Your search keyword '"Munro, Jane E"' showing total 4 results

1. Genomic risk scores for juvenile idiopathic arthritis and its subtypes.

Author

Cánovas, Rodrigo, Cobb, Joanna, Brozynska, Marta, Bowes, John, Li, Yun R., Smith, Samantha Louise, Hakonarson, Hakon, Thomson, Wendy, Ellis, Justine A., Abraham, Gad, Munro, Jane E., and Inouye, Michael

Subjects

RESEARCH, RESEARCH methodology, ARTHRITIS Impact Measurement Scales, JUVENILE idiopathic arthritis, GENETIC polymorphisms, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, DISEASE susceptibility, RESEARCH funding, LONGITUDINAL method

Abstract

Objectives: Juvenile idiopathic arthritis (JIA) is an autoimmune disease and a common cause of chronic disability in children. Diagnosis of JIA is based purely on clinical symptoms, which can be variable, leading to diagnosis and treatment delays. Despite JIA having substantial heritability, the construction of genomic risk scores (GRSs) to aid or expedite diagnosis has not been assessed. Here, we generate GRSs for JIA and its subtypes and evaluate their performance.Methods: We examined three case/control cohorts (UK, US-based and Australia) with genome-wide single nucleotide polymorphism (SNP) genotypes. We trained GRSs for JIA and its subtypes using lasso-penalised linear models in cross-validation on the UK cohort, and externally tested it in the other cohorts.Results: The JIA GRS alone achieved cross-validated area under the receiver operating characteristic curve (AUC)=0.670 in the UK cohort and externally-validated AUCs of 0.657 and 0.671 in the US-based and Australian cohorts, respectively. In logistic regression of case/control status, the corresponding odds ratios (ORs) per standard deviation (SD) of GRS were 1.831 (1.685 to 1.991) and 2.008 (1.731 to 2.345), and were unattenuated by adjustment for sex or the top 10 genetic principal components. Extending our analysis to JIA subtypes revealed that the enthesitis-related JIA had both the longest time-to-referral and the subtype GRS with the strongest predictive capacity overall across data sets: AUCs 0.82 in UK; 0.84 in Australian; and 0.70 in US-based. The particularly common oligoarthritis JIA also had a GRS that outperformed those for JIA overall, with AUCs of 0.72, 0.74 and 0.77, respectively.Conclusions: A GRS for JIA has potential to augment clinical JIA diagnosis protocols, prioritising higher-risk individuals for follow-up and treatment. Consistent with JIA heterogeneity, subtype-specific GRSs showed particularly high performance for enthesitis-related and oligoarthritis JIA. [ABSTRACT FROM AUTHOR]

Published

2020

2. Variants in CXCR4 associate with juvenile idiopathic arthritis susceptibility.

Author

Finkel, Terri H., Jin Li, Zhi Wei, Wei Wang, Haitao Zhang, Behrens, Edward M., Reuschel, Emma L., Limou, Sophie, Wise, Carol, Punaro, Marilynn, Becker, Mara L., Munro, Jane E., Flatø, Berit, Førre, Øystein, Thompson, Susan D., Langefeld, Carl D., Glass, David N., Glessner, Joseph T., Kim, Cecilia E., and Frackelton, Edward

Subjects

JUVENILE idiopathic arthritis, CXCR4 receptors, DISEASE susceptibility, GENOTYPES, AUTOIMMUNITY, GENETICS

Abstract

Background: Juvenile idiopathic arthritis (JIA) is the most common chronic rheumatic disease among children, the etiology of which involves a strong genetic component, but much of the underlying genetic determinants still remain unknown. Our aim was to identify novel genetic variants that predispose to JIA. Methods: We performed a genome-wide association study (GWAS) and replication in a total of 1166 JIA cases and 9500 unrelated controls of European ancestry. Correlation of SNP genotype and gene expression was investigated. Then we conducted targeted resequencing of a candidate locus, among a subset of 480 cases and 480 controls. SUM test was performed to evaluate the association of the identified rare functional variants. Results: The CXCR4 locus on 2q22.1 was found to be significantly associated with JIA, peaking at SNP rs953387. However, this result is subjected to subpopulation stratification within the subjects of European ancestry. After adjusting for principal components, nominal significant association remained (p < 10-4). Because of its interesting known function in immune regulation, we carried out further analyses to assess its relationship with JIA. Expression of CXCR4 was correlated with CXCR4 rs953387 genotypes in lymphoblastoid cell lines (p = 0.014) and T-cells (p = 0.0054). In addition, rare non-synonymous and stop-gain sequence variants in CXCR4, putatively damaging for CXCR4 function, were significantly enriched in JIA cases (p = 0.015). Conclusion: Our results suggest the association of CXCR4 variants with JIA, implicating that this gene may be involved in the pathogenesis of autoimmune disease. However, because this locus is subjected to population stratification within the subjects of European ancestry, additional replication is still necessary for this locus to be considered a true risk locus for JIA. This cell-surface chemokine receptor has already been targeted in other diseases and may serve as a tractable therapeutic target for a specific subset of pediatric arthritis patients with additional replication and functional validation of the locus. [ABSTRACT FROM AUTHOR]

Published

2016

3. Independent confirmation of juvenile idiopathic arthritis genetic risk loci previously identified by immunochip array analysis.

Author

Chiaroni-Clarke, Rachel C., Munro, Jane E., Chavez, Raul A., Pezic, Angela, Allen, Roger C., Akikusa, Jonathan D., Piper, Susan E., Saffery, Richard, Ponsonby, Anne-Louise, and Ellis, Justine A.

Subjects

*IMMUNOASSAY, *JUVENILE idiopathic arthritis, *DISEASE susceptibility, *PEDIATRIC rheumatology, *GENETICS, *THERAPEUTICS

Abstract

Background Our understanding of the genetic factors underlying juvenile idiopathic arthritis (JIA) is growing, but remains incomplete. Recently, a number of novel genetic loci were reported to be associated with JIA at (or near) genome-wide significance in a large case-control discovery sample using the Immunochip genotyping array. However, independent replication of findings has yet to be performed. We therefore attempted to replicate these newly identified loci in the Australian CLARITY JIA case-control sample. Findings Genotyping was successfully performed on a total of 404 JIA cases (mean age 6.4 years, 68% female) and 676 healthy child controls (mean age 7.1 years, 42% female) across 19 SNPs previously associated with JIA. We replicated a significant association (p < 0.05, odds ratio (OR) in a direction consistent with the previous report) for seven loci, six replicated for the first time - C5orf56-IRF1 (rs4705862), ERAP2-LNPEP (rs27290), PRR5L (rs4755450), RUNX1 (rs9979383), RUNX3 (rs4648881), and UBE2L3 (rs2266959). Conclusions We have carried out the first independent replication of association for six genes implicated in JIA susceptibility. Our data significantly strengthens the evidence that these loci harbor true disease associated variants. Thus, this study makes an important contribution to the growing body of international data that is revealing the genetic risk landscape of JIA. [ABSTRACT FROM AUTHOR]

Published

2014

4. Epistasis amongst PTPN2 and genes of the vitamin D pathway contributes to risk of juvenile idiopathic arthritis.

Author

Ellis, Justine A., Scurrah, Katrina J., Li, Yun R., Ponsonby, Anne-Louise, Chavez, Raul A., Pezic, Angela, Dwyer, Terence, Akikusa, Jonathan D., Allen, Roger C., Becker, Mara L., Thompson, Susan D., Lie, Benedicte A., Flatø, Berit, Førre, Øystein, Punaro, Marilynn, Wise, Carol, Finkel, Terri H., Hakonarson, Hakon, and Munro, Jane E.

Subjects

*EPISTASIS (Genetics), *JUVENILE idiopathic arthritis, *PHYSIOLOGICAL effects of vitamin D, *DISEASE susceptibility, *HERITABILITY, *TYPE 1 diabetes, *DISEASE risk factors

Abstract

Juvenile idiopathic arthritis (JIA) is a leading cause of childhood-onset disability. Although epistasis (gene–gene interaction) is frequently cited as an important component of heritability in complex diseases such as JIA, there is little compelling evidence that demonstrates such interaction. PTPN2, a vitamin D responsive gene, is a confirmed susceptibility gene in JIA, and PTPN2 has been suggested to interact with vitamin D pathway genes in type 1 diabetes. We therefore, tested for evidence of epistasis amongst PTPN2 and the vitamin D pathway genes GC , VDR , CYP24A1 , CYP2R1 , and DHCR7 in two independent JIA case-control samples (discovery and replication). In the discovery sample (318 cases, 556 controls), we identified evidence in support of epistasis across six gene–gene combinations ( e.g. , GC rs1155563 and PTPN2 rs2542151, OR int = 0.45, p = 0.00085). Replication was obtained for three of these combinations. That is, for GC and PTPN2 , CYP2R1 and VDR , and VDR and PTPN2 , similar epistasis was observed using the same SNPs or correlated proxies in an independent JIA case-control sample (1008 cases, 9287 controls). Using SNP data imputed across a 4 MB region spanning each gene, we obtained highly significant evidence for epistasis amongst all 6 gene–gene combinations identified in the discovery sample ( p -values ranging from 5.6 × 10 −9 to 7.5 × 10 −7 ). This is the first report of epistasis in JIA risk. Epistasis amongst PTPN2 and vitamin D pathway genes was both demonstrated and replicated. [ABSTRACT FROM AUTHOR]

Published

2015