regulatory network analyses reveal genome-wide potentiation of lif signaling by glucocorticoids and define an innate cell defense response监管网络分析揭示基因组势差现象制药业信号由糖皮质激素和定义一个天生的细胞防御反应.pdfVIP
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regulatory network analyses reveal genome-wide potentiation of lif signaling by glucocorticoids and define an innate cell defense response监管网络分析揭示基因组势差现象制药业信号由糖皮质激素和定义一个天生的细胞防御反应
Regulatory Network Analyses Reveal Genome-Wide
Potentiation of LIF Signaling by Glucocorticoids and
Define an Innate Cell Defense Response
´
David Langlais, Catherine Couture, Aurelio Balsalobre*, Jacques Drouin*
´ ´ ´ ´ ´
Laboratoire de Genetique Moleculaire, Institut de Recherches Cliniques de Montreal (IRCM), Montreal, Quebec, Canada
Abstract
While the hypothalamo-pituitary-adrenal axis (HPA) activates a general stress response by increasing glucocorticoid (Gc)
synthesis, biological stress resulting from infections triggers the inflammatory response through production of cytokines.
The pituitary gland integrates some of these signals by responding to the pro-inflammatory cytokines IL6 and LIF and to a
negative Gc feedback loop. The present work used whole-genome approaches to define the LIF/STAT3 regulatory network
and to delineate cross-talk between this pathway and Gc action. Genome-wide ChIP-chip identified 3,449 STAT3 binding
sites, whereas 2,396 genes regulated by LIF and/or Gc were found by expression profiling. Surprisingly, LIF on its own
changed expression of only 85 genes but the joint action of LIF and Gc potentiated the expression of more than a thousand
genes. Accordingly, activation of both LIF and Gc pathways also potentiated STAT3 and GR recruitment to many STAT3
targets. Our analyses revealed an unexpected gene cluster that requires both stimuli for delayed activation; 83% of the
genes in this cluster are involved in different cell defense mechanisms. Thus, stressors that trigger both general stress and
inflammatory responses lead to activation of a stereotypic innate cellular defense response.
Citation: Langlais D, Couture C, Balsalobre A, Drouin J (2008) Regulatory N
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