Prx i suppresses K-ras-driven lung tumorigenesis by opposing redox-sensitive ERK/Cyclin D1 pathway

Young Ho Park; Sun Uk Kim; Bo Kyoung Lee; Hyun Sun Kim; In Sung Song; Hye Jun Shin; Ying Hao Han; Kyu Tae Chang; Jin Man Kim; Dong Seok Lee; Yeul Hong Kim; Chang Min Choi; Bo Yeon Kim; Dae Yeul Yu

doi:10.1089/ars.2011.4421

Prx i suppresses K-ras-driven lung tumorigenesis by opposing redox-sensitive ERK/Cyclin D1 pathway

Young Ho Park
, Sun Uk Kim
, Bo Kyoung Lee
, Hyun Sun Kim
, In Sung Song
, Hye Jun Shin
, Ying Hao Han
, Kyu Tae Chang
, Jin Man Kim
, Dong Seok Lee
, Yeul Hong Kim
, Chang Min Choi
, Bo Yeon Kim
, Dae Yeul Yu

Research output: Contribution to journal › Article › peer-review

51 Scopus citations

Abstract

Aims: Coupled responses of mutated K-ras and oxidative stress are often an important etiological factor in non-small-cell lung cancer (NSCLC). However, relatively few studies have examined the control mechanism of oxidative stress in oncogenic K-ras-driven NSCLC progression. Here, we studied whether the redox signaling pathway governed by peroxiredoxin I (Prx I) is involved in K-ras ^G12D-mediated lung adenocarcinogenesis. Results: Using human-lung adenocarcinoma tissues and lung-specific K-ras^G12D-transgenic mice, we found that Prx I was significantly up-regulated in the tumor regions via activation of nuclear erythroid 2-related factor 2 (Nrf2) transcription. Interestingly, the increased reactive oxygen species (ROS) by null mutation of Prx I greatly promoted K-ras^G12D-driven lung tumorigenesis in number and size, which appeared to require the activation of the ROS-dependent extracellular signal-regulated kinase (ERK)/cyclin D1 pathway. Innovation: Taken together, these results suggest that Prx I functions as an Nrf2-dependently inducible tumor suppressant in K-ras-driven lung adenocarcinogenesis by opposing ROS/ERK/cyclin D1 pathway activation. Conclusion: These findings provide a better understanding of oxidative stress-mediated lung tumorigenesis. Antioxid. Redox Signal. 19, 482-496.

Original language	English
Pages (from-to)	482-496
Number of pages	15
Journal	Antioxidants and Redox Signaling
Volume	19
Issue number	5
DOIs	https://doi.org/10.1089/ars.2011.4421
State	Published - 10 Aug 2013

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@article{e541149461944f398264b1ff31c8e472,

title = "Prx i suppresses K-ras-driven lung tumorigenesis by opposing redox-sensitive ERK/Cyclin D1 pathway",

abstract = "Aims: Coupled responses of mutated K-ras and oxidative stress are often an important etiological factor in non-small-cell lung cancer (NSCLC). However, relatively few studies have examined the control mechanism of oxidative stress in oncogenic K-ras-driven NSCLC progression. Here, we studied whether the redox signaling pathway governed by peroxiredoxin I (Prx I) is involved in K-ras G12D-mediated lung adenocarcinogenesis. Results: Using human-lung adenocarcinoma tissues and lung-specific K-rasG12D-transgenic mice, we found that Prx I was significantly up-regulated in the tumor regions via activation of nuclear erythroid 2-related factor 2 (Nrf2) transcription. Interestingly, the increased reactive oxygen species (ROS) by null mutation of Prx I greatly promoted K-rasG12D-driven lung tumorigenesis in number and size, which appeared to require the activation of the ROS-dependent extracellular signal-regulated kinase (ERK)/cyclin D1 pathway. Innovation: Taken together, these results suggest that Prx I functions as an Nrf2-dependently inducible tumor suppressant in K-ras-driven lung adenocarcinogenesis by opposing ROS/ERK/cyclin D1 pathway activation. Conclusion: These findings provide a better understanding of oxidative stress-mediated lung tumorigenesis. Antioxid. Redox Signal. 19, 482-496.",

author = "Park, \{Young Ho\} and Kim, \{Sun Uk\} and Lee, \{Bo Kyoung\} and Kim, \{Hyun Sun\} and Song, \{In Sung\} and Shin, \{Hye Jun\} and Han, \{Ying Hao\} and Chang, \{Kyu Tae\} and Kim, \{Jin Man\} and Lee, \{Dong Seok\} and Kim, \{Yeul Hong\} and Choi, \{Chang Min\} and Kim, \{Bo Yeon\} and Yu, \{Dae Yeul\}",

year = "2013",

month = aug,

day = "10",

doi = "10.1089/ars.2011.4421",

language = "English",

volume = "19",

pages = "482--496",

journal = "Antioxidants and Redox Signaling",

issn = "1523-0864",

publisher = "Mary Ann Liebert Inc.",

number = "5",

}

TY - JOUR

T1 - Prx i suppresses K-ras-driven lung tumorigenesis by opposing redox-sensitive ERK/Cyclin D1 pathway

AU - Park, Young Ho

AU - Kim, Sun Uk

AU - Lee, Bo Kyoung

AU - Kim, Hyun Sun

AU - Song, In Sung

AU - Shin, Hye Jun

AU - Han, Ying Hao

AU - Chang, Kyu Tae

AU - Kim, Jin Man

AU - Lee, Dong Seok

AU - Kim, Yeul Hong

AU - Choi, Chang Min

AU - Kim, Bo Yeon

AU - Yu, Dae Yeul

PY - 2013/8/10

Y1 - 2013/8/10

N2 - Aims: Coupled responses of mutated K-ras and oxidative stress are often an important etiological factor in non-small-cell lung cancer (NSCLC). However, relatively few studies have examined the control mechanism of oxidative stress in oncogenic K-ras-driven NSCLC progression. Here, we studied whether the redox signaling pathway governed by peroxiredoxin I (Prx I) is involved in K-ras G12D-mediated lung adenocarcinogenesis. Results: Using human-lung adenocarcinoma tissues and lung-specific K-rasG12D-transgenic mice, we found that Prx I was significantly up-regulated in the tumor regions via activation of nuclear erythroid 2-related factor 2 (Nrf2) transcription. Interestingly, the increased reactive oxygen species (ROS) by null mutation of Prx I greatly promoted K-rasG12D-driven lung tumorigenesis in number and size, which appeared to require the activation of the ROS-dependent extracellular signal-regulated kinase (ERK)/cyclin D1 pathway. Innovation: Taken together, these results suggest that Prx I functions as an Nrf2-dependently inducible tumor suppressant in K-ras-driven lung adenocarcinogenesis by opposing ROS/ERK/cyclin D1 pathway activation. Conclusion: These findings provide a better understanding of oxidative stress-mediated lung tumorigenesis. Antioxid. Redox Signal. 19, 482-496.

AB - Aims: Coupled responses of mutated K-ras and oxidative stress are often an important etiological factor in non-small-cell lung cancer (NSCLC). However, relatively few studies have examined the control mechanism of oxidative stress in oncogenic K-ras-driven NSCLC progression. Here, we studied whether the redox signaling pathway governed by peroxiredoxin I (Prx I) is involved in K-ras G12D-mediated lung adenocarcinogenesis. Results: Using human-lung adenocarcinoma tissues and lung-specific K-rasG12D-transgenic mice, we found that Prx I was significantly up-regulated in the tumor regions via activation of nuclear erythroid 2-related factor 2 (Nrf2) transcription. Interestingly, the increased reactive oxygen species (ROS) by null mutation of Prx I greatly promoted K-rasG12D-driven lung tumorigenesis in number and size, which appeared to require the activation of the ROS-dependent extracellular signal-regulated kinase (ERK)/cyclin D1 pathway. Innovation: Taken together, these results suggest that Prx I functions as an Nrf2-dependently inducible tumor suppressant in K-ras-driven lung adenocarcinogenesis by opposing ROS/ERK/cyclin D1 pathway activation. Conclusion: These findings provide a better understanding of oxidative stress-mediated lung tumorigenesis. Antioxid. Redox Signal. 19, 482-496.

UR - https://www.scopus.com/pages/publications/84877597805

U2 - 10.1089/ars.2011.4421

DO - 10.1089/ars.2011.4421

M3 - Article

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SN - 1523-0864

VL - 19

SP - 482

EP - 496

JO - Antioxidants and Redox Signaling

JF - Antioxidants and Redox Signaling

IS - 5

ER -

Prx i suppresses K-ras-driven lung tumorigenesis by opposing redox-sensitive ERK/Cyclin D1 pathway

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