The anti-mesothelin monoclonal antibody amatuximab enhances the anti-tumor effect of gemcitabine against mesothelin-high expressing pancreatic cancer cells in a peritoneal metastasis mouse model.

Tatsuzo Mizukami,Fumihiko Matsuzawa,Hirofumi Kamachi,Yutaka Hatanaka,Takahiro Einama,Nozomi Kobayashi,Yuki Fujii,Akinobu Taketomi,Futoshi Kawamata

doi:10.18632/oncotarget.26117

Tatsuzo Mizukami, Fumihiko Matsuzawa + Show 7 more

Open Access

https://doi.org/10.18632/oncotarget.26117

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Journal: Oncotarget	Publication Date: Sep 18, 2018
Citations: 20	License type: cc-by

Affiliation: Hokkaido University, Hokkaido University Hospital

Abstract

Pancreatic cancer often has a very poor prognosis, even after complete resection. The recurrence of hepatic and peritoneal metastases is an important prognostic factor; therefore, the development of improved adjuvant therapy is urgently required. Mesothelin is a cell surface glycoprotein whose expression is restricted to a variety of cancer types, including pancreatic cancer. This expression pattern makes mesothelin an attractive target for cancer therapy, and several agents targeting mesothelin are currently in clinical trials. Here, we used the chimerized high-affinity anti-mesothelin monoclonal antibody amatuximab to investigate its effect on peritoneal metastasis. We used the AsPC-1 pancreatic cancer cell line engineered to express Gaussia luciferase (Gluc), (AsPC-1-Gluc) for in vivo experiments. Results showed that while amatuximab was not directly cytotoxic on an AsPC-1-Gluc tumor cells in a peritoneal metastasis model, it prevented the formation of tumor growth. In combination therapy with gemcitabine, amatuximab exhibited synergistic killing. Our results suggest that blockade of mesothelin by amatuximab may be a useful strategy for preventing the peritoneal dissemination of pancreatic cancer under an adjuvant setting.

Highlights

Pancreatic cancer is the fourth leading cause of cancer death in the United States, and its 5-year survival rate is only 6% [1]
We demonstrated that the anti-mesothelin antibody amatuximab suppressed peritoneal metastases and enhanced the anti-tumor effects of gemcitabine in peritoneal metastases of AsPC-1-Gaussia luciferase (Gluc) cells in a mouse model of pancreatic cancer
This effect appeared as a result of amatuximab to preventing the development of tumor masses, reduction in tumor cell viability and overall gross tumor mass

Summary

Introduction

Pancreatic cancer is the fourth leading cause of cancer death in the United States, and its 5-year survival rate is only 6% [1]. Surgical resection remains the only potentially curative therapeutic option. Pancreatic cancer proceeds asymptomatically in many cases, and surgical resection is feasible in only 10%–20% of patients at the time of initial diagnosis [2]. The long-term survival rate remains very poor [3, 4]. Hepatic and peritoneal metastasis were reported to be important prognosticators in pancreatic cancer [5]. Curative resection of pancreatic carcinoma revealed frequent micrometastatic dissemination, which is not detected by imaging or gross pathology in cases of radical treatment [6]. Controlling the microdissemination of residual malignant cells postoperation is critical for improving prognosis

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