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外周血Treg/Th17比值作为新诊断多发性骨髓瘤预后免疫生物标志物的意义及其与1q21获得/扩增的相关性。

Significance of the peripheral blood Treg/Th17 ratio as a prognostic immune biomarker in newly diagnosed multiple myeloma and its correlation with 1q21 gain/amplification.

作者信息

Wen Jingjing, Zhou Qiaolin, Xu Fang, Yue Jing, Zhang Ya, Liu Yiping, Su Jing, Liang Xiaogong

机构信息

Department of Hematology, Mianyang Central Hospital, School of Medicine, University of Electronic Science and Technology of China, National Health Commission Key Laboratory of Nuclear Technology Medical Transformation, Mianyang, Sichuan, China.

出版信息

Front Immunol. 2025 May 29;16:1595613. doi: 10.3389/fimmu.2025.1595613. eCollection 2025.

Abstract

BACKGROUND

Regulatory T (Treg) and T helper 17 (Th17) cells play opposing roles in immune responses, and their balance critically regulates the multiple myeloma (MM) microenvironment. Despite advances in immunotherapy, current risk stratification lacks immune biomarkers.

METHODS

We collected the peripheral blood and bone marrow samples from MM patients to investigate the relationships among 1q21 gain/amplification, the Treg/Th17 ratio, and gene abnormalities at diagnosis, remission, and relapse. Additionally, we evaluated the prognostic impact of the Treg/Th17 ratio.

RESULTS

A total of 130 newly diagnosed MM patients were enrolled, with 82 patients evaluated for 1q21 gain/amplification. During remission, patients with 1q21 gain/amplification had a significantly higher Treg/Th17 ratio (1.59 vs. 0.85, P = 0.042) and expression levels (70.54% vs. 32.76%, P = 0.042) compared to those without 1q21 gain/amplification. Furthermore, patients with an elevated Treg/Th17 ratio (>0.7) during remission exhibited slightly higher expression (45.70% vs. 30.60%) than those with lower ratios (P = 0.451). Patients achieving partial response or better exhibited significantly higher Th17 levels (3.34%, range: 0.19-10.80%) at diagnosis compared to those without remission (0.29%, range: 0-2.18%, P = 0.033). The group of elevated Treg/Th17 ratio (> 1.0) at diagnosis exhibited significantly shorter PFS compared to the reduced ratio (≤ 1.0) group (13.87 months vs. 30.67 months, P = 0.006). R2-ISS staging showed no significant impact on PFS (P = 0.236). By assigning scores to R2-ISS stages and elevated Treg/Th17 ratio at diagnosis, patients were stratified into low-risk (1-3 scores) and high-risk (4-5 scores) groups. High-risk patients exhibited significantly worse PFS compared to low-risk patients (P = 0.022). The combined model integrating R2-ISS staging and Treg/Th17 ratio achieved a concordance index(C-index) of 0.8, surpassing the C-index of R2-ISS staging alone (0.562), demonstrating better predictive performance.

CONCLUSION

A potential mechanistic connection exists between 1q21 gain/amplification and immunosuppression, and the role of the gene in this mechanism has garnered substantial interest. Patients with a higher Treg/Th17 ratio at diagnosis are more prone to relapse. The combination of R2-ISS staging and the Treg/Th17 ratio at diagnosis demonstrates stronger predictive ability for relapse.

摘要

背景

调节性T(Treg)细胞和辅助性T细胞17(Th17)在免疫反应中发挥相反作用,它们之间的平衡对多发性骨髓瘤(MM)微环境起着关键调节作用。尽管免疫治疗取得了进展,但目前的风险分层缺乏免疫生物标志物。

方法

我们收集了MM患者的外周血和骨髓样本,以研究1q21获得/扩增、Treg/Th17比值与诊断、缓解及复发时基因异常之间的关系。此外,我们评估了Treg/Th17比值对预后的影响。

结果

共纳入130例新诊断的MM患者,其中82例患者进行了1q21获得/扩增评估。缓解期,与无1q21获得/扩增的患者相比,有1q21获得/扩增的患者Treg/Th17比值显著更高(1.59对0.85,P = 0.042),且表达水平更高(70.54%对32.76%,P = 0.042)。此外,缓解期Treg/Th17比值升高(>0.7)的患者表达略高于比值较低的患者(45.70%对30.60%,P = 0.451)。达到部分缓解或更好缓解的患者在诊断时Th17水平显著高于未缓解患者(3.34%,范围:0.19 - 10.80%对0.29%,范围:0 - 2.18%,P = 0.033)。诊断时Treg/Th17比值升高(>1.0)的组与比值降低(≤1.0)的组相比,无进展生存期显著更短(13.87个月对30.67个月,P = 0.006)。R2-ISS分期对无进展生存期无显著影响(P = 0.236)。通过对R2-ISS分期和诊断时升高的Treg/Th17比值进行评分,将患者分为低风险(1 - 3分)和高风险(4 - 5分)组。高风险患者的无进展生存期显著差于低风险患者(P = 0.022)。整合R2-ISS分期和Treg/Th17比值的联合模型一致性指数(C指数)为0.8,超过单独R2-ISS分期的C指数(0.562),显示出更好的预测性能。

结论

1q21获得/扩增与免疫抑制之间存在潜在的机制联系,且该基因在这一机制中的作用已引起广泛关注。诊断时Treg/Th17比值较高的患者更容易复发。R2-ISS分期与诊断时的Treg/Th17比值相结合对复发具有更强的预测能力。

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