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白细胞介素-10 基因多态性与霍奇金淋巴瘤患者免于治疗失败相关。

Interleukin-10 gene polymorphisms are associated with freedom from treatment failure for patients with Hodgkin lymphoma.

机构信息

Department of Hematology and Oncology, Medical Center of the Georg-August-University Göttingen, 37099 Göttingen, Germany.

出版信息

Oncologist. 2013;18(1):80-9. doi: 10.1634/theoncologist.2012-0291. Epub 2013 Jan 8.

Abstract

BACKGROUND

Hodgkin lymphoma (HL) is a lymphoid malignancy characterized by the production of various cytokines possibly involved in immune deregulation. Interleukin-10 (IL-10) serum levels have been associated with clinical outcome in patients with HL. Because host genetic variations are known to alter the expression and function of cytokines and their receptors, we investigated whether genetic variations influence clinical outcome of patients with HL.

METHODS

A total of 301 patients with HL who were treated within randomized trials by the German Hodgkin Study Group were included in this exploratory retrospective study. Gene variations of IL-10 (IL-10(-597AC), rs1800872; IL-10(-824CT), rs1800871; IL-10(-1087AG), rs1800896; IL-10(-3538AT), rs1800890; IL-10(-6208CG), rs10494879; IL-10(-6752AT), rs6676671; IL-10(-7400InDel)), IL-13 (IL-13(-1069CT), rs1800925; IL-13(Q144R), rs20541), and IL-4R (IL-4R(I75V), rs1805010; IL-4R(Q576R), rs1801275) were genotyped.

RESULTS

Inferior freedom from treatment failure (FFTF) was found in patients harboring the IL-10(-597AA), IL-10(-824TT), or the IL-10(-1087AA) genotype. In contrast, the IL-10(-1087G-824C-597C) haplotype present in about 48% of analyzed HL patients is nominally significant for a better FFTF in a Cox-Regression model accounting for stage and treatment. No associations were observed between the other IL-10 gene variations, IL-13(-1069CT), IL-13(Q144R), IL-4R(I75V), IL-4R(Q576R) and the clinical outcome of patients with HL.

CONCLUSIONS

Our study provides further evidence that proximal IL-10 promoter gene variations are associated with clinical course of patients with HL. However, treatment success and survival rates are already at a very high rate, supporting the need to design studies focusing on identification of predictors to reduce the side effects of therapy.

摘要

背景

霍奇金淋巴瘤(HL)是一种淋巴恶性肿瘤,其特征是产生各种细胞因子,这些细胞因子可能参与免疫失调。白细胞介素 10(IL-10)的血清水平与 HL 患者的临床预后相关。由于宿主遗传变异可改变细胞因子及其受体的表达和功能,我们研究了遗传变异是否影响 HL 患者的临床预后。

方法

本研究为回顾性探索性研究,共纳入 301 例在德国霍奇金研究组的随机临床试验中接受治疗的 HL 患者。对 IL-10(IL-10(-597AC),rs1800872;IL-10(-824CT),rs1800871;IL-10(-1087AG),rs1800896;IL-10(-3538AT),rs1800890;IL-10(-6208CG),rs10494879;IL-10(-6752AT),rs6676671;IL-10(-7400InDel))、IL-13(IL-13(-1069CT),rs1800925;IL-13(Q144R),rs20541)和 IL-4R(IL-4R(I75V),rs1805010;IL-4R(Q576R),rs1801275)的基因变异进行了基因分型。

结果

携带 IL-10(-597AA)、IL-10(-824TT)或 IL-10(-1087AA)基因型的患者,无治疗失败(FFTF)的自由度较差。相反,在大约 48%的分析 HL 患者中存在的 IL-10(-1087G-824C-597C)单倍型,在考虑到分期和治疗的 Cox 回归模型中,对 FFTF 具有名义显著性。在 HL 患者中,未观察到其他 IL-10 基因变异、IL-13(-1069CT)、IL-13(Q144R)、IL-4R(I75V)、IL-4R(Q576R)与临床结局之间存在相关性。

结论

本研究进一步证明,IL-10 启动子基因的近端变异与 HL 患者的临床病程有关。然而,治疗成功率和生存率已经非常高,这支持了需要设计研究来确定预测因子以减少治疗副作用的需要。

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