XPC inhibits NSCLC cell proliferation and migration by enhancing E-Cadherin expression

Tiantian Cui; Amit Kumar Srivastava; Chunhua Han; Linlin Yang; Ran Zhao; Ning Zou; Meihua Qu; Wenrui Duan; Xiaoli Zhang; Qi-En Wang

doi:10.18632/oncotarget.3542

Oncotarget

Oncotarget (a primarily oncology-focused, peer-reviewed, open access journal) aims to maximize research impact through insightful peer-review; eliminate borders between specialties by linking different fields of oncology, cancer research and biomedical sciences; and foster application of basic and clinical science.

Its scope is unique. The term "oncotarget" encompasses all molecules, pathways, cellular functions, cell types, and even tissues that can be viewed as targets relevant to cancer as well as other diseases. The term was introduced in the inaugural Editorial, Introducing Oncotarget.

As of January 1, 2022, Oncotarget has shifted to a continuous publishing model. Papers will now be published continuously within yearly volumes in their final and complete form and then quickly released to Pubmed.

Subscribe to receive alerts once a paper has been published by Oncotarget.

Impact Journals, LLC is the publisher of Oncotarget: www.impactjournals.com.

Impact Journals is a member of the Wellcome Trust List of Compliant Publishers.

Impact Journals is a member of the Society for Scholarly Publishing.

On December 23, 2022, Oncotarget server experienced a DDoS attack. As a result, Oncotarget site was inaccessible for a few hours. Oncotarget team swiftly dealt with the situation and took it under control. This malicious action will be reported to the FBI.

Research Papers:

XPC inhibits NSCLC cell proliferation and migration by enhancing E-Cadherin expression

Tiantian Cui, Amit Kumar Srivastava, Chunhua Han, Linlin Yang, Ran Zhao, Ning Zou, Meihua Qu, Wenrui Duan, Xiaoli Zhang and Qi-En Wang _

PDF | HTML | Supplementary Files | How to cite

Oncotarget. 2015; 6:10060-10072. https://doi.org/10.18632/oncotarget.3542

Metrics: PDF 4015 views | HTML 3669 views | ?

Abstract

Tiantian Cui1, Amit Kumar Srivastava1, Chunhua Han1, Linlin Yang2, Ran Zhao1, Ning Zou1, Meihua Qu1, Wenrui Duan3, Xiaoli Zhang4 and Qi-En Wang1

1 Department of Radiology, The Ohio State University Wexner Medical Center, Columbus, OH, USA

2 Department of Radiation Oncology, The Ohio State University Wexner Medical Center, Columbus, OH, USA

3 Department of Internal Medicine, The Ohio State University Wexner Medical Center, Columbus, OH, USA

4 Center for Biostatistics, The Ohio State University Wexner Medical Center, Columbus, OH, USA

Correspondence to:

Qi-En Wang, email:

Keywords: XPC, E-Cadherin, non-small-cell lung cancer, Snail, ERK pathway

Received: December 28, 2014 Accepted: February 13, 2015 Published: March 12, 2015

Abstract

Xeroderma pigmentosum complementation group C (XPC) protein is an important DNA damage recognition factor in nucleotide excision repair. Deletion of XPC is associated with early stages of human lung carcinogenesis, and reduced XPC mRNA levels predict poor patient outcome for non-small cell lung cancer (NSCLC). However, the mechanisms linking loss of XPC expression and poor prognosis in lung cancer are still unclear. Here, we report evidence that XPC silencing drives proliferation and migration of NSCLC cells by down-regulating E-Cadherin. XPC knockdown enhanced proliferation and migration while decreasing E-Cadherin expression in NSCLC cells with an epithelial phenotype. Restoration of E-Cadherin in these cells suppressed XPC knockdown-induced cell growth both in vitro and in vivo. Mechanistic studies showed that the loss of XPC repressed E-Cadherin expression by activating the ERK pathway and upregulating Snail expression. Our findings indicate that XPC silencing-induced reduction of E-Cadherin expression contributes, at least in part, to the poor outcome of NSCLC patients with low XPC expression.

All site content, except where otherwise noted, is licensed under a Creative Commons Attribution 4.0 License.
PII: 3542

Publication Alerts

Research Papers:

XPC inhibits NSCLC cell proliferation and migration by enhancing E-Cadherin expression

Abstract