RETRACTED ARTICLE: Ibrutinib facilitates the sensitivity of colorectal cancer cells to ferroptosis through BTK/NRF2 pathway

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作者
Jin-Feng Zhu
Yi Liu
Wen-Ting Li
Ming-Hui Li
Chao-Hui Zhen
Pei-Wei Sun
Ji-Xin Chen
Wen-Hao Wu
Wei Zeng
机构
[1] Shenzhen University General Hospital,Department of General Surgery
[2] Department of Gastrointestinal Surgery,Department of Cardiothoracic Surgery
[3] Shunde Hospital,Department of Pathology
[4] Southern Medical University (The First People’s Hospital of Shunde,Department of Ultrasound
[5] Foshan),Department of Oncology
[6] Shenzhen University General Hospital,undefined
[7] Shenzhen University General Hospital,undefined
[8] Shenzhen University General Hospital,undefined
[9] Shunde Hospital,undefined
[10] Southern Medical University (The First People’s Hospital of Shunde,undefined
[11] Foshan),undefined
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摘要
Ibrutinib is a drug that inhibits the protein Burton’s tyrosine kinase and thereby the nuclear translocation of Nrf2, which played a key role in mediating the activation of antioxidants during stress conditions and ferroptosis resistance. This study aimed to identify the effect of Ibrutinib and ferroptosis inducer on colorectal cancer (CRC) treatment and its underlying mechanism. In our study, we found the upregulation of Nrf2 was correlated with CRC progression and antioxidant proteins. Ibrutinib sensitized CRC to ferroptosis inducers, suggested by further reduced CRC cell viability, proliferation and decreased antioxidant protein levels in CRC cells after combination treatment of Ibrutinib and RSL3 or Ibrutinib and Erastin both in vivo and in vitro. Knockout of Nrf2 diminished the regulatory effect of Ibrutinib on CRC sensitivity to ferroptosis inducers. Altogether, this study demonstrated that Ibrutinib increases the sensitivity of CRC cell to ferroptosis inducers by inhibiting Nrf2.
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