate of the area under the curve to distinguish between pancreatic cancer (n = 106) and healthy controls (n = 106) was higher for apoA2-ATQ/AT [0.879, 95% confidence interval (CI): 0.832–0.925] than for CA19-9 (0.849, 95% CI 0.793–0.905) and achieved the primary end point. The cutoff apoA2-ATQ/AT of 59.5 μg/mL was defined based on a specificity of 95% in 2000 healthy samples, and the reliability of specificities was confirmed in two independent healthy cohorts as 95.3% (n = 106, 95% CI 89.4–98.0%) and 95.8% (n = 400, 95% CI 93.3–97.3%). The sensitivities of apoA2-ATQ/AT for detecting both stage I (47.4%) and I/II (50%) pancreatic cancers were higher than those of CA19-9 (36.8% and 46.7%, respectively). The combination of apoA2-ATQ/AT (cutoff, 59.5 μg/mL) and CA19-9 (37 U/mL) increased the sensitivity for pancreatic cancer to 87.7% compared with 69.8% for CA19-9 alone. The clinical performance of apoA2-is was blindly confirmed by the National Cancer Institute Early Detection Research Network. Conclusions The clinical performance of ApoA2-ATQ/AT as a blood biomarker is equivalent to or better than that of CA19-9.

Funder

Japan

Publisher

Springer Science and Business Media LLC

Subject

Gastroenterology

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