The Emerging Role of SOX2 in Cell Proliferation and Survival and Its Crosstalk with Oncogenic Signaling in Lung Cancer

Chou, Yu‐Ting; Lee, Chih Chan; Hsiao, Shih-Hsin; Lin, Sey‐En; Lin, Sheng Chieh; Chung, Chih‐Hung; Chung, Chi Hsiu; Kao, Yu Rong; Wang, Yuan Hung; Chen, Chien Tsun; Wei, Yau Huei; Wu, Cheng Wen

doi:10.1002/stem.1518

Cited by 103 publications

(107 citation statements)

References 32 publications

(38 reference statements)

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“…Functional analyses by gene knockdown and a chemical inhibitor revealed that ALDH and SOX2 are essential for the proliferation of ovarian CSCs. Of note, both ALDH1A and SOX2 expression contribute to chemo-resistance of ovarian cancer cell lines (35,(43)(44)(45). Therefore, SOX2 and ALDH may mediate its capability to confer chemo-resistance to ovarian CSCs as well as stem cell-related features.…”

Section: Discussionmentioning

confidence: 99%

Establishment and Characterization of an In Vitro Model of Ovarian Cancer Stem-like Cells with an Enhanced Proliferative Capacity

Ishiguro

Sato²,

Ohata³

et al. 2016

Cancer Research

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The establishment of cancer stem-like cell (CSC) culture systems may be instrumental in devising strategies to fight refractory cancers. Inhibition of the Rho kinase ROCK has been shown to favorably affect CSC spheroid cultures. In this study, we show how ROCK inhibition in human serous ovarian cancer (SOC) cells can help establish a CSC system, which illuminates cancer pathophysiology and its treatment in this setting. In the presence of a ROCK kinase inhibitor, spheroid cultures of SOC cells expressed characteristic CSC markers including ALDH1A1, CD133, and SOX2, along with differentiation and tumorigenic capabilities in mouse xenograft models of human SOC. High expression levels of ALDH, but not CD133, correlated with spheroid formation CSC marker expression and tumor forming capability. In clinical specimens of SOC, high levels of ALDH1A1 correlated with advanced stage and poor prognosis. Pharmacologic or genetic blockade of ALDH blocked cell proliferation and reduced expression of SOX2, the genetic ablation of which abolished spheroid formation, whereas SOX2 overexpression inhibited ALDH1A1 expression and blocked spheroid proliferation. Taken together, our findings illustrated a new method to culture human ovarian CSC, and they defined a reciprocal regulatory relationship between ALDH1A1 and SOX2, which impacts ovarian CSC proliferation and malignant progression. Cancer Res; 76(1); 150-60. Ó2015 AACR.

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Section: Discussionmentioning

confidence: 99%

Establishment and Characterization of an In Vitro Model of Ovarian Cancer Stem-like Cells with an Enhanced Proliferative Capacity

Ishiguro

Sato²,

Ohata³

et al. 2016

Cancer Research

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“…In lung cancer, SOX2 could regulate cancer cells apoptosis through MAP4K4-Survivin signaling pathway [27]. The emerging role of SOX2 in cell proliferation and survival by eliciting oncogenic EGFR and BCL2L1 signaling was identified as a prognosis marker and a therapeutic target [28]. Wnt signaling substantially could impact NSCLC tumorigenesis, prognosis, and resistance to therapy [29].…”

Section: Discussionmentioning

confidence: 99%

“…In various cancers, SOX2 has been indentified to promote proliferation and invasion [16,17]. Here, we explored whether the functional effect of miR-638 on NSCLC cell lines was dependent on SOX2.…”

Section: Silencing Of Sox2 By Sirna Partially Abolished the Enhancemementioning

confidence: 99%

Downregulation of miR‐638 promotes invasion and proliferation by regulating SOX2 and induces EMT in NSCLC

Xia

Liu

et al. 2014

FEBS Letters

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Edited by Tamas DalmayKeywords: miR-638 SRY (sex determining region Y)-box 2 Proliferation Invasion Epithelial-to-mesenchymal transition Non-small-cell lung cancer a b s t r a c t Aberrant expression of microRNAs has been shown to regulate the biological processes of lung cancer cells. However, the role of miR-638 in the development of NSCLC is still unclear. In this study, low miR-638 and high SOX2 were shown to be associated with tumor size and metastasis of NSCLC patients. Downregulated miR-638 could promote cell invasion and proliferation, while high miR-638 expression reversed the effect. Furthermore, miR-638 could regulate SOX2 by directly binding to its 3 0 -UTR. Silencing of SOX2 by siRNA partially abolished the enhancement of cell invasion and proliferation induced by downregulated miR-638. Aberrant miR-638 expression could modulate the expression levels of markers of epithelial-to-mesenchymal transition. Our results indicate that miR-638 may play a pivotal role in the development of NSCLC.

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“…Tissue sections were stained overnight at 4 °C with each CSLC marker anti-human antibody (Table 1). We used seven markers that have been reported to be CSLC markers for lung or other solid malignant tumors (Caveolin, Notch, CD44, CD166, SOX2, Aldehyde dehydrogenase 1 [ALDH1], and Musashi1) (Chou et al 2013;Fischer et al 2011;Jiang et al 2009;Kuang et al 2013;Leung et al 2010;Palaniyandi et al 2012;Zhang et al 2012). The slides were subsequently incubated with EnVision™ (DAKO, Glostrup, Denmark) for 1 h at room temperature, and the color reaction developed.…”

Section: Immunohistochemical Analyses Evaluation and Scoringmentioning

confidence: 99%

Clinicopathological significance of cancer stem-like cell markers in high-grade neuroendocrine carcinoma of the lung

Morise

Hishida

Takahashi

et al. 2015

J Cancer Res Clin Oncol

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The Emerging Role of SOX2 in Cell Proliferation and Survival and Its Crosstalk with Oncogenic Signaling in Lung Cancer

Cited by 103 publications

References 32 publications

Establishment and Characterization of an In Vitro Model of Ovarian Cancer Stem-like Cells with an Enhanced Proliferative Capacity

Establishment and Characterization of an In Vitro Model of Ovarian Cancer Stem-like Cells with an Enhanced Proliferative Capacity

Downregulation of miR‐638 promotes invasion and proliferation by regulating SOX2 and induces EMT in NSCLC

Clinicopathological significance of cancer stem-like cell markers in high-grade neuroendocrine carcinoma of the lung

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