Intestinal myofibroblast-specific Tpl2-Cox-2-PGE
            <sub>2</sub>
            pathway links innate sensing to epithelial homeostasis

Roulis, Manolis; Nikolaou, Christoforos; Kotsaki, Elena; Kaffe, Eleanna; Karagianni, Niki; Koliaraki, Vasiliki; Salpea, Klelia D.; Ragoussis, Jiannis; Aidinis, Vassilis; Martini, Eva; Becker, Christoph; Herschman, Harvey R.; Vetrano, Stefania; Danese, Silvio; Kollias, George

doi:10.1073/pnas.1415762111

Cited by 86 publications

(83 citation statements)

References 54 publications

(68 reference statements)

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“…The secretion of PGE2 by adipocytes was also reduced in these experimental conditions. Thus, our data indicate that Tpl2 in adipocytes is a positive regulator of COX-2 expression and PGE2 production as previously shown in macrophages, T cells and intestinal myofibroblasts (35,39,46). By contrast, in other cellular contexts Tpl2 negatively regulates COX-2 expression and PGE2 production (37).…”

Section: Discussionsupporting

confidence: 87%

The Tpl2 Kinase Regulates the COX-2/Prostaglandin E2 Axis in Adipocytes in Inflammatory Conditions

Berthou

Ceppo

Dumas

et al. 2015

Molecular Endocrinology

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Bioactive lipid mediators such as prostaglandin E2 (PGE2) have emerged as potent regulator of obese adipocyte inflammation and functions. PGE2 is produced by cyclooxygenases (COXs) from arachidonic acid, but inflammatory signaling pathways controlling COX-2 expression and PGE2 production in adipocytes remain ill-defined. Here, we demonstrated that the MAP kinase kinase kinase tumor progression locus 2 (Tpl2) controls COX-2 expression and PGE2 secretion in adipocytes in response to different inflammatory mediators. We found that pharmacological- or small interfering RNA-mediated Tpl2 inhibition in 3T3-L1 adipocytes decreased by 50% COX-2 induction in response to IL-1β, TNF-α, or a mix of the 2 cytokines. PGE2 secretion induced by the cytokine mix was also markedly blunted. At the molecular level, nuclear factor κB was required for Tpl2-induced COX-2 expression in response to IL-1β but was inhibitory for the TNF-α or cytokine mix response. In a coculture between adipocytes and macrophages, COX-2 was mainly increased in adipocytes and pharmacological inhibition of Tpl2 or its silencing in adipocytes markedly reduced COX-2 expression and PGE2 secretion. Further, Tpl2 inhibition in adipocytes reduces by 60% COX-2 expression induced by a conditioned medium from lipopolysaccharide (LPS)-treated macrophages. Importantly, LPS was less efficient to induce COX-2 mRNA in adipose tissue explants of Tpl2 null mice compared with wild-type and Tpl2 null mice displayed low COX-2 mRNA induction in adipose tissue in response to LPS injection. Collectively, these data established that activation of Tpl2 by inflammatory stimuli in adipocytes and adipose tissue contributes to increase COX-2 expression and production of PGE2 that could participate in the modulation of adipose tissue inflammation during obesity.

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Section: Discussionsupporting

confidence: 87%

The Tpl2 Kinase Regulates the COX-2/Prostaglandin E2 Axis in Adipocytes in Inflammatory Conditions

Berthou

Ceppo

Dumas

et al. 2015

Molecular Endocrinology

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“…20,21 Map3k8 plays a unique role in the production of inflammatory mediators in vivo, 14,19,22 modifying the activation state of macrophages, monocytes, astrocytes, dendritic cells, stellate cells, myofibroblasts, and plasma cells, and no other protein can replace Map3k8 in this role. 16,18,[23][24][25][26][27][28][29] We show here that, in atherogenic conditions, Map3k8 is required to maintain the number of monocytes, by limiting apoptosis. Furthermore, the strong expression of CCR2 on Ly6C high monocytes and the firm adhesion of leukocytes to arterioles and venules in vivo are dependent on Map3k8.…”

Section: Ly6cmentioning

confidence: 60%

Map3k8 Modulates Monocyte State and Atherogenesis in ApoE ^−/− Mice

Sanz‐Garcia

Sánchez

Contreras‐Jurado

et al. 2017

ATVB

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“…In contrast, TPL2 in myofibroblasts protects from epithelial injury-induced colitis. 44 Therefore, given the distinct role of TPL2 in different cell types during various forms of intestinal inflammation, it will be important to clearly dissect the outcomes of TPL2 signalling in a variety of IBD-relevant cell types.…”

Section: Discussionmentioning

confidence: 99%

ATPL2 (MAP3K8)disease-risk polymorphism increases TPL2 expression thereby leading to increased pattern recognition receptor-initiated caspase-1 and caspase-8 activation, signalling and cytokine secretion

Hedl

Abraham

2015

Gut

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Objective IBD is characterised by dysregulated intestinal immune homeostasis and cytokine secretion. In the intestine, properly regulating pattern recognition receptor (PRR)-mediated signalling and cytokines is crucial given the ongoing host–microbial interactions. TPL2 (MAP3K8, COT) contributes to PRR-initiated pathways, yet the mechanisms for TPL2 signalling contributions in primary human myeloid cells are incompletely understood and its role in intestinal myeloid cells is poorly defined. Furthermore, functional consequences for the IBD-risk locus rs1042058 in TPL2 are unknown. Methods We analysed protein, cytokine and RNA expression, and signalling in human monocyte-derived macrophages (MDMs) through western blot, ELISA, real-time PCR and flow cytometry. Results PRR-induced cytokine secretion was increased in MDMs from rs1042058 TPL2 GG risk individuals. TPL2 activation by the Crohn's disease-associated PRR nucleotide-oligomerisation domain (NOD)2 required PKC, and IKKβ, IKKα and IKKγ signalling. TPL2, in turn, significantly enhanced NOD2-induced ERK, JNK and NFκB signalling. We found that another major mechanism for the TPL2 contribution to NOD2 signalling was through ERK-dependent and JNK-dependent caspase-1 and caspase-8 activation, which in turn, led to early autocrine interleukin (IL)-1β and IL-18 secretion and amplification of long-term cytokines. Importantly, Salmonella typhimurium-induced cytokines from human intestinal myeloid-derived cells required TPL2 as well as autocrine IL-1β and IL-18. Finally, rs1042058 GG risk carrier MDMs from healthy individuals and patients with Crohn's disease had increased TPL2 expression and NOD2-initiated TPL2 phosphorylation, ERK, JNK and NFκB activation, and early autocrine IL-1β and IL-18 secretion. Conclusions Taken together, the rs1042058 GG IBD-risk polymorphism in TPL2 results in a gain-of-function by increasing TPL2 expression and signalling, thereby amplifying PRR-initiated outcomes.

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Intestinal myofibroblast-specific Tpl2-Cox-2-PGE ₂ pathway links innate sensing to epithelial homeostasis

Cited by 86 publications

References 54 publications

The Tpl2 Kinase Regulates the COX-2/Prostaglandin E2 Axis in Adipocytes in Inflammatory Conditions

The Tpl2 Kinase Regulates the COX-2/Prostaglandin E2 Axis in Adipocytes in Inflammatory Conditions

Map3k8 Modulates Monocyte State and Atherogenesis in ApoE ^−/− Mice

ATPL2 (MAP3K8)disease-risk polymorphism increases TPL2 expression thereby leading to increased pattern recognition receptor-initiated caspase-1 and caspase-8 activation, signalling and cytokine secretion

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Intestinal myofibroblast-specific Tpl2-Cox-2-PGE 2 pathway links innate sensing to epithelial homeostasis

Cited by 86 publications

References 54 publications

The Tpl2 Kinase Regulates the COX-2/Prostaglandin E2 Axis in Adipocytes in Inflammatory Conditions

The Tpl2 Kinase Regulates the COX-2/Prostaglandin E2 Axis in Adipocytes in Inflammatory Conditions

Map3k8 Modulates Monocyte State and Atherogenesis in ApoE −/− Mice

ATPL2 (MAP3K8)disease-risk polymorphism increases TPL2 expression thereby leading to increased pattern recognition receptor-initiated caspase-1 and caspase-8 activation, signalling and cytokine secretion

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Intestinal myofibroblast-specific Tpl2-Cox-2-PGE ₂ pathway links innate sensing to epithelial homeostasis

Map3k8 Modulates Monocyte State and Atherogenesis in ApoE ^−/− Mice