Oncotarget

Research Papers:

TRIB2 contributes to cisplatin resistance in small cell lung cancer

Yuanxin Liang, Dong Yu, Roman Perez-Soler, Jim Klostergaard and Yiyu Zou _

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Oncotarget. 2017; 8:109596-109608. https://doi.org/10.18632/oncotarget.22741

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Abstract

Yuanxin Liang1,4, Dong Yu2, Roman Perez-Soler1, Jim Klostergaard3 and Yiyu Zou1

1Department of Medicine/Cancer Center, Albert Einstein College of Medicine, Bronx, NY, USA

2Department of Respiratory and Oncology, Hubei Provincial Corps Hospital, Wuhan, China

3Department of Molecular and Cellular Oncology, MD Anderson Cancer Center, Houston, TX, USA

4Department of Pathology, Tufts Medical Center, Boston, MA, USA

Correspondence to:

Yiyu Zou, email: [email protected]

Keywords: TRIB2; CEBPA; small cell lung cancer; cisplatin; resistance

Received: January 17, 2017     Accepted: August 28, 2017     Published: November 27, 2017

ABSTRACT

Small cell lung cancer (SCLC) is the most aggressive lung-cancer subtype and so far, no favorable therapeutic strategy has been established for chemo-resistant SCLC. Cisplatin is one of the most important components among all standard poly-chemotherapeutic regimens for SCLC; therefore, this study focused on revealing Cisplatin-resistance mechanism(s) in this disease. Cisplatin-resistant SCLC cells were generated in the NCI-H69 xenograft model in nude mice by continuous intravenous administration of Cisplatin; Cisplatin resistance of the tumor cells was confirmed by in vitro and in vivo tests, and the gene expression profile of the resistant cells was determined using microarray analysis. A significantly higher expression of tribbles pseudokinase 2 (TRIB2) mRNA in the Cisplatin-resistant cells was found compared to parental H69 cells. Further, the Cisplatin-resistance level was decreased when TRIB2 expression was knocked down. The mRNA and protein levels of CCAAT/enhancer binding protein alpha (CEBPA), known to be a transcription factor regulating cell differentiation and a target for degradation by TRIB2, as well as selected cancer stem cell makers in the Cisplatin-resistant cells, were measured. We found that CEBPA protein levels could be upregulated by knocking down the overexpressed TRIB2, which also reversed the Cisplatin-resistance of these cells; further, the Cisplatin-resistant SCLC cells demonstrated certain cancer stem cell-like properties. Similar patterns were also observed in limited human tumor specimens of chemo-resistant SCLC patients: namely, overexpressed TRIB2 and undetected CEBPA proteins. Our study revealed a possible molecular mechanism for Cisplatin-resistant SCLC involving induced TRIB2 overexpression and downregulation of CEBPA protein. We propose that this mechanism is a potential therapeutic target to circumvent chemo-resistance in SCLC.


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