| Literature DB >> 33782542 |
Kai-Long Jiang1,2, Le-Xian Tong3, Tao Wang4, Han-Lin Wang1,2,5, Xiao-Bei Hu1,6, Gao-Ya Xu1, Ting-Ting Jin3, Wei-Juan Kan1, Lei Xu1,2,6, Jia-Nan Li1,7, Kai-Xiang Zhang1,2, Ning Song1,2,5, Jie-Yu Liu1,2, Meng-Meng Zhang1, Wen-Biao Wu1,2, Yu-Qi Xiang1,2,5, An-Hui Gao1, Yong-Zhou Hu3, Yu-Bo Zhou8,9,10, Tao Liu11, Jian-Min Yang12, Jia Li13,14,15,16.
Abstract
Checkpoint kinase 1 inhibitors (CHK1i) have shown impressive single-agent efficacy in treatment of certain tumors, as monotherapy or potentiators of chemotherapy in clinical trials, but the sensitive tumor types and downstream effectors to dictate the therapeutic responses to CHK1i remains unclear. In this study we first analyzed GDSC (Genomics of Drug Sensitivity in Cancer) and DepMap database and disclosed that hematologic malignancies (HMs) were relatively sensitive to CHK1i or CHK1 knockdown. This notion was confirmed by examining PY34, a new and potent in-house selective CHK1i, which exhibited potent anti-HM effect in vitro and in vivo, as single agent. We demonstrated that the downregulation of c-Myc and its signaling pathway was the common transcriptomic profiling response of sensitive HM cell lines to PY34, whereas overexpressing c-Myc could partially rescue the anticancer effect of PY34. Strikingly, we revealed the significant correlations between downregulation of c-Myc and cell sensitivity to PY34 in 17 HM cell lines and 39 patient-derived cell (PDC) samples. Thus, our results demonstrate that HMs are more sensitive to CHK1i than solid tumors, and c-Myc downregulation could represent the CHK1i efficacy in HMs.Entities:
Keywords: CHK1 inhibitors; PY34; c-Myc; drug sensitivity; hematologic malignancies
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Year: 2021 PMID: 33782542 PMCID: PMC8724279 DOI: 10.1038/s41401-021-00652-1
Source DB: PubMed Journal: Acta Pharmacol Sin ISSN: 1671-4083 Impact factor: 6.150