Activation of a Latent Epitope Causing Differential Binding of Antineutrophil Cytoplasmic Antibodies to Proteinase 3

Moura, Marta Casal; Thompson, Gwen; Nelson, Darlene R.; Fussner, Lynn A.; Hummel, Amber M.; Jenne, Dieter E.; Emerling, Daniel; Fervenza, Fernando C.; Kallenberg, Cees G. M.; Langford, Carol A.; McCune, W. Joseph; Merkel, Peter A.; Monach, Paul A.; Seo, Philip; Spiera, Robert; Clair, E. William St.; Ytterberg, Steven R.; Stone, John H.; Robinson, William H.; Specks, Ulrich

doi:10.1002/art.42418

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“…We previously showed that remote mutations and engagement of distal epitopes by an anti-PR3 monoclonal antibody can increase the local mobility and expose latent PR3 epitopes, leading to conformational adaptation facilitating or necessary for antibody binding 16 17. This type of epitope activation—achieved in vitro by remote mutations, or in vivo either by polymorphisms or by binding of another autoantibody or protein ligand—may be an important contributor of PR3-AAV pathogenesis 16 17. Our observation that homozygosity for the PRTN3-Val 119 Ile polymorphism is associated with a different risk for severe relapses is consistent with the hypothesis that the two different PR3 antigen variants may interact differently with pathogenic PR3-ANCA.…”

Section: Discussionsupporting

confidence: 87%

“…Consequently, homozygosity for this polymorphism, which is the only one resulting in a change of the amino acid sequence of PR3, may represent an additional identifiable risk factor for severe relapse. Moreover, our data suggest that the quantity of PR3 expressed in patients with AAV compared with healthy controls and conformational changes of the autoantigen may modulate its interactions with pathogenic PR3-ANCA promoting disease activity 17 18. Further studies are necessary to validate and better understand the association of this observation with the risk of severe relapse and its possible molecular mechanisms.…”

Section: Discussionmentioning

confidence: 86%

“…Moreover, our data suggest that the quantity of PR3 expressed in patients with AAV compared with healthy controls and conformational changes of the autoantigen may modulate its interactions with pathogenic PR3-ANCA promoting disease activity. 17 18 Further studies are necessary to validate and better understand the association of this observation with the risk of severe relapse and its possible molecular mechanisms.…”

Section: Discussionmentioning

confidence: 99%

“…We hypothesise that, in vivo, the presence of polymorphisms in proteins might modulate their antigenicity particularly during states of severe inflammation, similarly to what was found in vitro. We previously showed that remote mutations and engagement of distal epitopes by an anti-PR3 monoclonal antibody can increase the local mobility and expose latent PR3 epitopes, leading to conformational adaptation facilitating or necessary for antibody binding 16 17. This type of epitope activation—achieved in vitro by remote mutations, or in vivo either by polymorphisms or by binding of another autoantibody or protein ligand—may be an important contributor of PR3-AAV pathogenesis 16 17.…”

Section: Discussionmentioning

confidence: 99%

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Risk of relapse of ANCA-associated vasculitis among patients homozygous for the proteinase 3 gene Val119Ile polymorphism

et al. 2023

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BackgroundThe frequency of proteinase 3 gene (PRTN3) polymorphisms in patients with antineutrophil cytoplasmic antibody (ANCA)-associated vasculitis (AAV) is not fully characterised. We hypothesise that the presence of a PRTN3 gene polymorphism (single nucleotide polymorphism (SNP) rs351111) is relevant for clinical outcomes.MethodsDNA variant calling for SNP rs351111 (chr.19:844020, c.355G>A) in PRTN3 gene assessed the allelic frequency in patients with PR3-AAV included in the Rituximab in ANCA-Associated Vasculitis trial. This was followed by RNA-seq variant calling to characterise the mRNA expression. We compared clinical outcomes between patients homozygous for PRTN3-Ile119or PRTN3-Val119.ResultsWhole blood samples for DNA calling were available in 188 patients. 75 patients with PR3-AAV had the allelic variant: 62 heterozygous PRTN3-Val119Ile and 13 homozygous for PRTN3-Ile119. RNA-seq was available for 89 patients and mRNA corresponding to the allelic variant was found in 32 patients with PR3-AAV: 25 heterozygous PRTN3-Val119Ile and 7 homozygous for PRTN3-Ile119. The agreement between the DNA calling results and mRNA expression of the 86 patients analysed by both methods was 100%. We compared the clinical outcomes of 64 patients with PR3-AAV: 51 homozygous for PRTN3-Val119and 13 homozygous for PRTN3-Ile119. The frequency of severe flares at 18 months in homozygous PRTN3-Ile119was significantly higher when compared with homozygous PRTN3-Val119(46.2% vs 19.6%, p=0.048). Multivariate analysis identified homozygous PR3-Ile119as main predictor of severe relapse (HR 4.67, 95% CI 1.16 to 18.86, p=0.030).ConclusionIn patients with PR3-AAV, homozygosity for PRTN3-Val119Ile polymorphism appears associated with higher frequency of severe relapse. Further studies are necessary to better understand the association of this observation with the risk of severe relapse.

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Section: Discussionsupporting

confidence: 87%

Section: Discussionmentioning

confidence: 86%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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