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银屑病患者全身性治疗反应的生物标志物:范围综述。

Biomarkers of systemic treatment response in people with psoriasis: a scoping review.

机构信息

Centre for Reviews and Dissemination, University of York, York, UK.

St John's Institute of Dermatology, School of Basic & Medical Biosciences, Faculty of Life Sciences & Medicine, King's College London, London, UK.

出版信息

Br J Dermatol. 2022 Oct;187(4):494-506. doi: 10.1111/bjd.21677. Epub 2022 Jul 20.

DOI:10.1111/bjd.21677
PMID:35606928
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9796396/
Abstract

BACKGROUND

Responses to the systemic treatments commonly used to treat psoriasis vary. Biomarkers that accurately predict effectiveness and safety would enable targeted treatment selection, improved patient outcomes and more cost-effective healthcare.

OBJECTIVES

To perform a scoping review to identify and catalogue candidate biomarkers of systemic treatment response in psoriasis for the translational research community.

METHODS

A systematic search of CENTRAL, Embase, LILACS and MEDLINE was performed for relevant articles published between 1990 and December 2021. Eligibility criteria were studies involving patients with psoriasis (any age, n ≥ 50) reporting biomarkers associated with systemic treatment response. The main outcomes were any measure of systemic treatment efficacy or safety. Data were extracted by one reviewer and checked by a second; studies meeting minimal quality criteria (use of methods to control for confounding) were formally assessed for bias. Candidate biomarkers were identified by an expert multistakeholder group using a majority voting consensus exercise and mapped to relevant cellular and molecular pathways.

RESULTS

Of 71 included studies (67 studying effectiveness outcomes and eight safety outcomes; four studied both), most reported genomic or proteomic biomarkers associated with response to biologics (48 studies). Methodological or reporting limitations frequently compromised the interpretation of findings, including inadequate control for key covariates, lack of adjustment for multiple testing, and selective outcome reporting. We identified candidate biomarkers of efficacy to tumour necrosis factor inhibitors [variation in CARD14, CDKAL1, IL1B, IL12B and IL17RA loci, and lipopolysaccharide-induced phosphorylation of nuclear factor (NF)-κB in type 2 dendritic cells] and ustekinumab (HLA-C*06:02 and variation in an IL1B locus). None were supported by sufficient evidence for clinical use without further validation studies. Candidate biomarkers were found to be involved in the immune cellular crosstalk implicated in psoriasis pathogenesis, most notably antigen presentation, T helper (Th)17 cell differentiation, positive regulation of NF-κB, and Th17 cell activation.

CONCLUSIONS

This comprehensive catalogue provides a key resource for researchers and reveals a diverse range of biomarker types and outcomes in the included studies. The candidate biomarkers identified require further evaluation in methodologically robust studies to establish potential clinical utility. Future studies should aim to address the common methodological limitations highlighted in this review to expedite discovery and validation of biomarkers for clinical use. What is already known about this topic? Responses to the systemic treatments commonly used to treat psoriasis vary. Biomarkers that accurately predict effectiveness and safety would enable targeted treatment selection, improved patient outcomes and more cost-effective healthcare. What does this study add? This review provides a comprehensive catalogue of investigated biomarkers of systemic treatment response in psoriasis. A diverse range of biomarker types and outcomes was found in the included studies, serving as a key resource for the translational research community.

摘要

背景

用于治疗银屑病的系统治疗方法的反应各不相同。能够准确预测疗效和安全性的生物标志物将能够实现靶向治疗选择、改善患者结局和更具成本效益的医疗保健。

目的

进行范围综述,以确定和编目银屑病系统治疗反应的候选生物标志物,为转化研究界提供参考。

方法

对 CENTRAL、Embase、LILACS 和 MEDLINE 进行了系统检索,以查找 1990 年至 2021 年 12 月期间发表的相关文章。纳入标准为:涉及银屑病患者(任何年龄,n≥50)的研究报告与系统治疗反应相关的生物标志物。主要结局为任何衡量系统治疗有效性或安全性的指标。由一名评审员进行数据提取,另一名评审员进行核对;符合最低质量标准(使用控制混杂因素的方法)的研究被正式评估偏倚。候选生物标志物由一个多利益相关者专家组使用多数投票共识共识来确定,并映射到相关的细胞和分子途径。

结果

在 71 项纳入的研究中(67 项研究有效性结局,8 项研究安全性结局,4 项研究同时研究了两者),大多数研究报告了与生物制剂反应相关的基因组或蛋白质组生物标志物(48 项研究)。方法学或报告方面的局限性经常影响研究结果的解释,包括关键协变量的控制不足、未对多次检验进行调整以及选择性报告结局。我们确定了肿瘤坏死因子抑制剂疗效的候选生物标志物[CARD14、CDKAL1、IL1B、IL12B 和 IL17RA 基因座的变异,以及 2 型树突状细胞中 NF-κB 的脂多糖诱导磷酸化]和乌司奴单抗(HLA-C*06:02 和 IL1B 基因座的变异)。没有足够的证据支持这些候选生物标志物在没有进一步验证研究的情况下用于临床应用。候选生物标志物被发现与银屑病发病机制中的免疫细胞相互作用有关,尤其是抗原呈递、Th17 细胞分化、NF-κB 的正调控和 Th17 细胞激活。

结论

这份全面的目录为研究人员提供了一个关键资源,并揭示了纳入研究中广泛的生物标志物类型和结局。确定的候选生物标志物需要在方法学上稳健的研究中进一步评估,以确定其潜在的临床效用。未来的研究应旨在解决本综述中强调的常见方法学局限性,以加快生物标志物的发现和验证,从而实现临床应用。

关于这个主题,已知的信息有哪些? 用于治疗银屑病的系统治疗方法的反应各不相同。能够准确预测疗效和安全性的生物标志物将能够实现靶向治疗选择、改善患者结局和更具成本效益的医疗保健。

本研究增加了哪些新的信息? 本综述提供了银屑病系统治疗反应候选生物标志物的综合目录。纳入研究中的生物标志物类型和结局多种多样,为转化研究界提供了一个关键资源。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e107/9796396/c2085d8a3cdf/BJD-187-494-g003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e107/9796396/3a3cf63a523b/BJD-187-494-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e107/9796396/c2085d8a3cdf/BJD-187-494-g003.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e107/9796396/3a3cf63a523b/BJD-187-494-g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e107/9796396/c2085d8a3cdf/BJD-187-494-g003.jpg

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