Identification of a truncated splice variant of IL-18 receptor alpha in the human and rat, with evidence of wider evolutionary conservation

Booker, Chris S.; Grattan, David R.

doi:10.7717/peerj.560

Cited by 7 publications

(6 citation statements)

References 63 publications

(82 reference statements)

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“…The iHS test, aimed at defining evidence of recent positive selection, detected selective sweeps for three tightly linked SNPs in the IL18R1 gene, which encodes a cytokine receptor from the interleukin 1 receptor family. It has been previously discussed that the conserved across evolutionary branches mechanism of regulating IL18 signaling might represent a target for selective pressure 40 . This assumption is consistent with the fact that the top IL18R1 SNP rs2001461 (iHS CEU score 4.54) was associated with the IL18R1 expression (GWAS trait P value = 3.00E−129).…”

Section: Discussionmentioning

confidence: 99%

Cytokines mapping for tissue-specific expression, eQTLs and GWAS traits

Salnikova

Khadzhieva

Kolobkov

et al. 2020

Sci Rep

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Dysregulation in cytokine production has been linked to the pathogenesis of various immune-mediated traits, in which genetic variability contributes to the etiopathogenesis. GWA studies have identified many genetic variants in or near cytokine genes, nonetheless, the translation of these findings into knowledge of functional determinants of complex traits remains a fundamental challenge. In this study we aimed at collection, analysis and interpretation of data on cytokines focused on their tissue-specific expression, eQTLs and GWAS traits. Using GO annotations, we generated a list of 314 cytokines and analyzed them with the GTEx resource. Cytokines were highly tissue-specific, 82.3% of cytokines had Tau expression metrics ≥ 0.8. In total, 3077 associations for 1760 unique SNPs in or near 244 cytokines were mapped in the NHGRI-EBI GWAS Catalog. According to the Experimental Factor Ontology resource, the largest numbers of disease associations were related to ‘Inflammatory disease’, ‘Immune system disease’ and ‘Asthma’. The GTEx-based analysis revealed that among GWAS SNPs, 1142 SNPs had eQTL effects and influenced expression levels of 999 eGenes, among them 178 cytokines. Several types of enrichment analysis showed that it was cytokines expression variability that fundamentally contributed to the molecular origins of considered immune-mediated conditions.

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Section: Discussionmentioning

confidence: 99%

Cytokines mapping for tissue-specific expression, eQTLs and GWAS traits

Salnikova

Khadzhieva

Kolobkov

et al. 2020

Sci Rep

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“…It is well established that IL18 mediates its biological effects in a variety of organ systems and cell types 9 through stepwise binding to IL18R1 and IL18RAP, and subsequent juxtaposition of the intracellular toll/interleukin-1 receptor (TIR) domains of both receptors 50 . However, additional truncated variants of IL18R1 and IL18RAP, lacking this domain essential for recruitment of MYD88 adaptor protein and subsequent activation of (NF)-ΚΒ and MAPK pathways, have been reported in humans and rodents (arbitrary named type II receptors) 10 11 51 . Though their exact role is yet to be fully established, they are proposed to act as competitors of the canonical receptors in heterodimer formation thereby inhibiting IL18 actions 10 11 .…”

Section: Discussionmentioning

confidence: 99%

Divergent responses to thermogenic stimuli in BAT and subcutaneous adipose tissue from interleukin 18 and interleukin 18 receptor 1-deficient mice

Pazos

Lima

Tovar

et al. 2015

Sci Rep

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Brown and beige adipocytes recruitment in brown (BAT) or white adipose tissue, mainly in the inguinal fat pad (iWAT), meet the need for temperature adaptation in cold-exposure conditions and protect against obesity in face of hypercaloric diets. Using interleukin18 (Il18) and Il18 receptor 1- knockout (Il18r1-KO) mice, this study aimed to investigate the role of IL18 signaling in BAT and iWAT activation and thermogenesis under both stimuli. Il18-KO, extremely dietary obesity-prone as previously described, failed to develop diet-induced thermogenesis as assessed by BAT and iWAT Ucp1 mRNA levels. Overweight when fed standard chow but not HFD, HFD-fed Il18r1-KO mice exhibited increased iWAT Ucp1 gene expression. Energy expenditure was reduced in pre-obese Il18r1-KO mice and restored upon HFD-challenge. Cold exposure lead to similar results; Il18r1-KO mice were protected against acute body temperature drop, displaying a more brown-like structure, alternative macrophage activation and thermogenic gene expression in iWAT than WT controls. Opposite effects were observed in Il18-KO mice. Thus, Il18 and Il18r1 genetic ablation disparate effects on energy homeostasis are likely mediated by divergent BAT responses to thermogenic stimuli as well as iWAT browning. These results suggest that a more complex receptor-signaling system mediates the IL18 adipose-tissue specific effects in energy expenditure.

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“…Their function has not been clarified, and there is no information as to whether they are generated by alternative splicing or proteolytic cleavage. IL‐1R5 can undergo alternative splicings that generate soluble receptors in mice and rats and a non‐signaling membrane receptor, similar to IL‐1R2, in humans . Both sIL‐1R5 and sIL‐1R7, forming complexes with IL‐18, have been found at increased levels in the serum of patients with rheumatoid arthritis and adult‐onset Still's disease .…”

Section: Regulation In the Il‐1r Familymentioning

confidence: 99%

“…IL-1R5 can undergo alternative splicings that generate soluble receptors in mice and rats and a non-signaling membrane receptor, similar to IL-1R2, in humans. 380,381 Both sIL-1R5 and sIL-1R7, forming complexes with IL-18, have been found at increased levels in the serum of patients with rheumatoid arthritis and adult-onset Still's disease. 188 In mice, it has been shown that sIL-1R7 worsens experimental arthritis through upregulation of Th17 activation and concomitant downregulation of Th1, Th2, and Treg activity, 382 but whether this effect has anything to do with IL-18 inhibition is not known.…”

Section: Soluble Forms Of Il-1r5 and Il-1r7 The Receptor And Co-recementioning

confidence: 99%

The family of the interleukin‐1 receptors

Boraschi

Italiani

Weil

et al. 2017

Immunological Reviews

246

219

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The extracellular forms of the IL-1 cytokines are active through binding to specific receptors on the surface of target cells. IL-1 ligands bind to the extracellular portion of their ligand-binding receptor chain. For signaling to take place, a non-binding accessory chain is recruited into a heterotrimeric complex. The intracellular approximation of the Toll-IL-1-receptor (TIR) domains of the 2 receptor chains is the event that initiates signaling. The family of IL-1 receptors (IL-1R) includes 10 structurally related members, and the distantly related soluble protein IL-18BP that acts as inhibitor of the cytokine IL-18. Over the years the receptors of the IL-1 family have been known with many different names, with significant confusion. Thus, we will use here a recently proposed unifying nomenclature. The family includes several ligand-binding chains (IL-1R1, IL-1R2, IL-1R4, IL-1R5, and IL-1R6), 2 types of accessory chains (IL-1R3, IL-1R7), molecules that act as inhibitors of signaling (IL-1R2, IL-1R8, IL-18BP), and 2 orphan receptors (IL-1R9, IL-1R10). In this review, we will examine how the receptors of the IL-1 family regulate the inflammatory and anti-inflammatory functions of the IL-1 cytokines and are, more at large, involved in modulating defensive and pathological innate immunity and inflammation. Regulation of the IL-1/IL-1R system in the brain will be also described, as an example of the peculiarities of organ-specific modulation of inflammation.

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Identification of a truncated splice variant of IL-18 receptor alpha in the human and rat, with evidence of wider evolutionary conservation

Cited by 7 publications

References 63 publications

Cytokines mapping for tissue-specific expression, eQTLs and GWAS traits

Cytokines mapping for tissue-specific expression, eQTLs and GWAS traits

Divergent responses to thermogenic stimuli in BAT and subcutaneous adipose tissue from interleukin 18 and interleukin 18 receptor 1-deficient mice

The family of the interleukin‐1 receptors

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