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首页> 外文期刊>Oncoimmunology. >Serum anti-MDM2 and anti-c-Myc autoantibodies as biomarkers in the early detection of lung cancer
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Serum anti-MDM2 and anti-c-Myc autoantibodies as biomarkers in the early detection of lung cancer

机译:血清抗MDM2和抗C-MYC自身抗体作为生物标志物在早期发现肺癌

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摘要

This study aims to investigate the clinical significance of serum autoantibodies against MDM2 and c-Myc and evaluate their feasibility in the immunodiagnosis of lung cancer. 50 sera samples with 43 available paired lung cancer tissue and adjacent normal tissue slides with follow up information and 44 sera from normal human controls (NHC) were used in the research group. Another 62 lung cancer sera and 43 NHC sera were used in the validation group. The results of IHC showed that MDM2 and c-Myc protein were overexpressed in lung cancer tissues compared to adjacent normal tissues (p < 0.001). Likewise, significantly higher levels of serum autoantibodies against MDM2 and c-Myc were found in lung cancer compared to NHC both in research and validation groups. Further analysis on IHC and ELISA results showed that serum level of autoantibodies against these two TAAs were positively associated with tissue staining scores (both p < 0.05). The area under curve (AUC) values of anti-MDM2 and anti-cMyc autoantibodies for discriminating lung cancers from NHC were 0.698 and 0.636 in research group, 0.777 and 0.815 in the validation group, respectively. Both anti-MDM2 and anti-c-Myc autoantibodies can discriminate stage I lung cancer patients from NHC with AUC values of 0.703 and 0.662. Kaplan-Meier analysis showed that higher level of serum anti-c-Myc autoantibodies was significantly related to shortened disease-free survival (DFS) (p = 0.041). In conclusion, our finding suggested that serum MDM2 and c-Myc autoantibodies may have the potential to serve as non-invasive diagnostic biomarkers in patients with lung cancer.
机译:本研究旨在探讨血清自身抗体对MDM2和C-MYC的临床意义,评价它们在肺癌免疫诊断中的可行性。研究组使用了50种具有43种可用配对肺癌组织和相邻的正常组织载玻片的血清样品,以及来自正常人体对照(NHC)的邻近的正常组织载玻片。在验证组中使用另外62例肺癌血清和43个NHC血清。与相邻的正常组织相比,IHC的结果表明,MDM2和C-MYC蛋白在肺癌组织中过表达(P <0.001)。同样,与研究和验证组中的NHC相比,在肺癌中发现了对MDM2和C-MYC的显着更高的血清自身抗体水平。 IHC和ELISA结果的进一步分析表明,针对这两个TAA的血清自身抗体水平与组织染色分数正相关(P <0.05)。抗MDM2的曲线(AUC)的区域和用于鉴别NHC的肺癌的抗CMYC自身抗体的区域分别在研究组中为0.698和0.636,分别在验证组中为0.777和0.815。抗MDM2和抗C-MYC自身抗体均可歧视Ⅰ期肺癌患者,NHC具有0.703和0.662的AUC值。 Kaplan-Meier分析表明,血清抗C-myc自身抗体较高含量与缩短无病存活(DFS)有显着相关(P = 0.041)。总之,我们的发现表明,血清MDM2和C-MYC自身抗体可能有可能作为肺癌患者的非侵入性诊断生物标志物。

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