Literature DB >> 21969819

NRF2 mutation confers malignant potential and resistance to chemoradiation therapy in advanced esophageal squamous cancer.

Tatsuhiro Shibata1, Akiko Kokubu, Shigeru Saito, Mako Narisawa-Saito, Hiroki Sasaki, Kazuhiko Aoyagi, Yuki Yoshimatsu, Yuji Tachimori, Ryoji Kushima, Tohru Kiyono, Masayuki Yamamoto.   

Abstract

Esophageal squamous cancer (ESC) is one of the most aggressive tumors of the gastrointestinal tract. A combination of chemotherapy and radiation therapy (CRT) has improved the clinical outcome, but the molecular background determining the effectiveness of therapy remains unknown. NRF2 is a master transcriptional regulator of stress adaptation, and gain of-function mutation of NRF2 in cancer confers resistance to stressors including anticancer therapy. Direct resequencing analysis revealed that Nrf2 gain-of-function mutation occurred recurrently (18/82, 22%) in advanced ESC tumors and ESC cell lines (3/10). The presence of Nrf2 mutation was associated with tumor recurrence and poor prognosis. Short hairpin RNA-mediated down-regulation of NRF2 in ESC cells that harbor only mutated Nrf2 allele revealed that themutant NRF2 conferred increased cell proliferation, attachment-independent survival, and resistance to 5-fluorouracil and γ-irradiation. Based on the Nrf2 mutation status, gene expression signatures associated with NRF2 mutation were extracted from ESC cell lines, and their potential utility for monitoring and prognosis was examined in a cohort of 33 pre-CRT cases of ESC. The molecular signatures of NRF2 mutation were significantly predictive and prognostic for CRT response. In conclusion, recurrent NRF2 mutation confers malignant potential and resistance to therapy in advanced ESC, resulting in a poorer outcome. Molecular signatures of NRF2 mutation can be applied as predictive markers of response to CRT, and efficient inhibition of aberrant NRF2 activation could be a promising approach in combination with CRT.

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Year:  2011        PMID: 21969819      PMCID: PMC3182278          DOI: 10.1593/neo.11750

Source DB:  PubMed          Journal:  Neoplasia        ISSN: 1476-5586            Impact factor:   5.715


  37 in total

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Review 4.  Alcohol drinking, cigarette smoking, and the development of squamous cell carcinoma of the esophagus: epidemiology, clinical findings, and prevention.

Authors:  Masaru Morita; Ryuichi Kumashiro; Nobuhide Kubo; Yuichiro Nakashima; Rintaro Yoshida; Keiji Yoshinaga; Hiroshi Saeki; Yasunori Emi; Yoshihiro Kakeji; Yoshihisa Sakaguchi; Yasushi Toh; Yoshihiko Maehara
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6.  Oncogenic NRF2 mutations in squamous cell carcinomas of oesophagus and skin.

Authors:  Yoo Ri Kim; Ji Eun Oh; Min Sung Kim; Mi Ran Kang; Sang Wook Park; Ji Youn Han; Hyeon Seok Eom; Nam Jin Yoo; Sug Hyung Lee
Journal:  J Pathol       Date:  2010-03       Impact factor: 7.996

7.  Global mapping of binding sites for Nrf2 identifies novel targets in cell survival response through ChIP-Seq profiling and network analysis.

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Journal:  Nucleic Acids Res       Date:  2010-05-11       Impact factor: 16.971

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10.  Nrf2-regulated glutathione recycling independent of biosynthesis is critical for cell survival during oxidative stress.

Authors:  C J Harvey; R K Thimmulappa; A Singh; D J Blake; G Ling; N Wakabayashi; J Fujii; A Myers; S Biswal
Journal:  Free Radic Biol Med       Date:  2008-11-05       Impact factor: 7.376

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Review 6.  The Keap1-Nrf2 pathway: promising therapeutic target to counteract ROS-mediated damage in cancers and neurodegenerative diseases.

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7.  Role of KEAP1/NRF2 and TP53 Mutations in Lung Squamous Cell Carcinoma Development and Radiation Resistance.

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Review 8.  Targeted therapy of esophageal squamous cell carcinoma: the NRF2 signaling pathway as target.

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Journal:  Ann N Y Acad Sci       Date:  2018-05-11       Impact factor: 5.691

Review 9.  Radiation and inflammation.

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10.  Geldanamycin-Derived HSP90 Inhibitors Are Synthetic Lethal with NRF2.

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