白细胞介素33与银屑病的相关性:系统回顾和荟萃分析

Keshav Kc, Hua Hu, Tilak Mahatara, S. Koirala, S. Shrestha, Shiv K. Sharma, Xiangfeng Song, Zhongwei Tian
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摘要

牛皮癣是一种常见的遗传性自身免疫性疾病,全球患病率为2-3%。银屑病的发病机制尚不完全清楚,但在银屑病中,表皮增生和炎症与免疫细胞的明显浸润有关,这些细胞产生不同类型的细胞因子-白细胞介素。IL-33作为IL-1细胞因子家族的新成员,在一些研究中,IL-33与银屑病有关,与正常健康皮肤相比,银屑病斑块中IL-33的血清浓度较高。尽管如此,IL-33与牛皮癣之间的关系尚不清楚。本文旨在探讨血清IL-33水平与银屑病的相关性。我们使用固定或随机效应模型进行了meta分析,以计算合并标准均值差异。我们发现,银屑病组的平均血清IL-33水平在0.35 pg/mL至586 pg/mL之间,健康对照组的平均血清IL-33水平在0 pg/mL至87.7 pg/mL之间。在五项研究中,有四项研究报告了IL-33水平的统计学差异,但合并估计(SMD = 0.340 95% CI: - 0.308至0.988)并未表明IL-33与牛皮癣之间存在显着关系。该分析显示银屑病人群与健康对照组相比血清IL-33水平无显著差异。这可能是因为我们没有包括任何动物研究、实验室研究、任何其他混合标记物或任何其他混合疾病病例。然而,由于纳入研究的低质量和观察性,本分析受到限制,需要进一步的研究来证实报告的相关性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
The Correlation between Interleukin 33 and Psoriasis: A Systematic Review and Meta-Analysis
Psoriasis is a common genetic autoimmune disorder with a global prevalence of 2–3%. The clear pathogenesis of psoriasis is not fully understood, but hyperproliferation and inflammation of the epidermis with marked infiltration of immune cells have been indicated in psoriasis with such cells producing different types of cytokines- interleukin. As such a new member of the IL-1 cytokine family, in some research, IL-33 has been linked with psoriasis showing high serum concentration of IL-33 in human psoriatic plaques compared to normal healthy skin. Despite this, the association between IL-33 and psoriasis is not clear. Herein, in this review, we aim to investigate the correlation between serum IL-33 levels and psoriasis. We conducted meta-analysis using fixed or random-effects models to calculate pooled standard mean differences. We found that the mean IL-33 serum levels were reported between 0.35 pg/mL to 586 pg/mL in the psoriatic group and 0 pg/mL to 87.7 pg/mL in the healthy control group. Out of five, four individual studies included in the analysis reported statistically significant differences in IL-33 levels, the pooled estimate (SMD = 0.340 95% CI: −0.308 to 0.988), however, did not indicate a significant relation between IL-33 and psoriasis. This analysis revealed no significant difference between serum IL-33 levels in the psoriatic population in comparison to healthy controls. This may be because we did not include any animal studies, lab-based studies, any other markers mixed together, or any other cases of diseases mixed together. However, further research is warranted to confirm the reported association as this analysis is limited by the low-quality and observational nature of the included studies.
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