Identification of CD90 as Putative Cancer Stem Cell Marker and Therapeutic Target in Insulinomas

Publication date

2016

Authors

Buishand, Floryne OISNI 0000000505973386
Arkesteijn, Ger J A
Feenstra, Laurien R
Oorsprong, Claire W D
Mestemaker, Margiet
Starke, Achim
Speel, Ernst-Jan M
Kirpensteijn, JolleISNI 0000000393643429
Mol, Jan AISNI 0000000109723801

Editors

Advisors

Supervisors

Document Type

Article
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License

taverne

Abstract

The long-term prognosis after surgical resection of malignant insulinoma (INS) is poor. Novel adjuvant therapies, specifically targeting cancer stem cells (CSCs), are warranted. Therefore, the goal of this study was to characterize and target putative INS CSCs. Using fluorescence-activated cell sorting, human INS cell line CM and pancreatic carcinoid cell line BON1 were screened for the presence of stem cell-associated markers. CD90, CD166, and GD2 were identified as potential CSC markers. Only CD90(+) INS cells had an increased tumor-initiating potential in athymic nude mice. Anti-CD90 monoclonal antibodies decreased the viability and metastatic potential of injected cells in a zebrafish embryo INS xenograft model. Primary INS stained positive for CD90 by immunohistochemistry, however also intratumoral fibroblasts and vascular endothelium showed positive staining. The results of this study suggest that anti-CD90 monoclonals form a potential novel adjuvant therapeutic modality by targeting either INS cells directly, or by targeting the INS microenvironment.

Keywords

Taverne, SDG 3 - Good Health and Well-being

Citation

Buishand, F O, Arkesteijn, G J A, Feenstra, L R, Oorsprong, C W D, Mestemaker, M, Starke, A, Speel, E-J M, Kirpensteijn, J & Mol, J A 2016, 'Identification of CD90 as Putative Cancer Stem Cell Marker and Therapeutic Target in Insulinomas', Stem Cells and Development, vol. 25, no. 11, pp. 826-835. https://doi.org/10.1089/scd.2016.0032