Dynamic NF-κB and E2F interactions control the priority and timing of inflammatory signalling and cell proliferation.
John M AnkersRaheela AwaisNicholas A JonesJames BoydSheila RyanAntony D AdamsonClaire V HarperLloyd BridgeDavid G SpillerDean A JacksonPawel PaszekViolaine SéeMichael R H WhitePublished in: eLife (2016)
Dynamic cellular systems reprogram gene expression to ensure appropriate cellular fate responses to specific extracellular cues. Here we demonstrate that the dynamics of Nuclear Factor kappa B (NF-κB) signalling and the cell cycle are prioritised differently depending on the timing of an inflammatory signal. Using iterative experimental and computational analyses, we show physical and functional interactions between NF-κB and the E2 Factor 1 (E2F-1) and E2 Factor 4 (E2F-4) cell cycle regulators. These interactions modulate the NF-κB response. In S-phase, the NF-κB response was delayed or repressed, while cell cycle progression was unimpeded. By contrast, activation of NF-κB at the G1/S boundary resulted in a longer cell cycle and more synchronous initial NF-κB responses between cells. These data identify new mechanisms by which the cellular response to stress is differentially controlled at different stages of the cell cycle.
Keyphrases
- cell cycle
- nuclear factor
- cell proliferation
- signaling pathway
- pi k akt
- toll like receptor
- lps induced
- oxidative stress
- gene expression
- induced apoptosis
- inflammatory response
- physical activity
- magnetic resonance
- dna methylation
- magnetic resonance imaging
- computed tomography
- machine learning
- endoplasmic reticulum stress
- electronic health record
- heat stress
- deep learning
- cell death
- dual energy