Recent insights into targeting the IL-6 cytokine family in inflammatory diseases and cancer

Jones, Simon A.; Jenkins, Brendan J.

doi:10.1038/s41577-018-0066-7

Cited by 776 publications

(733 citation statements)

References 271 publications

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“…Classical IL‐6R signalling activity is mediated through the membrane‐bound IL‐6R complex and is limited to cells expressing both IL‐6Rα and gp130. In contrast, the IL‐6 trans‐signalling refers to processes including IL‐6 binding to a soluble IL‐6Rα (SIL‐6R) that maintains the circulating half‐life of IL‐6 and increases its bioavailability . IL‐6 trans‐signalling is now considered the main player in local IL‐6‐driven pathology and the hallmarks of inflammatory or degenerative forms of arthritis are primarily regulated by STAT3.…”

Section: Introductionmentioning

confidence: 99%

A directly GP130‐targeting small molecule ameliorates collagen‐induced arthritis (CIA) by inhibiting IL‐6/GP130 signalling and Th17 differentiation

Park

Kim

Heo

2020

Clin Exp Pharma Physio

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Rheumatoid arthritis is a chronic inflammatory disease associated with joint inflammation and destruction driven by T helper 17 (Th17) cells. Interleukin‐6 (IL‐6) is secreted by many cell types, including macrophages and synovial fibroblasts. It induces the differentiation and function of Th17 cells that can increase lymphocytic infiltration in the joint. LMT‐28 can suppress IL‐6 signalling through direct binding to glycoprotein‐130 and alleviate inflammatory diseases such as rheumatoid arthritis and inflammatory bowel disease. The purpose of this study was to assess whether LMT‐28 could potently inhibit Th17 differentiation and to determine the mechanism involved in the attenuating effect of LMT‐28 on rheumatoid arthritis through the IL‐6 signalling pathway. LMT‐28 reduced the arthritis score and showed protective effects against bone and cartilage destruction in collagen‐induced arthritis (CIA) mice. In mice with CIA, LMT‐28 markedly decreased serum levels of IL‐6, TNF and IL‐1β compared to vehicle control. Moreover, LMT‐28 attenuated Th17 cell activation in lymph nodes of CIA mice. We demonstrated that LMT‐28 suppressed differentiation of Th17 in mouse splenocytes and human peripheral blood mononuclear cells (PBMCs). Additionally, LMT‐28 inhibited phosphorylation of GP130, STAT3 and ERK induced by Hyper‐IL‐6 in human fibroblast‐like synoviocytes (FLS). Collectively, these results suggest that LMT‐28 can inhibit differentiated/activated‐Th17 cells in rheumatoid arthritis by blocking activation of the STAT3 pathway. LMT‐28 can attenuate rheumatoid arthritis by inhibiting differentiation/activation of Th17 cells and suppressing the proliferation and signalling activation of the IL‐6/solubleIL‐6 receptor complex stimulated FLS.

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Section: Introductionmentioning

confidence: 99%

A directly GP130‐targeting small molecule ameliorates collagen‐induced arthritis (CIA) by inhibiting IL‐6/GP130 signalling and Th17 differentiation

Park

Kim

Heo

2020

Clin Exp Pharma Physio

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“…Furthermore, we refer to the prospect of targeting ADAM17 versus sIL‐6R‐dependent trans‐signaling in LAC, the latter with existing antibody‐mediated therapeutic strategies. The rationale to target trans‐signaling in disease, rather than the “classic” IL‐6 signaling mode which is dependent on the membrane‐bound IL‐6R, is based on the opposing roles of IL‐6 in either maintaining homeostatic processes (e.g., regulation of B‐cell function, the acute phase response, and hematopoiesis), or conversely, driving chronic disease states such as inflammation and cancer (Scheller et al , ; Mihara et al , ; Jones & Jenkins, ). Here, IL‐6‐mediated homeostatic processes are facilitated by classic signaling, while the disease‐associated functions of IL‐6 primarily (or even exclusively) reside with trans‐signaling (Hunter & Jones, ; Jones & Jenkins, ).…”

Section: Discussionmentioning

confidence: 99%

“…The rationale to target trans‐signaling in disease, rather than the “classic” IL‐6 signaling mode which is dependent on the membrane‐bound IL‐6R, is based on the opposing roles of IL‐6 in either maintaining homeostatic processes (e.g., regulation of B‐cell function, the acute phase response, and hematopoiesis), or conversely, driving chronic disease states such as inflammation and cancer (Scheller et al , ; Mihara et al , ; Jones & Jenkins, ). Here, IL‐6‐mediated homeostatic processes are facilitated by classic signaling, while the disease‐associated functions of IL‐6 primarily (or even exclusively) reside with trans‐signaling (Hunter & Jones, ; Jones & Jenkins, ). Notably, the experimental mouse IL‐6R antibodies (1F7 and 25F10) used in our current study block IL‐6 trans‐signaling in the mouse, and have previously been reported to ameliorate tumorigenesis in the Kras G12D LAC model, albeit not as effectively as the robust anti‐tumor activity observed here with A17pro (Brooks et al , ).…”

Section: Discussionmentioning

confidence: 99%

“…Notably, the experimental mouse IL‐6R antibodies (1F7 and 25F10) used in our current study block IL‐6 trans‐signaling in the mouse, and have previously been reported to ameliorate tumorigenesis in the Kras G12D LAC model, albeit not as effectively as the robust anti‐tumor activity observed here with A17pro (Brooks et al , ). In addition, existing anti‐IL‐6R antibody therapies used in the clinic (and for that matter, also those against IL‐6), such as tocilizumab and sarilumab, block both protective (i.e., classic) and pathological (i.e., trans) signaling activities of IL‐6, causing side effects such as compromised host defense against bacteria (i.e., infections), imbalanced metabolism leading to higher blood cholesterol and triglyceride levels, and increased risk of gastrointestinal tract perforations (Rose‐John et al , ; Jones & Jenkins, ). Therefore, highly selective and potent ADAM17 inhibitors such as A17pro used in our current study, which specifically block pathological mouse/human trans‐signaling, promise to be more effective in suppressing disease states, including LAC, associated with IL‐6 trans‐signaling, and with less adverse effects.…”

Section: Discussionmentioning

confidence: 99%

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ADAM 17 selectively activates the IL ‐6 trans‐signaling/ ERK MAPK axis in KRAS ‐addicted lung cancer

et al. 2019

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Oncogenic KRAS mutations are major drivers of lung adenocarcinoma ( LAC ), yet the direct therapeutic targeting of KRAS has been problematic. Here, we reveal an obligate requirement by oncogenic KRAS for the ADAM 17 protease in LAC . In genetically engineered and xenograft (human cell line and patient‐derived) Kras G12D ‐driven LAC models, the specific blockade of ADAM 17, including with a non‐toxic prodomain inhibitor, suppressed tumor burden by reducing cellular proliferation. The pro‐tumorigenic activity of ADAM 17 was dependent upon its threonine phosphorylation by p38 MAPK , along with the preferential shedding of the ADAM 17 substrate, IL ‐6R, to release soluble IL ‐6R that drives IL ‐6 trans‐signaling via the ERK 1/2 MAPK pathway. The requirement for ADAM 17 in Kras G12D ‐driven LAC was independent of bone marrow‐derived immune cells. Furthermore, in KRAS mutant human LAC , there was a significant positive correlation between augmented phospho‐ ADAM 17 levels, observed primarily in epithelial rather than immune cells, and activation of ERK and p38 MAPK pathways. Collectively, these findings identify ADAM 17 as a druggable target for oncogenic KRAS ‐driven LAC and provide the rationale to employ ADAM 17‐based therapeutic strategies for targeting KRAS mutant cancers.

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“…IL-6 family consists of IL-6, IL-11, IL-27, IL-31, OSM, leukemia inhibitory factor (LIF), ciliary neurotrophic factor, cardiotrophin 1 and cardiotrophin-like cytokine factor 1 [4]. IL-6 family consists of IL-6, IL-11, IL-27, IL-31, OSM, leukemia inhibitory factor (LIF), ciliary neurotrophic factor, cardiotrophin 1 and cardiotrophin-like cytokine factor 1 [4].…”

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confidence: 99%

Oncostatin M expression in the mouse uterus during early pregnancy promotes embryo implantation and decidualization

Zheng

Zhang

et al. 2019

FEBS Letters

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Oncostatin M (OSM) is a member of the interleukin‐6 (IL‐6) family, which functions in embryo implantation and decidualization. The expression, function and regulation of Osm in mouse uteri during early pregnancy remain unknown. We show that Osm is mainly expressed in the uterine epithelium from days 1 to 4 of pregnancy and in decidual cells on day 5 of pregnancy. Osm promotes the attachment of Osm‐soaked blue beads, which mimic blastocysts, to a pseudopregnant mouse uterus. Prostaglandin E2 (PGE2)‐induced Osm in mouse uterine epithelial cells upregulates the levels of Il‐33 expression and phosphorylates Stat3. In vitro decidualization is significantly promoted by Osm. Our results indicate that PGE2‐induced Osm may mediate embryo implantation through Il‐33 and participate in decidualization via the Stat3‐Egr1 pathway.

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Recent insights into targeting the IL-6 cytokine family in inflammatory diseases and cancer

Cited by 776 publications

References 271 publications

A directly GP130‐targeting small molecule ameliorates collagen‐induced arthritis (CIA) by inhibiting IL‐6/GP130 signalling and Th17 differentiation

A directly GP130‐targeting small molecule ameliorates collagen‐induced arthritis (CIA) by inhibiting IL‐6/GP130 signalling and Th17 differentiation

ADAM 17 selectively activates the IL ‐6 trans‐signaling/ ERK MAPK axis in KRAS ‐addicted lung cancer

Oncostatin M expression in the mouse uterus during early pregnancy promotes embryo implantation and decidualization

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