[哥伦比亚银屑病关节炎患者样本中的 HLA 等位基因异质性]。

María Alejandra Meneses-Toro, Ómar Javier Calixto, Paula Andrea Chacón-Jaramillo, Mónica Acevedo-Godoy, Luisa Constanza Robayo-Beltrán, Camilo Vera-Parra, Juan Manuel Bello-Gualtero, Wilson Bautista-Molano, Verónica Noguera-Castro, Consuelo Romero-Sánchez
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引用次数: 0

摘要

目的目的:描述 PsA 中的 HLA 等位基因频率,并将其与人口统计学和临床变量相关联:方法:对确诊为PsA的成年患者(23人)和健康对照组(46人)进行回顾性研究,所有患者均要求检测HLA-A、B、C和DR。使用 HLA-PCR/SSO LifeCodes 进行分型,并在 LUMINEX IS100/200 xMAP® 系统上进行分析。(伦理/代码 HMC2022-014):结果:共纳入了 69 名 PsA 患者的 138 个等位基因,其中女性占 43.5%,年龄为(44.5±16.5)岁,平均发病年龄为(33.4±14)岁。只有9.5%的患者体重指数较高,血脂异常是最常见的合并症(34.8%),其次是高血压(26.1%)。82%的患者有皮肤表现,一旦确定为关节病,则主要是外周性疾病(74%),其中关节炎/关节痛占74%,趾关节炎占30%,趾间关节炎占13%。等位基因频率为 HLA*A 2402(13%)、3201(13%)和 2427(8.7%),HLA*B 1402(17.4%)、4002(17.4%)和 3801(13%),HLA*DR 0404(17.4%)和 0407(13%)。没有发现 HLA*B27,HLA*C0602 仅占 2.2%。HLA A*0201 和 DR*1301 在对照组和 PsA 中的出现频率较低(分别为 0.024 和 0.029),而 HLA*B1302 在 PsA 中的出现频率较高(P=0.035):结论:奇怪的是,HLAB*27没有阳性结果,这可能与人群组合有关。HLA Cw6 传统上与银屑病有关。然而,HLA Cw6 的缺失也与指甲疾病和 PsA 有关;因此,在我们的研究中,HLA Cw6 的频率较低(2.2%)。另一方面,HLA*B1302 与银屑病及其早期发病有关;在哥伦比亚的健康人群中,有 0.92% 的人患有此病;在我们的研究小组中,发现该基因在未建立临床关联的患者中具有重要意义。此前很少有研究报告哥伦比亚 PsA 患者的 HLA 结果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
[HLA alleles heterogeneity in a sample of colombian patients with a diagnosis of psoriatic arthritis].

Objective: The objective is to describe the HLA allelic frequency in PsA and correlate it with demographic and clinical variables.

Methods: Retrospective study of adult patients with a diagnosis of PsA (n=23) and healthy controls (n=46), all with a request for HLA-A, B, C, DR. Typing was performed using HLA-PCR/SSO LifeCodes and analyzed on the LUMINEX IS100/200 xMAP® system. (Ethics/Code HMC2022-014).

Results: One hundred thirty-eight alleles were included from 69 individuals, 43,5% women, aged 44,5±16,5 years in patients with PsA, with a mean age of disease onset of 33.4±14 years. Only 9.5% had a high Body Mass Index and dyslipidemia was the most frequent comorbidity (34.8%), followed by high blood pressure (26,1%). 82% debuted with skin manifestation and once the joint disease was established, the predominance was peripheral (74%) due to arthritis/arthralgia in 74%, enthesitis in 30% and dactylitis in 13%. The allele frequencies were for HLA*A 2402 (13%), 3201 (13%) and 2427 (8,7%), for HLA*B 1402 (17,4%), 4002 (17,4%), 3801 (13%) and HLA*DR 0404 (17,4%), 0407 (13%). No HLA*B27 was identified and HLA*C0602 was only 2,2%. HLA A*0201 and DR*1301 were less frequent in controls versus PsA (p=0.024 and 0,029, respectively), while HLA*B1302 was frequent in PsA (p=0,035).

Conclusions: Curiously, there were no positive results for HLAB*27, which may be related to the population mix. HLA Cw6 is traditionally associated with psoriasis. However, its absence has been linked to nail disorders and PsA; consequently, in our study, it had a low frequency (2,2%). On the other hand, HLA*B1302 has been related to the disease and its early onset; in the healthy Colombian population, it has been described in 0,92%; in our group, it is found to be significant in patients without establishing a clinical association. Few previous studies report HLA results in PsA in Colombia.

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