Systematic analysis of the
            <scp>IL</scp>
            ‐17 receptor signalosome reveals a robust regulatory feedback loop

Draberova, Helena; Janusova, Sarka; Knizkova, Daniela; Šemberová, Tereza; Pribikova, Michaela; Ujevic, Andrea; Harant, Karel; Knápková, Sofija; Hrdinka, Matouš; Fanfani, Viola; Stracquadanio, Giovanni; Drobek, Ales; Ruppova, Klara; Štěpánek, Ondřej; Dráber, Peter

doi:10.15252/embj.2019104202

Cited by 24 publications

(17 citation statements)

References 93 publications

(166 reference statements)

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“…One possibility is that HOIL1 plays a cell-intrinsic role in regulating ILC2, and this would be consistent with a requirement for HOIL1 in radiation-resistant, non-bone marrow-derived cells, since some ILC2 are thought to self-renew in tissues 40 . A recent study identified LUBAC as a component of the IL17RA/IL17RC receptor signaling complex (RSC) required for efficient signal transduction and NFκB activation 41 . The same study identified a negative feedback loop for the IL-17RSC, although LUBAC did not appear to be involved.…”

Section: Discussionmentioning

confidence: 99%

HOIL1 regulates group 2 innate lymphoid cell numbers and type 2 inflammation in the small intestine

et al. 2022

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Patients with mutations in HOIL1 experience a complex immune disorder including intestinal inflammation. To investigate the role of HOIL1 in regulating intestinal inflammation, we employed a mouse model of partial HOIL1 deficiency. The ileum of HOIL1-deficient mice displayed features of type 2 inflammation including tuft cell and goblet cell hyperplasia, and elevated expression of Il13, Il5 and Il25 mRNA. Inflammation persisted in the absence of T and B cells, and bone marrow chimeric mice revealed a requirement for HOIL1 expression in radiation-resistant cells to regulate inflammation. Although disruption of IL-4 receptor alpha (IL4Rα) signaling on intestinal epithelial cells ameliorated tuft and goblet cell hyperplasia, expression of Il5 and Il13 mRNA remained elevated. KLRG1hi CD90lo group 2 innate lymphoid cells were increased independent of IL4Rα signaling, tuft cell hyperplasia and IL-25 induction. Antibiotic treatment dampened intestinal inflammation indicating commensal microbes as a contributing factor. We have identified a key role for HOIL1, a component of the Linear Ubiquitin Chain Assembly Complex, in regulating type 2 inflammation in the small intestine. Understanding the mechanism by which HOIL1 regulates type 2 inflammation will advance our understanding of intestinal homeostasis and inflammatory disorders and may lead to the identification of new targets for treatment.

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Section: Discussionmentioning

confidence: 99%

HOIL1 regulates group 2 innate lymphoid cell numbers and type 2 inflammation in the small intestine

et al. 2022

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“…The microglia are a subtype of glial-immune sentinel cells in retina and highly express receptor for IL-17 in STZ-injected or OIR mice. Among the five receptors for IL-17 (IL17RA to IL-17RE), IL-17 has been shown to bind IL-17RA with high affinity and IL-17RA receptor has been shown to associate with other receptor such as IL-17RC, forming a IL-17R complex (Draberova et al, 2020). In the retina, IL-17RA and IL-17RC could be found to express on microglia, Muller cells, and astrocytes (Ke et al, 2009).…”

Section: Discussionmentioning

confidence: 99%

IL‐17 signaling induces iNOS+ microglia activation in retinal vascular diseases

Zhou

Liang

Yang

et al. 2021

Glia

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Activation of microglia and inflammation-mediated vascular damages are suggested to play a decisive role in the pathogenesis of various retinopathies. The inducible nitric oxide synthase (iNOS) was required for activated microglia-mediated injuries.However, the induction mechanism of microglia activation during retinal vascular diseases is still elusive. Here we showed that IL-17 induced microglia activation with high expression of iNOS and promoted the development of retinal vascular diseases.

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“…Act1 controls both the transcriptional as well as the post-transcriptional regulation of IL-17 responsive genes, by recruiting and activating different TRAF proteins (TRAF6, TRAF2), and also by directly interacting with RNAs ( Li et al, 2019 ). According to a recent study, the IL-17A/IL-17RA/IL-17RC heterotrimeric receptor recruits approximately six ACT1 molecules, which provide high-avidity docking sites for TRAF6 homotrimers ( Draberova et al, 2020 ). Non-degradative K63-linked polyubiquitination of TRAF6 by Act1 leads to the recruitment of downstream adaptor (ABIN1, TAX1BP1, TANK, NAP1), effector (TAK1, LUBAC, NEMO/IKKα/IKKβ), and regulatory proteins (IKKε, TBK1, A20, Cullin1, β-TrCP1/2) and ultimately to the activation of the NF-κB and MAP kinase pathways ( Amatya et al, 2017 ; Li et al, 2019 ; Draberova et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

IL-17-induced dimerization of IL-17RA drives the formation of the IL-17 signalosome to potentiate signaling

et al. 2022

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Systematic analysis of the IL ‐17 receptor signalosome reveals a robust regulatory feedback loop

Cited by 24 publications

References 93 publications

HOIL1 regulates group 2 innate lymphoid cell numbers and type 2 inflammation in the small intestine

HOIL1 regulates group 2 innate lymphoid cell numbers and type 2 inflammation in the small intestine

IL‐17 signaling induces iNOS+ microglia activation in retinal vascular diseases

IL-17-induced dimerization of IL-17RA drives the formation of the IL-17 signalosome to potentiate signaling

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