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Serum proteomics identify potential biomarkers for nasopharyngeal carcinoma sensitivity to radiotherapy

机译:血清蛋白质组学确定鼻咽癌对放疗敏感性的潜在生物标志物

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摘要

Radiotherapy is the primary treatment option for nasopharyngeal carcinoma (NPC). Local recurrence and metastasis caused by radioresistance become a bottleneck of curative effect for patients with NPC. Currently, serum predictive biomarkers of radioresistance are scare. We enrolled NPC patients, who underwent radiotherapy in the Department of Oncology, Xiangya Hospital, Central Southern University, and analyzed the serum proteins profiles in NPC patients using with quantitative label-free proteomics using ultra-definition MS. Patients were divided into those who were radioresistant and radiosensitive by the overall reduction (≤50% or >50%, respectively) in tumor extent. The MS/MS spectrum database search identified 911 proteins and 809 proteins are quantitatable. Eight proteins significantly up-regulated and 12 serum proteins were significantly down-regulated in the radioresistance group compared with radiosensitivity group (P<0.05). Finally, five proteins entered the optimal models, including secreted protein acidic and cysteine rich (SPARC) (P =0.032), serpin family D member 1S (ERPIND1) (P =0.040), complement C4B (C4B) (P =0.017), peptidylprolyl Isomerase B (PPIB) (P =0.042), and family with sequence similarity 173 member A (FAM173A) (P =0.017). In all patient, the area under the curves (AUC) for SPARC, SERPIND, C4B, PPIB, and FAM173A were 0.716 (95% CI: 0.574–0.881), 0.697 (95% CI: 0.837–0.858), 0.686 (95% CI: 0.522–0.850), 0.668 (95% CI: 0.502–0.834) and 0.657 (95% CI: 0.512–0.825), respectively. The AUC of five selected proteins was 0.968 (95% CI: 0.918–1.000) with the sensitivity of 0.941 and the specificity of 0.926. Our result indicated that a panel including five serum protein (SPARC SERPIND1 C4B PPIB FAM173A) based on serum proteomics provided a high discrimination ability for radiotherapy effects in NPC patients. Studies with larger sample size and longer follow-up outcome are required.
机译:放射疗法是鼻咽癌(NPC)的主要治疗选择。由放射线抗性引起的局部复发和转移成为NPC患者治疗效果的瓶颈。当前,放射线抗性的血清预测性生物标志物令人恐惧。我们招募了在中南大学湘雅医院肿瘤科接受放射治疗的NPC患者,并使用超高清MS结合定量无标签蛋白质组学技术分析了NPC患者的血清蛋白谱。根据肿瘤范围的总体减少(分别≤50%或> 50%)将患者分为放射耐受和放射敏感性患者。 MS / MS光谱数据库搜索确定了911个蛋白和809个蛋白是可定量的。与放射敏感性组相比,放射抵抗组中有8种蛋白显着上调,而12种血清蛋白显着下调(P <0.05)。最后,五种蛋白质进入了最佳模型,包括分泌的酸性蛋白质和富含半胱氨酸的蛋白质(SPARC)(P = 0.032),丝氨酸蛋白酶抑制剂家族D成员1S(ERPIND1)(P = 0.040),补体C4B(C4B)(P = 0.017),肽基脯氨酰基异构酶B(PPIB)(P = 0.042),以及具有序列相似性的173成员A家族(FAM173A)(P = 0.017)。在所有患者中,SPARC,SERPIND,C4B,PPIB和FAM173A的曲线下面积(AUC)分别为0.716(95%CI:0.574-0.881),0.697(95%CI:0.837-0.858),0.686(95% CI:0.522-0.850),0.668(95%CI:0.502-0.834)和0.657(95%CI:0.512-0.825)。五个选定蛋白的AUC为0.968(95%CI:0.918-1.000),灵敏度为0.941,特异性为0.926。我们的结果表明,基于血清蛋白质组学的包括五种血清蛋白(SPARC SERPIND1 C4B PPIB FAM173A)的检测组为NPC患者的放射治疗效果提供了高判别能力。需要更大样本量和更长随访结果的研究。

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