Functional Status and Quality of Life in Adult Patients With Juvenile Arthritis During the Long-Termcourse of Disease

Салугина, С. О.

doi:10.14412/1996-7012-2011-649

Cited by 2 publications

(2 citation statements)

References 25 publications

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“…В настоящей работе при выборе подтипов ЮИА для молекулярно-генетического анализа исходили из того, что профиль генетической изменчивости при РФ-негативном полиартрите (A*02, DRBI*08, DQAI*04) достаточно сильно перекрывается с ее профилем при олигоартрите [8], а также учитывали особенности течения различных типов ЮИА -для системной формы характерен высокий риск инвалидизации и развития тяжелых состояний типа синдрома активации макрофагов, поражений легких и сердца, тогда как у больных с персистирующим олигоарт ритом функциональная способность сохраняется в большей степени [11].…”

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“…В исследуемой выборке аллели A*02:01:01 (OR 0,39 [0,15-0,96], p = 0,047), DQB1*04:02:01 (OR 0,25 [0,06-0,97], p = 0,068), DRB1*08:01:01 (OR 0,16 [0,03-0,82], p = 0,027) у детей с системным ЮИА встречались со значительно меньшей частотой, чем среди детей с олигоартритом. При сравнении групп пациентов с контролем обнаружены аллели, повышающие риск развития олигоартикулярного ЮИА (DQB1*04:02:01 (OR 5,88 [1,[20][21][22][23][24][25][26][27][28]72], p = 0,026), DRB1*08:01:01 (OR 3,94 [1,[1][2][3][4][5][6][7][8][9][10][11][12][13][14][15]39], p = 0,07)). Кроме того, выявлены аллели, показавшие протективный эффект либо только по отношению к системному подтипу ЮИА (DRB1*03:01 (OR 0,11 [0,01-0,88], p = 0,03)), либо к обеим рассматриваемым формам заболевания (DQA1*05:01:01 (OR 0,08 [0,009-0,65], p = 0,007 и OR 0,16 [0,03-0,79], p = 0,026) и DQB1*02:01:01 (OR 0,09 [0,01-0,83], p = 0,01 и OR 0,20 [0,04-1,00], p = 0,046) для системного и олигоартикулярного ЮИА соответственно).…”

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Characteristic spectra of class I and II HLA-alleles in patients with different clinical forms of juvenile idiopathic arthritis in the Republic of Belarus

et al. 2020

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The genes of the major histocompatibility complex (HLA) play a significant role in the genetic predisposition to juvenile idiopathic arthritis (JIA) and determine up to 18 % of disease risk. This work was aimed to reveal associations of the HLA characteristic pattern with two clinically different forms of JIA in the Belarusian population. 24 patients diagnosed with systemic JIA, 24 patients with oligoarticular JIA and 24 healthy controls were included into the study. High-throughput HLA typing for 11 loci was performed using TruSight HLA v2 Sequencing Panel (Illumina) on the MiSeq system. DQB1*04:02:01 (p = 0.026; OR 5.88 [1.20–28.72]), DRB1*08:01:01 (p = 0.07; OR 3.94 [1.01–15.39]) and DR8-haplotype (p = 0.006; OR 3.95 [1.34–11.63]) frequencies were significantly higher in patients with oligoarthritis but not systemic JIA when compared with controls. While DQA1*05:01:01 and DQB1*02:01:01 alleles showed a protective effect against both systemic (p = 0.007, OR 0.08 [0.009–0.65]; p = 0.01, OR 0.09 [0.01–0.83]) and oliarticular JIA (p = 0.026, OR 0.16 [0.03–0.79]; p = 0.046, OR 0.2 [0.04–1.00], the negative association of the DRB1*03:01 allele was revealed only for systemic JIA (p = 0.03, OR 0.11 [0.01–0.88]). Thus, the obtained results suggest that different HLA-patterns are involved into the formation of various JIA subtypes.

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Characteristic spectra of class I and II HLA-alleles in patients with different clinical forms of juvenile idiopathic arthritis in the Republic of Belarus

et al. 2020

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Genetic susceptibility to juvenile idiopathic arthritis in the Belarusian population: gene-gene interactions analysis

Yatskiu

Савина

Никитченко

et al. 2019

Ecological genetics

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Background. GWASs revealed a huge amount of candidate genes for juvenile idiopathic arthritis (JIA) susceptibility. Individual SNP analysis has restrictions as an effect of each substitution may be too subtle to be detected but their interactions may significantly contribute to disease susceptibility. Materials and methods. 118 patients diagnosed with JIA and 202 controls were included into the study. The study was aimed to estimate interactions between SNPs of the immune and inflammatory responses genes: RUNX3 (rs11249215), RUNX1 (rs9979383), STAT4 (rs7574865), TRAF1/C5 (rs3761847), MIF (rs755622), CTLA4 (rs5742909, rs231775), PTPN2 (rs2542151) and to reveal their effects on the JIA susceptibility. SNPs were genotyped using PCR-RFLP and Real-time PCR. Multifactor dimensionality reduction analysis was performed using MDR 3.0.2 software. Results. RUNX3, STAT4 and PTPN2 polymorphisms were associated with systemic arthritis, RF- polyarthritis and oligoarthritis respectively. Interaction of CTLA4 (rs5742909, rs231775), TRAF1/C5 (rs3761847), RUNX1 (rs9979383), PTPN2 (rs2542151) SNPs is shown to be a risk factor for JIA (p = 0.0099). Conclusion. Some of the SNPs studied are associated with distinct JIA subtypes. MDR analysis identified a statistically significant high-order interaction of five polymorphisms which collectively may contribute to JIA genetic susceptibility in the Belarusian population.

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Functional Status and Quality of Life in Adult Patients With Juvenile Arthritis During the Long-Termcourse of Disease

Cited by 2 publications

References 25 publications

Characteristic spectra of class I and II HLA-alleles in patients with different clinical forms of juvenile idiopathic arthritis in the Republic of Belarus

Characteristic spectra of class I and II HLA-alleles in patients with different clinical forms of juvenile idiopathic arthritis in the Republic of Belarus

Genetic susceptibility to juvenile idiopathic arthritis in the Belarusian population: gene-gene interactions analysis

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