FBXW7α attenuates inflammatory signalling by downregulating C/EBPδ and its target gene Tlr4

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作者
Kuppusamy Balamurugan
Shikha Sharan
Kimberly D. Klarmann
Youhong Zhang
Vincenzo Coppola
Glenn H. Summers
Thierry Roger
Deborah K. Morrison
Jonathan R. Keller
Esta Sterneck
机构
[1] Laboratory of Cell and Developmental Signalling,Department of MVIMG
[2] National Cancer Institute-Frederick,Department of Medicine
[3] PO Box B,undefined
[4] Frederick,undefined
[5] Maryland 21702-1201,undefined
[6] USA,undefined
[7] Basic Science Program,undefined
[8] SAIC-Frederick,undefined
[9] Inc.,undefined
[10] Laboratory of Cancer Prevention,undefined
[11] Frederick National Laboratory for Cancer Research,undefined
[12] PO Box B,undefined
[13] Frederick,undefined
[14] Maryland 21702-1201,undefined
[15] USA,undefined
[16] Wexner Medical Center,undefined
[17] Ohio State University-Comprehensive Cancer Center,undefined
[18] Ohio State University-CCC,undefined
[19] 988 Biological Research Tower 460 West 12th Avenue,undefined
[20] Laboratory Animal Sciences Program,undefined
[21] SAIC-Frederick,undefined
[22] NCI,undefined
[23] FNLCR,undefined
[24] Infectious Diseases Service,undefined
[25] Centre Hospitalier Universitaire Vaudois and University of Lausanne,undefined
来源
Nature Communications | / 4卷
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摘要
Toll-like receptor 4 (Tlr4) has a pivotal role in innate immune responses, and the transcription factor CCAAT/enhancer binding protein delta (C/EBPδ, Cebpd) is a Tlr4-induced gene. Here we identify a positive feedback loop in which C/EBPδ activates Tlr4 gene expression in macrophages and tumour cells. In addition, we discovered a negative feedback loop whereby the tumour suppressor FBXW7α (FBW7, Cdc4), whose gene expression is inhibited by C/EBPδ, targets C/EBPδ for degradation when C/EBPδ is phosphorylated by GSK-3β. Consequently, FBXW7α suppresses Tlr4 expression and responses to the ligand lipopolysaccharide. FBXW7α depletion alone is sufficient to augment pro-inflammatory signalling in vivo. Moreover, as inflammatory pathways are known to modulate tumour biology, Cebpd null mammary tumours, which have reduced metastatic potential, show altered expression of inflammation-associated genes. Together, these findings reveal a role for C/EBPδ upstream of Tlr4 signalling and uncover a function for FBXW7α as an attenuator of inflammatory signalling.
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