Genetically Distinct Subsets within ANCA-Associated Vasculitis

Lyons, Paul; Rayner, Tim; Trivedi, Sapna; Holle, Julia; Watts, Richard A.; Jayne, David; Baslund, Bo; Brenchley, Paul; Bruchfeld, Annette; Chaudhry, Afzal; Tervaert, Jan Willem Cohen; Deloukas, Panos; Feighery, Conleth; Gross, Wolfgang L.; Guillevin, Loı̈c; Gunnarsson, Iva; Harper, Lorraine; Hrušková, Zdenka; Little, Mark A.; Martorana, Davide; Neumann, Thomas; Ohlsson, Sophie; Padmanabhan, Sandosh; Pusey, Charles D.; Salama, Alan D.; Sanders, Jan-Stephan; Savage, Caroline O.S.; Segelmark, Mårten; Stegeman, Coen A.; Tesař, Vladimı́r; Vaglio, Augusto; Wieczorek, Stefan; Wilde, Benjamin; Zwerina, Jochen; Rees, Andrew J.; Clayton, David; Smith, Kenneth G. C.

doi:10.1056/nejmoa1108735

Cited by 856 publications

(662 citation statements)

References 41 publications

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“…This association was limited to the GPA and PR3‐ANCA subsets (Table 2) and is consistent with prior GWAS data showing that a significant association with another SERPINA1 SNP, rs7151526, depended entirely on the concomitant presence of the Z allele 2.…”

Section: Resultssupporting

confidence: 90%

“…A significant association of AAV with rs62132293, a SNP located 2.6 kb upstream of the PRTN3 transcription start site, was also observed ( P = 8.60 × 10 −11 ); this finding is in keeping with previously observed associations at this locus (albeit with different SNPs) in AAV candidate gene and GWAS analyses (Table 1 and Supplementary Figures 3 and 4 [http://onlinelibrary.wiley.com/doi/10.1002/art.40034/abstract]) 2, 16. This association was limited to the GPA and PR3‐ANCA subsets (Table 2), consistent with the pathophysiologic relevance of the PRTN3 ‐encoded PR3 serine protease to these phenotypes 17.…”

Section: Resultssupporting

confidence: 87%

“…Consistent with a prior study that demonstrated genetic distinctions between PR3‐ANCA–positive vasculitis and MPO‐ANCA–positive vasculitis 2, we detected peak associations of the HLA–DPB1 and HLA–DPA1 variants with positivity for PR3‐ANCAs, whereas in those with MPO‐ANCAs, the HLA–DQA2 and HLA–DQB1 variants showed the strongest associations. Differential effects of these variants also distinguished patients with GPA from those with MPA, suggesting that GPA and PR3‐ANCA–positive AAV share a composite set of MHC class II risk alleles that is largely distinct from those conferring risk of MPA and MPO‐ANCA–positive AAV.…”

Section: Discussionsupporting

confidence: 91%

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Identification of Functional and Expression Polymorphisms Associated With Risk for Antineutrophil Cytoplasmic Autoantibody–Associated Vasculitis

Merkel

Xie

Monach

et al. 2017

Arthritis & Rheumatology

139

154

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ObjectiveTo identify risk alleles relevant to the causal and biologic mechanisms of antineutrophil cytoplasmic antibody (ANCA)–associated vasculitis (AAV).MethodsA genome‐wide association study and subsequent replication study were conducted in a total cohort of 1,986 cases of AAV (patients with granulomatosis with polyangiitis [Wegener's] [GPA] or microscopic polyangiitis [MPA]) and 4,723 healthy controls. Meta‐analysis of these data sets and functional annotation of identified risk loci were performed, and candidate disease variants with unknown functional effects were investigated for their impact on gene expression and/or protein function.ResultsAmong the genome‐wide significant associations identified, the largest effect on risk of AAV came from the single‐nucleotide polymorphism variants rs141530233 and rs1042169 at the HLA–DPB1 locus (odds ratio [OR] 2.99 and OR 2.82, respectively) which, together with a third variant, rs386699872, constitute a triallelic risk haplotype associated with reduced expression of the HLA–DPB1 gene and HLA–DP protein in B cells and monocytes and with increased frequency of complementary proteinase 3 (PR3)–reactive T cells relative to that in carriers of the protective haplotype. Significant associations were also observed at the SERPINA1 and PTPN22 loci, the peak signals arising from functionally relevant missense variants, and at PRTN3, in which the top‐scoring variant correlated with increased PRTN3 expression in neutrophils. Effects of individual loci on AAV risk differed between patients with GPA and those with MPA or between patients with PR3‐ANCAs and those with myeloperoxidase‐ANCAs, but the collective population attributable fraction for these variants was substantive, at 77%.ConclusionThis study reveals the association of susceptibility to GPA and MPA with functional gene variants that explain much of the genetic etiology of AAV, could influence and possibly be predictors of the clinical presentation, and appear to alter immune cell proteins and responses likely to be key factors in the pathogenesis of AAV.

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Section: Resultssupporting

confidence: 90%

Section: Resultssupporting

confidence: 87%

Section: Discussionsupporting

confidence: 91%

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Identification of Functional and Expression Polymorphisms Associated With Risk for Antineutrophil Cytoplasmic Autoantibody–Associated Vasculitis

Merkel

Xie

Monach

et al. 2017

Arthritis & Rheumatology

139

154

View full text Add to dashboard Cite

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“…This difference probably reflects the strong link between genetic background, AAV subtype, and ANCA subtype (15). Furthermore, the prevalence of pulmonary involvement in patients with MPA is higher in Japan than in European countries (5).…”

mentioning

confidence: 98%

Prevalence and Responsiveness to Treatment of Lung Abnormalities on Chest Computed Tomography in Patients With Microscopic Polyangiitis: A Multicenter, Longitudinal, Retrospective Study of One Hundred Fifty Consecutive Hospital‐Based Japanese Patients

Yamagata

Ikeda

Tsushima

et al. 2016

Arthritis & Rheumatology

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Objective. To determine the prevalence of lung abnormalities on chest computed tomography (CT) in patients with microscopic polyangiitis (MPA), to assess the responsiveness of such abnormalities to initial treatment, and to assess associations between these abnormalities and patient and disease characteristics and mortality.Methods. We retrospectively identified 167 consecutive hospital-based patients with MPA in 3 hospitals in Japan. We longitudinally collected clinical information for 150 of these patients, for whom CT images obtained before treatment were available. We then determined the presence of 22 imaging components of lung abnormalities in these patients.Results. The vast majority of patients (97%) had at least 1 lung abnormality on chest CT images, including interstitial lung lesions (66%), airway lesions (66%), pleural lesions (53%), and emphysematous lesions (37%). In multivariate analyses, ground-glass opacity was associated with the Birmingham Vasculitis Activity Score, whereas 3 of 4 airway lesions were associated with myeloperoxidase-antineutrophil cytoplasmic antibodies. Latent class analysis identified a distinct group of patients with airwaypredominant lung lesions. Airway lesions such as bronchiolitis and bronchovascular bundle thickening were among the components that showed improvement within 3 months of the initial treatment. An idiopathic pulmonary fibrosis pattern was the only chest CT variable that was independently associated with shorter survival.Conclusion. Abnormalities in a wide range of anatomic areas, including the whole airway, can be identified in the lungs of patients with MPA before treatment. The prevalence, clustering patterns, and responsiveness to treatment of individual lung abnormalities provide groundwork for informing future studies to understand the pathophysiology of MPA.Microscopic polyangiitis (MPA) is a necrotizing systemic vasculitis that affects small to medium-sized vessels. In MPA, immune deposits on the vessel wall are usually absent, and serum antineutrophil cytoplasmic antibodies (ANCAs) are frequently present. MPA shares these

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“…These three AAV, especially GPA (WG) and MPA, are included in the same clinical studies. However, a recent genome-wide association study (GWAS) has provided evidence that GPA (WG) and MPA are indeed different diseases, while the strongest genetic associations were with the antigenic specificity of ANCA, not with the clinical syndrome [27]. GPA (WG) is associated with different HLA genes compared with MPA, and singlenucleotide polymorphisms associated with the genes encoding α1-antitrypsin and proteinase 3 [27].…”

Section: Small-vessel Vasculitismentioning

confidence: 99%

Vasculitis: do we know more to classify better?

Batu

Özen

2014

Pediatr Nephrol

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The systemic vasculitides are a heterogeneous group of disorders characterized by the inflammation of blood vessels. The development and implementation of advanced diagnostic tests and genetic studies have resulted in substantial improvement in our understanding of vasculitis pathogenesis, resulting in the revision of the nomenclature and classification for vasculitis. Multicenter, collaborative studies are currently underway to develop improved diagnostic criteria. In this review, the major nomenclature and classification systems for vasculitides are summarized, with special emphasis on those emerging from the recent 2012 Chapel Hill Consensus Conference (CHCC).

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Genetically Distinct Subsets within ANCA-Associated Vasculitis

Cited by 856 publications

References 41 publications

Identification of Functional and Expression Polymorphisms Associated With Risk for Antineutrophil Cytoplasmic Autoantibody–Associated Vasculitis

Identification of Functional and Expression Polymorphisms Associated With Risk for Antineutrophil Cytoplasmic Autoantibody–Associated Vasculitis

Prevalence and Responsiveness to Treatment of Lung Abnormalities on Chest Computed Tomography in Patients With Microscopic Polyangiitis: A Multicenter, Longitudinal, Retrospective Study of One Hundred Fifty Consecutive Hospital‐Based Japanese Patients

Vasculitis: do we know more to classify better?

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