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Cooperation Between Pten and Smad4 in Murine Salivary Gland Tumor Formation and Progression

Authors :
Yu Cao
Han Liu
Liwei Gao
Ling Lu
Li Du
Han Bai
Jiang Li
Sherif Said
Xiao-Jing Wang
John Song
Natalie Serkova
Minjie Wei
Jing Xiao
Shi-Long Lu
Source :
Neoplasia: An International Journal for Oncology Research, Vol 20, Iss 8, Pp 764-774 (2018)
Publication Year :
2018
Publisher :
Elsevier, 2018.

Abstract

Salivary gland tumor (SGT) is a rare tumor type, which exhibits broad-spectrum phenotypic, biological, and clinical heterogeneity. Currently, the molecular mechanisms that cause SGT pathogenesis remain poorly understood. A lack of animal models that faithfully recapitulate the naturally occurring process of human SGTs has hampered research progress on this field. In this report, we developed an inducible keratin 5-driven conditional knockout mouse model to delete gene(s) of interest in murine salivary gland upon local RU486 delivery. We have deleted two major tumor suppressors, Pten, a negative regulator of the PI3K pathway, and Smad4, the central signaling mediator of TGFβ pathway, in the murine salivary gland. Our results have shown that deletion of either Pten or Smad4 in murine salivary gland resulted in pleomorphic adenomas, the most common tumor in human SGT patients. Deletion of both Pten and Smad4 in murine salivary gland developed several malignancies, with salivary adenoid cystic carcinoma (SACC) being the most frequently seen. Molecular characterization showed that SACC exhibited mTOR activation and TGFβ1 overexpression. Examination of human SGT clinical samples revealed that loss of Pten and Smad4 is common in human SACC samples, particularly in the most aggressive solid form, and is correlated with survival of SACC patients, highlighting the human relevance of the murine models. In summary, our results offer significant insight into synergistic role of Pten and Smad4 in SGT, providing a rationale for targeting mTOR and/or TGFβ signaling to control SGT formation and progression.

Details

Language :
English
ISSN :
14765586
Volume :
20
Issue :
8
Database :
Directory of Open Access Journals
Journal :
Neoplasia: An International Journal for Oncology Research
Publication Type :
Academic Journal
Accession number :
edsdoj.981be65cc9ff4d45907ab2c5e928323e
Document Type :
article
Full Text :
https://doi.org/10.1016/j.neo.2018.05.009