Alterations in nuclear pore architecture allow cancer cell entry into or exit from drug-resistant dormancy.

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Publication Details

Output type: Journal article

Author list: Kinoshita, Kalir, Rahaman, Dottino, Kohtz

Publisher: Elsevier

Publication year: 2012

Volume number: 180

Issue number: 1

Start page: 375

End page: 89

Number of pages: -285

ISSN: 0002-9440

eISSN: 1525-2191

Languages: English-Great Britain (EN-GB)

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Open access status: hybrid

Full text URL: http://ajp.amjpathol.org/article/S000294401100914X/pdf

Abstract

Phenotypic diversity arises in tumors just as it does in developing organisms, and tumor recurrence frequently manifests from the selective survival of divergent drug-resistant cells. Although the expanding tumor cell population may be successfully targeted, drug-resistant cells may persist and sustain the tumor or enter dormancy before igniting a future relapse. Herein, we show that partial knockdown of nucleoporin p62 (NUP62) by small-interfering RNA confers cisplatin resistance to cultured high-grade ovarian carcinoma cells. Treatment with NUP62 small-interfering RNA and cisplatin leaves resistant cells in a state of dormancy; some dormant cells can be induced to proliferate by transient induction of NUP62 expression from an ectopic expression construct. In addition to suggesting functional links between nuclear pore complex architecture and cancer cell survival, the culture system provides a novel experimental window into the dynamics of tumor cell drug resistance and dormancy.

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