| Literature DB >> 28954237 |
Jungeun Sarah Kwon1, Nicholas J Everetts1, Xia Wang1, Weikang Wang2, Kimiko Della Croce1, Jianhua Xing3, Guang Yao4.
Abstract
Quiescence is a non-proliferative cellular state that is critical to tissue repair and regeneration. Although often described as the G0 phase, quiescence is not a single homogeneous state. As cells remain quiescent for longer durations, they move progressively deeper and display a reduced sensitivity to growth signals. Deep quiescent cells, unlike senescent cells, can still re-enter the cell cycle under physiological conditions. Mechanisms controlling quiescence depth are poorly understood, representing a currently underappreciated layer of complexity in growth control. Here, we show that the activation threshold of a Retinoblastoma (Rb)-E2F network switch controls quiescence depth. Particularly, deeper quiescent cells feature a higher E2F-switching threshold and exhibit a delayed traverse through the restriction point (R-point). We further show that different components of the Rb-E2F network can be experimentally perturbed, following computer model predictions, to coarse- or fine-tune the E2F-switching threshold and drive cells into varying quiescence depths.Entities:
Keywords: Rb-E2F pathway; activation threshold; bistable switch; cell cycle entry; cell growth; cell proliferation; cellular quiescence; model simulation; quiescence depth; quiescence heterogeneity
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Year: 2017 PMID: 28954237 PMCID: PMC6571029 DOI: 10.1016/j.celrep.2017.09.007
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423