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外周血单细胞转录组图谱揭示B细胞驱动的急性胰腺炎严重程度预测特征。

Single-Cell Transcriptomic Atlas of Peripheral Blood Reveals B-Cell-Driven Signature Predictive of Acute Pancreatitis Severity.

作者信息

Xie Rongli, Xiao Guohui, Yang Kaige, Wang Xiaofeng, Chen Cong, Ding Min, Zhou Tong, Mukherjee Rajarshi, Sutton Robert, Chen Erzhen, Chen Ying, Huang Wei, Xu Dan, Fei Jian

机构信息

Department of General Surgery RuiJin Hospital Lu Wan Branch Shanghai Jiao Tong University School of Medicine Shanghai China.

Department of General Surgery Ruijin Hospital Shanghai Jiao Tong University School of Medicine Shanghai China.

出版信息

MedComm (2020). 2025 Sep 14;6(10):e70350. doi: 10.1002/mco2.70350. eCollection 2025 Oct.

Abstract

Effective early prediction of acute pancreatitis (AP) severity remains an unmet clinical need due to limited molecular characterization of systemic immune responses. We performed integrated single-cell RNA sequencing with T- and B-cell receptor profiling on peripheral blood mononuclear cells from AP patients ( = 7) at days 1, 3, and 7 after admission. Immune landscape analysis revealed marked inter-patient heterogeneity, with a distinct expansion of MZB1-expressing plasma cells that were strongly associated with complicated AP and recovery. Functional validation in an independent cohort ( = 14) confirmed disease-associated plasma cell markers, alongside altered serum immunoglobulin and cytokine profiles ( = 32). From these findings, we established a nine-gene B-cell-derived transcriptomic signature (, , , , , , , , and ) predictive of AP severity. This model demonstrated high discriminative performance in internal validation ( = 114; AUROC > 0.95, superior to standard clinical scoring systems), and sustained accuracy in external validation cohorts of AP ( = 87) and AP combined with non-AP sepsis ( = 174) for predicting persistent organ failure. Our study identifies a mechanistic and predictive role for MZB1⁺ plasma cells in AP pathogenesis, offering a novel immune-based stratification strategy with potential for precision clinical management.

摘要

由于全身免疫反应的分子特征有限,急性胰腺炎(AP)严重程度的有效早期预测仍是一项未满足的临床需求。我们对入院后第1天、第3天和第7天的AP患者(n = 7)的外周血单个核细胞进行了T细胞和B细胞受体谱分析的综合单细胞RNA测序。免疫图谱分析揭示了患者间明显的异质性,表达MZB1的浆细胞显著扩增,这与复杂性AP和恢复密切相关。在一个独立队列(n = 14)中的功能验证证实了疾病相关的浆细胞标志物,以及血清免疫球蛋白和细胞因子谱的改变(n = 32)。基于这些发现,我们建立了一个预测AP严重程度的九基因B细胞来源的转录组特征(BCL2、BCL6、CXCR4、IRF4、MYC、PAX5、SOCS1、TOX和XBP1)。该模型在内部验证(n = 114;AUROC > 0.95,优于标准临床评分系统)中表现出高鉴别性能,并且在AP(n = 87)和AP合并非AP脓毒症(n = 174)的外部验证队列中预测持续性器官衰竭时具有持续的准确性。我们的研究确定了MZB1⁺浆细胞在AP发病机制中的机制和预测作用,提供了一种基于免疫的新型分层策略,具有精准临床管理的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/35c5/12434316/18fdf8431e85/MCO2-6-e70350-g003.jpg

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