CDK7 Inhibition Potentiates Genome Instability Triggering Anti-tumor Immunity in Small Cell Lung Cancer.

Hua Zhang,Camilla L. Christensen,Ruben Dries,Matthew Oser,Jiehui Deng,Brian Diskin,Fei Li,Yuanwang Pan,Xuzhu Zhang,Yandong Yin,Eleni Papadopoulos,Val Pyon,Cassandra Thakurdin,Nicholas Kwiatkowski,Kandarp Jani,Alexandra R. Rabin,Dayanne M. Castro,Ting Chen,Heather Silver,Qingyuan Huang,Mirna Bulatovic,Catríona M. Dowling,Belen Sundberg,Alan L. Leggett,Michela Ranieri,Han Han,Shuai Li,Annan Yang,Kristen E. Labbe,Christina Almonte,Vladislav O. Sviderskiy,Max M. Quinn,Jack Donaghue,Eric S. Wang,Tinghu Zhang,Zhixiang He,V Velcheti,Peter S. Hammerman,Gordon J. Freeman,Richard Bonneau,William G. Kaelin,Kate D. Sutherland,Ariena Kersbergen,Andrew J. Aguirre,Guo-Cheng Yuan,Eli Rothenberg,George Miller,Nathanael S. Gray,Kwok-Kin Wong

CDK7 Inhibition Potentiates Genome Instability Triggering Anti-tumor Immunity in Small Cell Lung Cancer.

2020

Summary Cyclin-dependent kinase 7 (CDK7) is a central regulator of the cell cycle and gene transcription. However, little is known about its impact on genomic instability and cancer immunity. Using a selective CDK7 inhibitor, YKL-5-124, we demonstrated that CDK7 inhibition predominately disrupts cell-cycle progression and induces DNA replication stress and genome instability in small cell lung cancer (SCLC) while simultaneously triggering immune-response signaling. These tumor-intrinsic events provoke a robust immune surveillance program elicited by T cells, which is further enhanced by the addition of immune-checkpoint blockade. Combining YKL-5-124 with anti-PD-1 offers significant survival benefit in multiple highly aggressive murine models of SCLC, providing a rationale for new combination regimens consisting of CDK7 inhibitors and immunotherapies.

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