Wang Wei, Liu Cong, Firestein Gary, Skene Peter, Deane Kevin, Holers Michael, Buckner Jane
Res Sq. 2025 Mar 31:rs.3.rs-6165802. doi: 10.21203/rs.3.rs-6165802/v1.
Elevated anti-citrullinated protein antibodies (ACPA) levels in the peripheral blood are associated with an increased risk for developing rheumatoid arthritis (RA). Currently, no treatments are available that prevent progression to RA in these at-risk individuals. In addition, diverse pathogenic mechanisms underlying a common clinical phenotype in RA complicate therapy as no single agent is universally effective. We propose that a unifying set of transcription factor and their downstream pathways regulate a pro-inflammatory cell communication network, and that this network allows multiple cell types to serve as pathogenic drivers in at-risk individuals and in early RA. To test this hypothesis, we identified ACPA-positive at-risk individuals, patients with early ACPA-positive RA and matched controls. We measured single cell chromatin accessibility and transcriptomic profiles from their peripheral blood mononuclear cells. The datasets were then integrated to define key TF, as well as TF-regulated targets and pathways. A distinctive TF signature was enriched in early RA and at-risk individuals that involved key pathogenic mechanisms in RA, including SUMOylation, RUNX2, YAP1, NOTCH3, and β-Catenin Pathways. Interestingly, this signature was identified in multiple cell types, including T cells, B cells, and monocytes, and the pattern of cell type involvement varied among the at-risk and early RA participants, supporting our hypothesis. Similar patterns of individualized gene expression patterns and cell types were confirmed in single cell studies of RA synovium. Cell communication analysis provided biological validation that diverse lineages can deliver the same core set of pro-inflammatory mediators to receiver cells that subsequently orchestrate rheumatoid inflammation. These cell-type-specific signature pathways could explain the personalized pathogenesis of RA and contribute to the diversity of clinical responses to targeted therapies. Furthermore, these data could provide opportunities for stratifying individuals at-risk for RA, and selecting therapies tailored for prevention or treatment of RA. Overall, this study supports a new paradigm to understand how a common clinical phenotype could arise from diverse pathogenic mechanisms and demonstrates the relevance of peripheral blood cells to synovial disease.
外周血中抗瓜氨酸化蛋白抗体(ACPA)水平升高与类风湿关节炎(RA)发病风险增加相关。目前,尚无治疗方法可预防这些高危个体发展为RA。此外,RA常见临床表型背后的多种致病机制使治疗变得复杂,因为没有单一药物能普遍有效。我们提出,一组统一的转录因子及其下游通路调节促炎细胞通讯网络,并且该网络使多种细胞类型在高危个体和早期RA中充当致病驱动因素。为了验证这一假设,我们确定了ACPA阳性的高危个体、早期ACPA阳性RA患者及匹配的对照。我们测量了他们外周血单个核细胞的单细胞染色质可及性和转录组谱。然后整合数据集以确定关键转录因子以及转录因子调控的靶点和通路。一种独特的转录因子特征在早期RA和高危个体中富集,涉及RA的关键致病机制,包括SUMO化、RUNX2、YAP1、NOTCH3和β-连环蛋白通路。有趣的是,这种特征在多种细胞类型中被发现,包括T细胞、B细胞和单核细胞,并且细胞类型参与模式在高危和早期RA参与者中有所不同,支持了我们的假设。在RA滑膜的单细胞研究中证实了个性化基因表达模式和细胞类型的类似模式。细胞通讯分析提供了生物学验证,即不同谱系可将相同核心组的促炎介质传递给受体细胞,随后这些受体细胞协调类风湿炎症。这些细胞类型特异性特征通路可以解释RA的个性化发病机制,并有助于对靶向治疗的临床反应多样性。此外,这些数据可为对RA高危个体进行分层以及选择针对RA预防或治疗的定制疗法提供机会。总体而言,本研究支持一种新范式,以理解常见临床表型如何由多种致病机制产生,并证明外周血细胞与滑膜疾病的相关性。
