EphA2 Proteolytic Fragment as a Sensitive Diagnostic Biomarker for Very Early-stage Pancreatic Ductal Carcinoma

Author:

Sato Shinya123ORCID,Nakagawa Masatoshi45ORCID,Terashima Takeshi6ORCID,Morinaga Soichiro7ORCID,Miyagi Yohei12ORCID,Yoshida Eisaku3ORCID,Yoshimura Toru3ORCID,Seiki Motoharu8ORCID,Kaneko Shuichi8ORCID,Ueno Makoto9ORCID,Yamashita Taro8ORCID,Koshikawa Naohiko510ORCID

Affiliation:

1. 1Molecular Pathology and Genetics Division, Kanagawa Cancer Center Research Institute, Yokohama, Japan.

2. 2Department of Pathology, Kanagawa Cancer Center Hospital, Yokohama, Japan.

3. 3Morphological Analysis Laboratory, Kanagawa Cancer Center Research Institute, Yokohama, Japan.

4. 4Research and Development, Abbott Japan LLC, Chiba, Japan.

5. 5Department of Life Science and Technology, Tokyo Institute of Technology, Yokohama, Japan.

6. 6Advanced Preventive Medical Sciences Research Center, Kanazawa University Hospital, Kanazawa, Japan.

7. 7Department of Gastroenterological Surgery, Kanagawa Cancer Center Hospital, Yokohama, Japan.

8. 8Graduate School of Medical Sciences, Kanazawa University, Kanazawa, Japan.

9. 9Department of Gastroenterology, Kanagawa Cancer Center Hospital, Yokohama, Japan.

10. 10Clinical Cancer Proteomics Laboratory, Kanagawa Cancer Center Research Institute, Yokohama, Japan.

Abstract

Cleavage of erythropoietin-producing hepatocellular ephrin receptor A2 (EphA2) triggers malignant progression and yields an N-terminal fragment (EphA2-NF) detectable in sera from patients with pancreatic ductal carcinoma. We established a quantitative automated chemiluminescence immunoassay for EphA2-NF and evaluated serum EphA2-NF levels as a biomarker to diagnose pancreatic ductal carcinoma in the test and validation cohorts. The EphA2-NF value was elevated (above the cutoff: mean ± SD) in more than half of the patients with stage I/II pancreatic ductal carcinoma. Among patients receiving standard chemotherapy for pancreatic ductal carcinoma [gemcitabine plus nab-paclitaxel (GnP)], the median survival time of patients with elevated serum EphA2-NF was half that of patients with values below the cutoff. Patients with intraductal papillary mucinous neoplasm (IPMN), a precancerous pancreatic ductal carcinoma lesion, also show high serum EphA2 levels, which are associated with an increase in pancreatic duct size and the development of pancreatic ductal carcinoma in some cases. IHC showed loss of EphA2-NF staining in IPMN with pancreatic ductal carcinoma, but not in the normal epithelium or IPMN without pancreatic ductal carcinoma, regardless of the histologic grade. These results suggest that EphA2 cleavage is an essential event that occurs very early in pancreatic ductal carcinoma development, and that the consequent release of EphA2-NF can be detected in the serum. Thus, serum EphA2-NF could be a diagnostic biomarker for very early-stage pancreatic ductal carcinoma and pancreatic ductal carcinoma development from high-risk IPMN and as a prognostic biomarker after chemotherapy with GnP. Significance: EphA2 N-terminus deletion is involved in pancreatic ductal carcinoma development from high-risk IPMN and EphA2-NF produced by cleavage can be used as a serum biomarker to diagnose pancreatic ductal carcinoma and predict pancreatic ductal carcinoma development from high-risk IPMN.

Funder

Abbott Laboratories

Japan Agency for Medical Research and Development

MEXT | Japan Society for the Promotion of Science

Princess Takamatsu Cancer Research Fund

Publisher

American Association for Cancer Research (AACR)

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