TY - JOUR
T1 - Cell cycle plasticity driven by MTOR signaling
T2 - integral resistance to CDK4/6 inhibition in patient-derived models of pancreatic cancer
AU - Knudsen, Erik S.
AU - Kumarasamy, Vishnu
AU - Ruiz, Amanda
AU - Sivinski, Jared
AU - Chung, Sejin
AU - Grant, Adam
AU - Vail, Paris
AU - Chauhan, Shailender S.
AU - Jie, Tun
AU - Riall, Taylor S.
AU - Witkiewicz, Agnieszka K.
N1 - Funding Information:
Acknowledgements The authors thank all members of the laboratory group and colleagues in the discussion and preparation of this paper. The research was supported by a grant to AKW from the NCI.
Publisher Copyright:
© 2019, Springer Nature Limited.
PY - 2019/5/2
Y1 - 2019/5/2
N2 - Pancreatic ductal adenocarcinoma (PDAC), like many KRAS-driven tumors, preferentially loses CDKN2A that encodes an endogenous CDK4/6 inhibitor to bypass the RB-mediated cell cycle suppression. Analysis of a panel of patient-derived cell lines and matched xenografts indicated that many pancreatic cancers have intrinsic resistance to CDK4/6 inhibition that is not due to any established mechanism or published biomarker. Rather, there is a KRAS-dependent rapid adaptive response that leads to the upregulation of cyclin proteins, which participate in functional complexes to mediate resistance. In vivo, the degree of response is associated with the suppression of a gene expression signature that is strongly prognostic in pancreatic cancer. Resistance is associated with an adaptive gene expression signature that is common to multiple kinase inhibitors, but is attenuated with MTOR inhibitors. Combination treatment with MTOR and CDK4/6 inhibitors had potent activity across a large number of patient-derived models of PDAC underscoring the potential clinical efficacy.
AB - Pancreatic ductal adenocarcinoma (PDAC), like many KRAS-driven tumors, preferentially loses CDKN2A that encodes an endogenous CDK4/6 inhibitor to bypass the RB-mediated cell cycle suppression. Analysis of a panel of patient-derived cell lines and matched xenografts indicated that many pancreatic cancers have intrinsic resistance to CDK4/6 inhibition that is not due to any established mechanism or published biomarker. Rather, there is a KRAS-dependent rapid adaptive response that leads to the upregulation of cyclin proteins, which participate in functional complexes to mediate resistance. In vivo, the degree of response is associated with the suppression of a gene expression signature that is strongly prognostic in pancreatic cancer. Resistance is associated with an adaptive gene expression signature that is common to multiple kinase inhibitors, but is attenuated with MTOR inhibitors. Combination treatment with MTOR and CDK4/6 inhibitors had potent activity across a large number of patient-derived models of PDAC underscoring the potential clinical efficacy.
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U2 - 10.1038/s41388-018-0650-0
DO - 10.1038/s41388-018-0650-0
M3 - Article
C2 - 30696953
AN - SCOPUS:85060786753
SN - 0950-9232
VL - 38
SP - 3355
EP - 3370
JO - Oncogene
JF - Oncogene
IS - 18
ER -