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Anti-FIRs (PUF60) auto-antibodies are detected in the sera of early-stage colon cancer patients

机译:在早期结肠癌患者的血清中检测到抗FIR(PUF60)自身抗体

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摘要

Anti-PUF60, poly(U)-binding-splicing factor, autoantibodies are reported to be detected in the sera of dermatomyositis and Sjogren's syndrome that occasionally associated with malignancies. PUF60 is identical with far-upstream element-binding protein-interacting repressor (FIR) that is a transcriptional repressor of c-myc gene. In colorectal cancers, a splicing variant of FIR that lacks exon2 (FIRΔexon2) is overexpressed as a dominant negative form of FIR. In this study, to reveal the presence and the significance of anti-FIRs (FIR/FIRΔexon2) antibodies in cancers were explored in the sera of colorectal and other cancer patients. Anti-FIRs antibodies were surely detected in the preoperative sera of 28 colorectal cancer patients (32.2% of positive rates), and the detection rate was significantly higher than that in healthy control sera (Mann–Whitney U test, p < 0.01). The level of anti-FIRs antibodies significantly decreased after the operation (p < 0.01). Anti-FIRs antibodies were detected in the sera of early-stage and/or recurrent colon cancer patients in which anti-p53 antibodies, CEA, and CA19-9 were not detected as well as in the sera of other cancer patients. Furthermore, the area under the curve of receiver operating characteristic for anti-FIRs antibodies was significantly larger (0.85) than that for anti-p53 antibodies or CA19-9. In conclusions, the combination of anti-FIRs antibodies with other clinically available tumor markers further improved the specificity and accuracy of cancer diagnosis.
机译:据报道,在皮肌炎和干燥综合征(Sjogren's syndrome)的血清中检测到抗PUF60,poly(U)-结合剪接因子,自身抗体,这些血清有时与恶性肿瘤有关。 PUF60与远端上游元素结合蛋白相互作用阻遏物(FIR)相同,后者是c-myc基因的转录阻遏物。在大肠癌中,缺少外显子2(FIRΔexon2)的FIR剪接变体被过度表达为FIR的主要阴性形式。在这项研究中,揭示大肠癌和其他癌症患者血清中抗FIR(FIR /FIRΔexon2)抗体的存在及其意义。在28例大肠癌患者的术前血清中肯定检测到抗FIRs抗体(阳性率32.2%),并且检出率明显高于健康对照血清(Mann-Whitney U检验,p <0.01)。手术后抗FIRs抗体水平显着降低(p <0.01)。在未检测到抗p53抗体,CEA和CA19-9的早期和/或复发性结肠癌患者的血清中以及在其他癌症患者的血清中检测到抗FIRs抗体。此外,抗FIRs抗体的受体工作特性曲线下面积明显大于抗p53抗体或CA19-9的面积(0.85)。总之,抗FIRs抗体与其他临床可用的肿瘤标志物的组合进一步提高了癌症诊断的特异性和准确性。

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