4.4 Article

SOX2 Expression in Canine Neoplasia

Journal

VETERINARY PATHOLOGY
Volume 58, Issue 5, Pages 964-970

Publisher

SAGE PUBLICATIONS INC
DOI: 10.1177/0300985820960130

Keywords

cancer stem cells; canine; immunohistochemistry; neoplasia; sex-determining region Y-box 2 (SOX2); tumor-initiating cells

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SOX2 is widely expressed in canine cancers, with strong and diffuse expression in ectodermal and endodermal tumors, while negative, variable, or inconsistent expression is found in mesodermal tumors and tumors with dual or uncertain origin. Further studies are needed to understand the role of SOX2 in the biology of different canine cancers.
SOX2 is a major transcriptional regulator of stem cell pluripotency and self-renewability. Its expression in cancer stem cells from several different tumor types in humans and rodent models directly implicates SOX2 in tumorigenicity, metastasis, drug resistance, recurrence, and poor survival. Our objective was to investigate the expression of SOX2 in canine neoplasia. Immunohistochemistry for SOX2 was performed in sets of 10 archived formalin-fixed paraffin-embedded tissues from 45 distinct canine neoplasms. Normal expression of SOX2 was evaluated in a canine tissue microarray. Strong and diffuse SOX2 intranuclear immunolabeling was consistently found in the majority of ectodermal (13/15) and endodermal tumors (5/7). Negative, variable, or inconsistent SOX2 intranuclear immunolabeling was detected in the majority of mesodermal tumors (10/16) and in tumors with dual or uncertain origin (5/7). Although further studies are necessary to understand mechanistically how SOX2 contributes to the biology of each tumor type, this study demonstrates the expression of SOX2 in a wide variety of canine cancers. In the future, screening methods based on cellular plasticity and pluripotency biomarkers may provide avenues for the rational design of therapeutic strategies that target vulnerable signals upstream or downstream of SOX2 in different cancers, and possibly offer novel clinical applications for SOX2 as a prognostic indicator.

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