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Autoantibody profiling of alveolar rhabdomyosarcoma patients unveils tumor-associated antigens with diagnostic and prognostic significance

机译:肺泡横纹肌肉瘤患者的自身抗体分析揭示了肿瘤相关的抗原诊断和预后意义

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摘要

Alveolar rhabdomyosarcoma (ARMS) is a highly aggressive subtype of childhood cancer for which efficacious treatments are needed. Immunotherapy represents a new therapeutic opportunity to pursue, but it requires the identification of worthwhile tumor antigens. Herein, we exploited the capacity of ARMS autoantibodies to recognize tumor self-antigens, probing human protein microarrays with plasma from ARMS patients and healthy subjects. We assessed the autoantibody response in ARMS, validated data with independent techniques, and estimated autoantibodies diagnostic and prognostic significance by receiver-operator characteristic curves (ROC), uni- and multivariate analysis. Of the 48 tumor antigens identified, General Transcription Factor II–I (GTF2i) and Protocadherin Gamma Subfamily C5 (PCDHGC5) were selected as candidate targets to validate tumor-restricted antigen expression and autoantibody reactivity through an independent technique and wider cohort of cases. GTF2i and PCDHGC5 overexpression was observed in tumor tissues compared to normal counterparts, and anti-GTF2i and -PCDHGC5 autoantibodies were found able to distinguish ARMS patients from healthy subjects as well as cases with different histology. Moreover, low levels of PCDHGC5 autoantibodies characterized patients with worse event-free survival and proved to be an independent negative prognostic factor. This approach provided the first comprehensive autoantibody profile of ARMS, gave novel insights into the immune response of this malignancy and paved the way toward novel potential antibody-based therapeutic applications suitable to improve the survival of ARMS patients.
机译:泡型横纹肌肉瘤(ARMS)是儿童癌症的高度侵袭性亚型都需要其有效的治疗方法。免疫治疗代表了一种新的治疗机会去追求,但它需要值得肿瘤抗原的识别。在此,我们利用ARMS自身抗体识别肿瘤自身抗原的能力,探测人类蛋白质微阵列与来自组患者和健康受试者的血浆。我们评估了由接收器操作特征曲线(ROC),单向和多变量分析中ARMS自身抗体应答,具有独立的技术验证的数据,以及估计的自身抗体的诊断和预后意义。鉴定的48种肿瘤抗原的,通用转录因子II-I(GTF2i)和Protocadherinγ亚族C5(PCDHGC5)通过一个独立的技术和箱子更宽队列选择作为候选目标来验证肿瘤限制性抗原表达和自身抗体的反应性。在肿瘤组织中观察到GTF2i和PCDHGC5过表达相比正常对应,和抗GTF2i和-PCDHGC5自身抗体被发现能够区分患者ARMS来自健康受试者,以及与不同的组织学情况。此外,PCDHGC5自身抗体水平低的特点患者更差的无事件生存率,并证明是一个独立的不良预后因素。这种方法提供武器的第一个综合性自身抗体轮廓,给了新的见解这种恶性肿瘤的免疫反应,并朝着铺平适合于改善武器患者的生存新的潜在的基于抗体的治疗性应用程序的方式。

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