| Literature DB >> 35922477 |
Yoshiyuki Tsukamoto1, Shusaku Kurogi2, Tomotaka Shibata3, Kosuke Suzuki3, Yuka Hirashita2,4, Shoichi Fumoto5, Shinji Yano6, Kazuyoshi Yanagihara7, Chisato Nakada2,8, Fumi Mieno2, Keisuke Kinoshita2,4, Takafumi Fuchino2,4, Kazuhiro Mizukami4, Yoshitake Ueda9, Tsuyoshi Etoh3, Tomohisa Uchida2, Toshikatsu Hanada10, Mutsuhiro Takekawa11, Tsutomu Daa6, Kuniaki Shirao12, Shuichi Hironaka12, Kazunari Murakami4, Masafumi Inomata3, Naoki Hijiya2, Masatsugu Moriyama2.
Abstract
Despite recent advances in sequencing technology and large-scale drug screenings employing hundreds of cell lines, the predictive accuracy of mutation-based biomarkers is still insufficient as a guide for cancer therapy. Therefore, novel types of diagnostic methods using alternative biomarkers would be highly desirable. We have hypothesized that sensitivity-specific changes in the phosphorylation of signaling molecules could be useful in this respect. Here, with the aim of developing a method for predicting the response of cancers to cisplatin using a combination of specific biomarker(s) and patient-derived tumor organoids (PDOs), we found that cisplatin-sensitive cell lines or PDOs showed enhanced phosphorylation of c-Jun (p-c-Jun) within 24 h after cisplatin treatment. We also compared the responses of 6 PDOs to cisplatin with the therapeutic effect of neoadjuvant chemotherapy (docetaxel/cisplatin/5-fluorouracil) in 6 matched patients. Mechanistically, the c-Jun induction was partly related to TNF signaling induced by cisplatin. Our data suggest that enhanced phosphorylation of c-Jun in response to cisplatin treatment could be a predictive biomarker for the efficacy of cisplatin in selected cancer patients.Entities:
Year: 2022 PMID: 35922477 DOI: 10.1038/s41374-022-00827-2
Source DB: PubMed Journal: Lab Invest ISSN: 0023-6837 Impact factor: 5.502