Immunogenetics of juvenile idiopathic arthritis: A comprehensive review

Hersh, Aimee O.; Prahalad, Sampath

doi:10.1016/j.jaut.2015.08.002

Cited by 110 publications

(94 citation statements)

References 99 publications

(115 reference statements)

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“…Besides that, some mechanisms remain largely unknown, such as causal nucleotide changes, rare genetic variants or the missing heritability sequencing [19][20][21]. Indeed, the use of GWAS have been very disappointing, i.e., it is likely that there are loci that have not been identified due to a lack of statistical significance; this is true not only of PBC, but also for a variety of other AIDs, many of which have been recently reviewed [22][23][24][25][26][27][28][29][30][31][32][33]. As a consequence, progress towards understanding disease mechanisms has been limited by difficulties in assigning a molecular function to the vast majority of GWAS hits that do not affect protein-coding sequences.…”

Section: Introductionmentioning

confidence: 99%

The epigenetics of PBC: The link between genetic susceptibility and environment

Marzorati

Lleo

Carbone

et al. 2016

Clinics and Research in Hepatology and Gastroenterology

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Section: Introductionmentioning

confidence: 99%

The epigenetics of PBC: The link between genetic susceptibility and environment

Marzorati

Lleo

Carbone

et al. 2016

Clinics and Research in Hepatology and Gastroenterology

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“…Functional gene enrichment analysis (DAVID) of JIA relapse (n=6) or remission (n=6) patients versus healthy individuals (n=3) identified 5 common disease centric pathways that persisted from prior to after withdrawal of therapy (online supplementary Figure S5 and Table S4-5). Dysregulation in UBE2L3, IL-6, STAT4, TYK2, TNFAIP3 and PTPN2 were found in both relapse and remission individuals, have been previously associated with JIA [21,22]. We examined through Cytoscape and Reactome database for the gene associations involved in the 5 pathways (Figure 5A-E Table S3 and 6).…”

Section: Transcriptomic Divergence In Disease Centric Pathways That Pmentioning

confidence: 99%

An immunome perturbation is present in juvenile idiopathic arthritis patients who are in remission and will relapse upon anti-TNFα withdrawal

Leong

Chen

Yeo

et al. 2019

Preprint

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ObjectivesBiologics treatment with anti-TNFα is efficacious in juvenile idiopathic arthritic (JIA) patients. Despite displaying clinical inactivity during treatment, many patients will flare upon cessation of therapy. The inability to definitively discriminate patients who will relapse or continue to remain in remission after therapy withdrawal is currently a major unmet medical need. CD4 T cells have been implicated in active disease, yet how they contribute to disease persistence despite treatment is unknown.MethodsWe interrogated the circulatory reservoir of CD4+ immune subsets at the single cell resolution with mass cytometry (CyToF) of JIA patients (n=20) who displayed continuous clinical inactivity for at least 6 months with anti-TNFα, and were subsequently withdrawn from therapy for 8 months, and scored as relapse or remission. These patients were examined prior to therapy withdrawal for putative subsets that could discriminate relapse from remission. We verified on a separate JIA cohort (n=16), the continued dysregulation of these circulatory subsets 8 months into therapy withdrawal. The immunological transcriptomic signature of CD4 memory in relapse/remission patients was examined with Nanostring.ResultsAn inflammatory memory subset of CD3+CD4+CD45RA−TNFα+ T cells deficient in immune checkpoints (PD1−CD152−) was present in relapse patients prior to therapy withdrawal. Transcriptomic profiling reveals divergence between relapse and remission patients in disease centric pathways involving (a) TCR activation, (b) apoptosis, (c) TNFα, (d) NF-kB and (e) MAPK signalling.ConclusionsA unique discriminatory immunomic and transcriptomic signature is associated with relapse patients and may explain how relapse occurs.

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“…Furthermore, the presence of TNF, IL-6 and IL-1β strongly points to the involvement of macrophages-particularly type-I macrophages (M1 MØ) which, when activated, produce this combination of cytokines. Interestingly, a polymorphism in macrophage migration-inhibitory factor (MIF) has been found to be associated with SJIA [15,16]. Indeed, the diverse presentation of juvenile arthritis suggests that there is still much more to learn about the aetiology of arthritis in children.…”

Section: Inflammatory Cytokines In the Pathology Of Arthritides: Rheumentioning

confidence: 99%

Therapeutic Antibody‐Based Drugs in the Treatment of Human Inflammatory Disorders

Sedger¹,

Ranasinghe²,

McDermott³

et al. 2017

Immunotherapy - Myths, Reality, Ideas, Future

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Inflammation causes debilitating human conditions and older treatments rely on global immunosuppression that non-specifically alleviates symptoms. Currently, several monoclonal antibodies (mAbs) are available that specifically block pro-inflammatory cytokines. These include mAbs specific to tumour necrosis factor (TNF), interleukin (IL)-1β,I L -6 , IL-17 and IL-12/IL-23. The chapter summarises the key elements in human inflammatory disease conditions, including various forms of arthritis, psoriasis, Crohn's disease and ulcerative colitis, plus pyrin-associated inflammatory syndromes and periodic fevers, to explain the benefit of cytokine neutralisation through mAb-type reagents. The chapter reviews the efficacy and safety of the current repertoire of anti-cytokine/cytokine receptor mAbs. It also discusses the known side effects and adverse events that are sometimes associated with systemic blockade of cytokines in vivo, and concludes that the accumulating knowledge of treatment failures can reveal unappreciated aspects of cytokine biology and even new treatment opportunities. The chapter includes mention of the rapidly expanding cohort of biosimilar mAbs and the mAbs to IL-4, IL-5 and IL-13 that are now emerging, in addition to the need for treatments for disorders that remain refractory to the current repertoire of anti-cytokine mAbs and conventional treatments. Thus, here we summarise the current status of anti-cytokine mAbs for human inflammatory diseases.

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Immunogenetics of juvenile idiopathic arthritis: A comprehensive review

Cited by 110 publications

References 99 publications

The epigenetics of PBC: The link between genetic susceptibility and environment

The epigenetics of PBC: The link between genetic susceptibility and environment

An immunome perturbation is present in juvenile idiopathic arthritis patients who are in remission and will relapse upon anti-TNFα withdrawal

Therapeutic Antibody‐Based Drugs in the Treatment of Human Inflammatory Disorders

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