Plasma levels of miR-21b and miR-146a can discriminate rheumatoid arthritis diagnosis and severity.

IF 2.1 Q2 MEDICINE, GENERAL & INTERNAL
BioMedicine-Taiwan Pub Date : 2025-03-01 eCollection Date: 2025-01-01 DOI:10.37796/2211-8039.1637
Rizk S Sarhan, Amr M El-Hammady, Yasmin M Marei, Sania K Elwia, Doaa M Ismail, Emtethal A S Ahmed
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引用次数: 0

Abstract

Objectives: This study tried to examine the ability of the estimated plasma gene-expression levels (PGEL) of microRNA (miR)-146a and miR-21b to distinguish patients with early rheumatoid arthritis (RA) out of arthritis patients who did not fulfill the diagnostic spectrum of either RA or osteoarthritis (OA); the diagnostic Gray-Zone (GZ).

Patients & methods: Enrolled patients underwent full diagnostic workup and were categorized as highseropositive and fulfilled the diagnostic spectrum for RA (RA-group), seronegative and fulfilling the diagnostic spectrum of OA (OA-group) and low-seropositive or seronegative patients who did not fulfill diagnostic criteria of RA or OA (GZ-group). Blood samples were obtained for quantification of PGEL of miR-146a and miR-21-b using the quantitative Reverse-transcriptase polymerase chain reaction and results were related to patients' seropositivity and clinical data.

Results: The mean fold change of PGEL of miR-146a and miR-21b was significantly higher in patients than in control samples, in samples of high-seropositive patients than in other samples, and in samples of low-seropositive than in seronegative patients. Both markers showed a positive significant correlation with Disease Activity Score-28 for RA-activity and seropositivity. Using the ROC curve analysis, the PGEL of both microRNAs could identify high-seropositive among the studied arthritis patients, but Regression Analysis defined high PGEL of miR-146a as the most significant predictor to identify RA patients and predict their disease activity. Statistical analyses defined miR-146a as the significant parameter that could differentiate between early RA and OA patients among GZ patients.

Conclusion: Early arthritis that does not fulfill the diagnostic spectrum of a certain type of arthritis is not uncommon and challenges therapeutic decision-making. The estimated PGEL of MicroRNA-146a might enlighten this gray diagnostic zone and allow differentiation between patients with early RA and early OA, and help to stratify RA patients according to disease activity and severity.

血浆miR-21b和miR-146a水平可以区分类风湿关节炎的诊断和严重程度。
目的:本研究试图检验microRNA (miR)-146a和miR-21b的估计血浆基因表达水平(PGEL)区分早期类风湿关节炎(RA)患者和不符合RA或骨关节炎(OA)诊断谱的关节炎患者的能力;诊断灰色地带(GZ)。患者和方法:纳入的患者进行全面的诊断检查,分为高血清阳性且符合RA诊断谱的患者(RA-组)、血清阴性且符合OA诊断谱的患者(OA组)和低血清阳性或血清阴性但不符合RA或OA诊断谱的患者(gz组)。采集血样,采用定量逆转录酶聚合酶链反应定量检测miR-146a和miR-21-b的PGEL,结果与患者血清阳性及临床资料相关。结果:miR-146a和miR-21b PGEL的平均折叠变化在患者中显著高于对照样本,在高血清阳性患者样本中显著高于其他样本,在低血清阳性样本中显著高于血清阴性样本。两种标志物均与疾病活动评分-28的ra活性和血清阳性呈正相关。通过ROC曲线分析,两种microrna的PGEL均可识别所研究的关节炎患者的高血清阳性,但回归分析认为miR-146a的高PGEL是识别RA患者并预测其疾病活动性的最显著预测因子。统计学分析认为miR-146a是区分GZ患者早期RA和OA患者的重要参数。结论:早期关节炎不符合某种类型关节炎的诊断谱并不罕见,这对治疗决策提出了挑战。估计的MicroRNA-146a PGEL可能会照亮这一灰色诊断区,使早期RA和早期OA患者能够区分,并有助于根据疾病活动性和严重程度对RA患者进行分层。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
BioMedicine-Taiwan
BioMedicine-Taiwan MEDICINE, GENERAL & INTERNAL-
CiteScore
2.80
自引率
5.90%
发文量
21
审稿时长
24 weeks
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