Literature DB >> 33073679

mTOR Inhibition Ablates Cisplatin-Resistant Salivary Gland Cancer Stem Cells.

T Nakano1,2, K A Warner1, A E Oklejas1, Z Zhang1, C Rodriguez-Ramirez1, A G Shuman3, J E Nör1,3,4,5.   

Abstract

Patients with advanced salivary gland mucoepidermoid carcinoma (MEC) are treated with surgery and radiotherapy, as current systemic therapies are largely ineffective. As such, current treatment frequently leads to poor long-term survival due to locoregional recurrence or metastases. We have shown that salivary gland cancer stem cells (CSCs) are resistant to platinum-based chemotherapy and drive tumor progression. The purpose of this study was to investigate the effect of therapeutic inhibition of mTOR (mechanistic target of rapamycin) on resistance of CSCs to cisplatin, a prototypic platinum-based chemotherapeutic agent. Viability assays determined the effect of several inhibitors of PI3k/mTOR signaling (e.g., temsirolimus, BKM120, AZD8055, PF4708671) and/or cisplatin on survival of human MEC cells. The impact of mTOR inhibitors and/or cisplatin on MEC stemness was examined with salisphere assays, flow cytometry for ALDH/CD44 (CSC markers for MEC), and Western blots for Bmi-1 expression (marker of stem cell self-renewal). Salivary gland MEC patient-derived xenografts were used to examine the effect of cisplatin and/or temsirolimus on CSCs in vivo. We observed that cisplatin induced mTOR and S6K1 phosphorylation, increased the number and size of MEC salispheres, and induced Bmi-1 expression and the fraction of CSCs in MEC models in vitro. Cisplatin also increased the fraction of CSCs in vivo. In contrast, mTOR inhibition (e.g., temsirolimus) blocked cisplatin-induced Bmi-1 expression and salisphere formation in vitro. Remarkably, temsirolimus slowed down tumor growth and decreased the fraction of CSCs (P < 0.05) even in presence of cisplatin in a short-term in vivo experiment. Collectively, these results demonstrate that therapeutic inhibition of mTOR ablates cytotoxic-resistant CSCs, and they suggest that a combination of an mTOR inhibitor and platinum-based chemotherapy might be beneficial to patients with salivary gland mucoepidermoid carcinoma.

Entities:  

Keywords:  chemotherapy; head and neck cancer; rapamycin; self-renewal; targeted therapy; tumor initiating cell

Mesh:

Substances:

Year:  2020        PMID: 33073679      PMCID: PMC7989140          DOI: 10.1177/0022034520965141

Source DB:  PubMed          Journal:  J Dent Res        ISSN: 0022-0345            Impact factor:   8.924


  34 in total

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Journal:  J Natl Cancer Inst       Date:  2016-09-15       Impact factor: 13.506

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Authors:  Robert A Saxton; David M Sabatini
Journal:  Cell       Date:  2017-04-06       Impact factor: 41.582

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Journal:  Clin Cancer Res       Date:  2016-08-22       Impact factor: 12.531

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Authors:  Mario A Luna
Journal:  Adv Anat Pathol       Date:  2006-11       Impact factor: 3.875

Review 7.  Targeting mTOR and Metabolism in Cancer: Lessons and Innovations.

Authors:  Cedric Magaway; Eugene Kim; Estela Jacinto
Journal:  Cells       Date:  2019-12-06       Impact factor: 6.600

8.  A restricted cell population propagates glioblastoma growth after chemotherapy.

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Review 10.  B lymphoma Moloney murine leukemia virus insertion region 1: An oncogenic mediator in prostate cancer.

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Journal:  Asian J Androl       Date:  2019 May-Jun       Impact factor: 3.285

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  3 in total

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Authors:  Yang Chen; Hui Zhao; Weilian Liang; Erhui Jiang; Xiaocheng Zhou; Zhe Shao; Ke Liu; Zhengjun Shang
Journal:  Oncogene       Date:  2021-11-19       Impact factor: 9.867

2.  p-S6 as a Prognostic Biomarker in Canine Oral Squamous Cell Carcinoma.

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Review 3.  Oral Cancer Stem Cells: Therapeutic Implications and Challenges.

Authors:  Linah A Shahoumi
Journal:  Front Oral Health       Date:  2021-07-21
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