The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2015 |
| Outros Autores: | , , , , , , , , |
| Tipo de documento: | Artigo |
| Idioma: | eng |
| Título da fonte: | Repositório Institucional da UFRGS |
| Texto Completo: | http://hdl.handle.net/10183/175047 |
Resumo: | HLA-G is a regulatory molecule involved in immunologic tolerance. Growing evidence indicates that HLA-G plays a role in the regulation of inflammatory processes and autoimmune diseases. This study aimed at a systematic evaluation of soluble HLA-G (sHLA-G) in plasma of rheumatoid arthritis (RA) patients with long-lasting chronic inflammation. RA patients (n=68) and healthy controls (n=26) had their plasmatic sHLA-G measured by ELISA whereas the binding capability of sHLA-G to its cognate LILRB1 receptor was measured by a Luminex-based assay. All subjects were PCR-genotyped for HLA-G 14bp polymorphism (rs66554220). Significantly higher sHLA-G levels were observed in patients (p<0.001), however no significant differences were observed in LILRB1 binding capacity between RA patients and controls. Remarkably, the proportion of patients presenting specific binding of sHLA-G to LILRB1 was significantly decreased as compared to controls (56% vs. 81%, p=0.027). Patients without rheumatoid factor (RF-) were significantly overrepresented in the group of patients positive for LILRB1 binding as compared to patients without LILRB1 binding (31% vs 10%, p=0.033). Furthermore, methotrexate treated patients (n=58) revealed significantly lower LILRB1 binding to sHLA-G molecules than non-treated patients (medians: 12.2 vs. 67.7 units/ml, p=0.031). Unlike in controls, no significant differences in sHLAG levels were observed among patients grouped by 14pb genotype. Thus, in a substantial number of late RA patients, the circulating sHLA-G molecules are impaired regarding LILRB1 recognition, meaning that although increased levels are observed; these molecules are not qualified to exert their protective functions against inflammation. Our findings offer new insights into the immunopathology of RA patients with long-lasting anti-RA-treatment and highlight the importance to also measure the binding capability of sHLA-G to LILRB1. |
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Veit, Tiago DeganiChies, Jose Artur BogoSwitala, MagdalenaWagner, BettinaHorn, Peter A.Busatto, MauricioBrenol, Claiton ViegasBrenol, João Carlos TavaresXavier, Ricardo MachadoRebmann, Vera2018-04-26T02:33:07Z20151932-6203http://hdl.handle.net/10183/175047001066289HLA-G is a regulatory molecule involved in immunologic tolerance. Growing evidence indicates that HLA-G plays a role in the regulation of inflammatory processes and autoimmune diseases. This study aimed at a systematic evaluation of soluble HLA-G (sHLA-G) in plasma of rheumatoid arthritis (RA) patients with long-lasting chronic inflammation. RA patients (n=68) and healthy controls (n=26) had their plasmatic sHLA-G measured by ELISA whereas the binding capability of sHLA-G to its cognate LILRB1 receptor was measured by a Luminex-based assay. All subjects were PCR-genotyped for HLA-G 14bp polymorphism (rs66554220). Significantly higher sHLA-G levels were observed in patients (p<0.001), however no significant differences were observed in LILRB1 binding capacity between RA patients and controls. Remarkably, the proportion of patients presenting specific binding of sHLA-G to LILRB1 was significantly decreased as compared to controls (56% vs. 81%, p=0.027). Patients without rheumatoid factor (RF-) were significantly overrepresented in the group of patients positive for LILRB1 binding as compared to patients without LILRB1 binding (31% vs 10%, p=0.033). Furthermore, methotrexate treated patients (n=58) revealed significantly lower LILRB1 binding to sHLA-G molecules than non-treated patients (medians: 12.2 vs. 67.7 units/ml, p=0.031). Unlike in controls, no significant differences in sHLAG levels were observed among patients grouped by 14pb genotype. Thus, in a substantial number of late RA patients, the circulating sHLA-G molecules are impaired regarding LILRB1 recognition, meaning that although increased levels are observed; these molecules are not qualified to exert their protective functions against inflammation. Our findings offer new insights into the immunopathology of RA patients with long-lasting anti-RA-treatment and highlight the importance to also measure the binding capability of sHLA-G to LILRB1.application/pdfengPlos one. San Francisco. Vol. 10, no. 4 (Apr. 2015), e0123838, 14 p.Artrite reumatóidePolimorfismo genéticoAntígenos HLA-GReceptor B1 de leucócitos semelhante a imunoglobulinaThe paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patientsEstrangeiroinfo:eu-repo/semantics/articleinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFRGSinstname:Universidade Federal do Rio Grande do Sul (UFRGS)instacron:UFRGSORIGINAL001066289.pdf001066289.pdfTexto completo (inglês)application/pdf278544http://www.lume.ufrgs.br/bitstream/10183/175047/1/001066289.pdfcb864c05f9d42fc0da256ac2b1c99ff6MD51TEXT001066289.pdf.txt001066289.pdf.txtExtracted Texttext/plain43537http://www.lume.ufrgs.br/bitstream/10183/175047/2/001066289.pdf.txt158679e7faa92e49d59f43d42d6d0307MD52THUMBNAIL001066289.pdf.jpg001066289.pdf.jpgGenerated Thumbnailimage/jpeg1960http://www.lume.ufrgs.br/bitstream/10183/175047/3/001066289.pdf.jpg56ba02ba933c6487e477c8a9997fbc6dMD5310183/1750472023-09-23 03:35:33.75289oai:www.lume.ufrgs.br:10183/175047Repositório de PublicaçõesPUBhttps://lume.ufrgs.br/oai/requestopendoar:2023-09-23T06:35:33Repositório Institucional da UFRGS - Universidade Federal do Rio Grande do Sul (UFRGS)false |
| dc.title.pt_BR.fl_str_mv |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| title |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| spellingShingle |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients Veit, Tiago Degani Artrite reumatóide Polimorfismo genético Antígenos HLA-G Receptor B1 de leucócitos semelhante a imunoglobulina |
| title_short |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| title_full |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| title_fullStr |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| title_full_unstemmed |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| title_sort |
The paradox of high availability and low recognition of soluble HLA-G by LILRB1 receptor in rheumatoid arthritis patients |
| author |
Veit, Tiago Degani |
| author_facet |
Veit, Tiago Degani Chies, Jose Artur Bogo Switala, Magdalena Wagner, Bettina Horn, Peter A. Busatto, Mauricio Brenol, Claiton Viegas Brenol, João Carlos Tavares Xavier, Ricardo Machado Rebmann, Vera |
| author_role |
author |
| author2 |
Chies, Jose Artur Bogo Switala, Magdalena Wagner, Bettina Horn, Peter A. Busatto, Mauricio Brenol, Claiton Viegas Brenol, João Carlos Tavares Xavier, Ricardo Machado Rebmann, Vera |
| author2_role |
author author author author author author author author author |
| dc.contributor.author.fl_str_mv |
Veit, Tiago Degani Chies, Jose Artur Bogo Switala, Magdalena Wagner, Bettina Horn, Peter A. Busatto, Mauricio Brenol, Claiton Viegas Brenol, João Carlos Tavares Xavier, Ricardo Machado Rebmann, Vera |
| dc.subject.por.fl_str_mv |
Artrite reumatóide Polimorfismo genético Antígenos HLA-G Receptor B1 de leucócitos semelhante a imunoglobulina |
| topic |
Artrite reumatóide Polimorfismo genético Antígenos HLA-G Receptor B1 de leucócitos semelhante a imunoglobulina |
| description |
HLA-G is a regulatory molecule involved in immunologic tolerance. Growing evidence indicates that HLA-G plays a role in the regulation of inflammatory processes and autoimmune diseases. This study aimed at a systematic evaluation of soluble HLA-G (sHLA-G) in plasma of rheumatoid arthritis (RA) patients with long-lasting chronic inflammation. RA patients (n=68) and healthy controls (n=26) had their plasmatic sHLA-G measured by ELISA whereas the binding capability of sHLA-G to its cognate LILRB1 receptor was measured by a Luminex-based assay. All subjects were PCR-genotyped for HLA-G 14bp polymorphism (rs66554220). Significantly higher sHLA-G levels were observed in patients (p<0.001), however no significant differences were observed in LILRB1 binding capacity between RA patients and controls. Remarkably, the proportion of patients presenting specific binding of sHLA-G to LILRB1 was significantly decreased as compared to controls (56% vs. 81%, p=0.027). Patients without rheumatoid factor (RF-) were significantly overrepresented in the group of patients positive for LILRB1 binding as compared to patients without LILRB1 binding (31% vs 10%, p=0.033). Furthermore, methotrexate treated patients (n=58) revealed significantly lower LILRB1 binding to sHLA-G molecules than non-treated patients (medians: 12.2 vs. 67.7 units/ml, p=0.031). Unlike in controls, no significant differences in sHLAG levels were observed among patients grouped by 14pb genotype. Thus, in a substantial number of late RA patients, the circulating sHLA-G molecules are impaired regarding LILRB1 recognition, meaning that although increased levels are observed; these molecules are not qualified to exert their protective functions against inflammation. Our findings offer new insights into the immunopathology of RA patients with long-lasting anti-RA-treatment and highlight the importance to also measure the binding capability of sHLA-G to LILRB1. |
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2015 |
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2015 |
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2018-04-26T02:33:07Z |
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Plos one. San Francisco. Vol. 10, no. 4 (Apr. 2015), e0123838, 14 p. |
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