Lou Ning, Dai Liyuan, Gao Ruyun, Yang Jianliang, Gui Lin, Yang Sheng, Liu Peng, Shi Yuankai, Han Xiaohong
Clinical Pharmacology Research Center, Beijing Key Laboratory of Clinical PK & PD Investigation for Innovative Drugs, NMPA Key Laboratory for Clinical Research and Evaluation of Drug, State Key Laboratory of Complex Severe and Rare Diseases, Peking Union Medical College Hospital, Chinese Academy of Medical Sciences & Peking Union Medical College, Beijing, 100730, China.
Department of Medical Oncology, Beijing Key Laboratory of Clinical Study on Anticancer Molecular Targeted Drugs, National Cancer Center/National Clinical Research Center for Cancer/Cancer Hospital, Chinese Academy of Medical Sciences & Peking Union Medical College, Beijing, 100021, China.
Sci China Life Sci. 2025 May 15. doi: 10.1007/s11427-024-2849-2.
Current subtyping methods of diffuse large B-cell lymphoma (DLBCL) could not satisfy the clinical demands for risk assessment and prognostic prediction. We aimed to investigate the prognostic effect of autophagy-related genes (ARGs) in DLBCL. Transcriptomic data of 1,409 DLBCL patients, 531 healthy controls (HCs), and single-cell sequencing data of 4 DLBCL were included. Validation involved spatial transcriptomics from 10 DLBCL patients and 110 DLBCL proteomic data from a local cohort. We identified 153 differentially expressed ARGs between DLBCL patients (n=48) and HCs (n=531), classifying 414 DLBCL patients into two subtypes based on autophagy heterogeneity. Subtype I, characterized by upregulated T regulatory (Treg) cells (P<0.0001) and T follicular helper (Tfh) cells (P=0.0012), showed a superior prognosis (P=0.035). Eight prognostic ARGs were selected to construct an autophagy-related model, dividing patients into low- and high-risk groups. Kaplan-Meier survival analysis revealed significantly better outcomes for the low-risk group in both the discovery (P<0.0001) and validation cohorts (P=0.0041). High-risk patients exhibited elevated IDO1 (P=0.042) and LAG3 (P<0.001) levels. Among the eight signature proteins, higher FAS was further verified to indicate a better prognosis in the local cohort (n=110) using antibody array (P=0.0083). FAS was primarily expressed in T cells such as Treg and Tfh cells and was elevated in non-progressive disease patients. FAS-positive T cells showed increased interferon-gamma (normalized enrichment score (NES)=2.196, FDR<0.0001) and alpha (NES=1.836, FDR<0.01) response activities. We constructed an autophagy-related model and identified FAS as a prognostic biomarker. FAS+ Treg and Tfh cell-enriched TME indicated a favorable prognosis.
弥漫性大B细胞淋巴瘤(DLBCL)目前的亚型分类方法无法满足临床对风险评估和预后预测的需求。我们旨在研究自噬相关基因(ARG)在DLBCL中的预后作用。纳入了1409例DLBCL患者、531例健康对照(HC)的转录组数据以及4例DLBCL的单细胞测序数据。验证涉及来自10例DLBCL患者的空间转录组学数据和来自一个本地队列的110例DLBCL蛋白质组数据。我们鉴定出DLBCL患者(n = 48)和HC(n = 531)之间有153个差异表达的ARG,基于自噬异质性将414例DLBCL患者分为两个亚型。I型以调节性T(Treg)细胞(P < 0.0001)和滤泡辅助性T(Tfh)细胞上调(P = 0.0012)为特征,显示出较好的预后(P = 0.035)。选择8个预后ARG构建自噬相关模型,将患者分为低风险和高风险组。Kaplan-Meier生存分析显示,在发现队列(P < 0.0001)和验证队列(P = 0.0041)中,低风险组的结局均明显更好。高风险患者的吲哚胺2,3-双加氧酶1(IDO1)(P = 0.042)和淋巴细胞活化基因3(LAG3)(P < 0.001)水平升高。在8种标志性蛋白质中,使用抗体阵列进一步验证了较高的FAS水平在本地队列(n = 110)中表明预后较好(P = 0.0083)。FAS主要在Treg和Tfh等T细胞中表达,在非进展性疾病患者中升高。FAS阳性T细胞显示干扰素-γ(标准化富集分数(NES)= 2.196,FDR < 0.0001)和α(NES = 1.836,FDR < 0.01)反应活性增加。我们构建了自噬相关模型,并将FAS鉴定为预后生物标志物。富含FAS + Treg和Tfh细胞的肿瘤微环境表明预后良好。
