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Control of Expression of Key Cell Cycle Enzymes Drives Cell Line-Specific Functions of CDK7 in Human PDAC Cells

Lina Kolloch, Teresa Kreinest, Michael Meisterernst, Andrea Oeckinghaus

2022International Journal of Molecular Sciences12 citationsDOIOpen Access PDF

Abstract

Inhibition of the dual function cell cycle and transcription kinase CDK7 is known to affect the viability of cancer cells, but the mechanisms underlying cell line-specific growth control remain poorly understood. Here, we employed a previously developed, highly specific small molecule inhibitor that non-covalently blocks ATP binding to CDK7 (LDC4297) to study the mechanisms underlying cell line-specific growth using a panel of genetically heterogeneous human pancreatic tumor lines as model system. Although LDC4297 diminished both transcription rates and CDK T-loop phosphorylation in a comparable manner, some PDAC lines displayed significantly higher sensitivity than others. We focused our analyses on two well-responsive lines (Mia-Paca2 and Panc89) that, however, showed significant differences in their viability upon extended exposure to limiting LDC4297 concentrations. Biochemical and RNAseq analysis revealed striking differences in gene expression and cell cycle control. Especially the downregulation of a group of cell cycle control genes, among them CDK1/2 and CDC25A/C, correlated well to the observed viability differences in Panc89 versus Mia-Paca2 cells. A parallel downregulation of regulatory pathways supported the hypothesis of a feedforward programmatic effect of CDK7 inhibitors, eventually causing hypersensitivity of PDAC lines.

Topics & Concepts

Cyclin-dependent kinase 1BiologyCell cultureCell cycleDownregulation and upregulationCyclin-dependent kinaseCell growthCell biologyViability assayGene expressionCyclin-dependent kinase 7CellMolecular biologyGeneBiochemistryGeneticsCyclin-dependent kinase 2Pancreatic and Hepatic Oncology ResearchCancer-related Molecular PathwaysEpigenetics and DNA Methylation
Control of Expression of Key Cell Cycle Enzymes Drives Cell Line-Specific Functions of CDK7 in Human PDAC Cells | Litcius