医学
队列
肿瘤科
内科学
疾病
队列研究
前瞻性队列研究
人口统计学的
生物信息学
生物标志物
体内
回顾性队列研究
曲线下面积
计算生物学
危险分层
基因沉默
实时聚合酶链反应
试验预测值
全基因组关联研究
基因表达谱
免疫学
作者
Tianxing Wu,Jialiang Luo,Haoyuan Qiu,Weijie Shao,Yueyang Lu,Meixuan Luo,Zhaofeng Lin,Yan Zhang,Libo Zhang,Hong Wang,Jia Zhou,Guangfeng Ruan,Peihua Cao,Daming Zuo
标识
DOI:10.1002/advs.202514130
摘要
Psoriatic disease (PsD) is a chronic inflammatory disease, with significant challenges in early risk stratification and drug development. Integration of proteomic and genomic data provides an unprecedented opportunity to identify predictive biomarkers and therapeutic targets for PsD. Here, through systemic genetic analyses, expression validation, and prospective cohort study, CDSN and PRSS8 were identified as candidate biomarkers and potential therapeutic targets for PsD. Individuals with higher levels of CDSN and PRSS8 were nearly three times more likely to develop PsD compared to the general population. It develops prediction models in adults without PsD at baseline from the UK Biobank. Combining CDSN and PRSS8 with demographics produced desirable predictions for PsD (area under the curve (AUC) = 0.80) and exhibited high specificity. Moreover, PRSS8 and CDSN were both predominantly localized in keratinocytes, and in vivo gene silencing of these proteins significantly reduced PsD-like skin lesions and systemic inflammatory markers. The findings strongly suggested that CDSN and PRSS8 are promising biomarkers for PsD onset and progression, providing a 12-year risk assessment window and potential as novel therapeutic targets. These results had important implications for screening high-risk populations and facilitating early intervention for PsD.
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