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Leuk Lymphoma. 2012 Jun;53(6):1023-31. doi: 10.3109/10428194.2011.631638. Epub 2011 Dec 6.
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细胞遗传学定义的侵袭性疾病与 CLL/SLL 患者的细胞因子失调有关。

Aggressive disease defined by cytogenetics is associated with cytokine dysregulation in CLL/SLL patients.

机构信息

Division of Hematology/Oncology/Cell Therapy, Rush University Medical Center, 1725 W. Harrison St., Chicago, IL 60612, USA.

出版信息

J Leukoc Biol. 2013 Jan;93(1):161-70. doi: 10.1189/jlb.0612301. Epub 2012 Nov 7.

DOI:10.1189/jlb.0612301
PMID:23136257
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3525834/
Abstract

Early treatment of CLL/SLL does not impact survival-reflecting limitations in detecting progression early and identifying asymptomatic patients likely to benefit from early treatment. Improved understanding of CLL/SLL biology would identify better prognostic/predictive markers. This study attempts to address these issues by determining the relationship between cytokine aberrations and poor clinical outcomes in CLL/SLL in the context of a genetic-based prognostic model. Fifty-nine serum cytokines/chemokines were measured in 28 untreated CLL/SLL patients. Patients were stratified as GR or int/PR using cytogenetics. Comparison of CLL/SLL with 28 HCs revealed increased expression of Th2 cytokines (IL-10, IL-5, sIL-2Rα; P≤0.01) and decreased levels of Th1 cytokines (IL-17, IL-23, IFN-γ; P≤0.003). In a multivariate analysis of GR versus int/PR groups, differential expression of sIL-2Rα maintained significance with increased expression in int/PR CLL/SLL. With median follow-up of 54.3 months after diagnosis, four patients incurred disease progression, with an IL-17/sIL-2Rα model predicting need for treatment in all cases. In summary, specific cytokine signatures are associated with genetically defined aggressive disease and predict need for therapy. This suggests utility in detecting disease progression early, identifying those likely to incur a survival advantage with early treatment, and directing future therapy.

摘要

早期治疗 CLL/SLL 并不影响生存——这反映了早期检测进展和识别可能从早期治疗中获益的无症状患者的局限性。对 CLL/SLL 生物学的深入了解将确定更好的预后/预测标志物。本研究试图通过确定细胞因子异常与遗传预后模型背景下 CLL/SLL 不良临床结局之间的关系来解决这些问题。在 28 例未经治疗的 CLL/SLL 患者中测量了 59 种血清细胞因子/趋化因子。根据细胞遗传学将患者分层为 GR 或 int/PR。与 28 例 HC 相比,CLL/SLL 显示出 Th2 细胞因子(IL-10、IL-5、sIL-2Rα;P≤0.01)表达增加和 Th1 细胞因子(IL-17、IL-23、IFN-γ;P≤0.003)水平降低。在 GR 与 int/PR 组的多变量分析中,sIL-2Rα 的差异表达与 int/PR CLL/SLL 中的表达增加保持显著相关。在诊断后中位随访 54.3 个月时,4 例患者发生疾病进展,IL-17/sIL-2Rα 模型预测所有病例均需要治疗。总之,特定的细胞因子特征与遗传上定义的侵袭性疾病相关,并预测需要治疗。这表明它可用于早期检测疾病进展,识别可能从早期治疗中获得生存优势的患者,并指导未来的治疗。