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Mutant PIK3CA as a negative predictive biomarker for treatment with a highly selective PIM1 inhibitor in human colon cancer

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Abstract
Significant improvement in targeted therapy for colorectal cancer (CRC) has occurred over the past few decades since the approval of the EGFR inhibitor cetuximab. However, cetuximab is used only for patients possessing the wild-type oncogene KRAS, NRAS, and BRAF, and even most of these eventually acquire therapeutic resistance, via activation of parallel oncogenic pathways such as RAS-MAPK or PI3K/Akt/mTOR. The two aforementioned pathways also contribute to the development of therapeutic resistance in CRC patients, due to compensatory and feedback mechanisms. Therefore, combination drug therapies (versus monotherapy) targeting these multiple pathways may be necessary for further efficacy against CRC. In this study, we identified PIK3CA mutant (PIK3CA MT) as a determinant of resistance to SMI-4a, a highly selective PIM1 kinase inhibitor, in CRC cell lines. In CRC cell lines, SMI-4a showed its effect only in PIK3CA wild type (PIK3CA WT) cell lines, while PIK3CA MT cells did not respond to SMI-4a in cell death assays. In vivo xenograft and PDX experiments confirmed that PIK3CA MT is responsible for the resistance to SMI-4a. Inhibition of PIK3CA MT by PI3K inhibitors restored SMI-4a sensitivity in PIK3CA MT CRC cell lines. Taken together, these results demonstrate that sensitivity to SMI-4a is determined by the PIK3CA genotype and that co-targeting of PI3K and PIM1 in PIK3CA MT CRC patients could be a promising and novel therapeutic approach for refractory CRC patients.
Issued Date
2023
Yoon Sun Park
Joseph Kim
Yea Seong Ryu
Jai-Hee Moon
Yu Jin Shin
Jeong Hee Kim
Seung-Woo Hong
Soo-A Jung
Seul Lee
Seung-Mi Kim
Dae Hee Lee
Do Yeon Kim
Hyeseon Yun
Ji-Eun You
Dong Il Yoon
Chul Hee Kim
Dong-In Koh
Dong-Hoon Jin
Type
Article
Keyword
PIK3CAPIM1colorectal cancermutant KRASpredictive marker
DOI
10.1080/15384047.2023.2246208
URI
https://oak.ulsan.ac.kr/handle/2021.oak/16061
Publisher
CANCER BIOLOGY & THERAPY
Language
한국어
ISSN
1538-4047
Citation Volume
24
Citation Number
1
Citation Start Page
1
Citation End Page
10
Appears in Collections:
Medicine > Nursing
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