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Ratio of Autoantibodies of Tumor Suppressor AIMP2 and Its Oncogenic Variant Is Associated with Clinical Outcome in Lung Cancer

机译:肿瘤抑制因子AIMP2自身抗体的比例及其致癌变异与肺癌的临床结果相关

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Aminoacyl-tRNA synthetase-interacting multi-functional protein 2 (AIMP2) works as potent tumor suppressor, while its splicing variant lacking exon 2 (AIMP2-DX2) competes with AIMP2 for binding to target proteins and compromises its anti-tumor activity. Assuming that AIMP2 and its variant AIMP2-DX2 could be released out to human sera in pathological condition, we investigated the diagnostic and prognostic usefulness of autoantibodies against AIMP2 and AIMP2-DX2 by measuring their serum levels in 80 normal and lung cancer samples that were matched in age, gender and smoking status. The area under the curve of AIMP2-DX2, AIMP2, and AIMP2-DX2/AIMP2 autoantibody ratio was low (0.416, 0.579, and 0.357, respectively), suggesting limited diagnostic value. A total of 165 lung cancer patients were classified into low and high AIMP2-DX2, AIMP2, and AIMP2-DX2/AIMP2 based on the median expression of each parameter. The high AIMP2-DX2 group was older and had larger tumors (>3 cm) than the low AIMP2-DX2 group. The high AIMP2-DX2/AIMP2 group had higher CYFRA-21 levels and significantly shorter overall survival than the low AIMP2-DX2/AIMP2 group (18.6 vs. 48.9 months, P = 0.021, Log Rank Test). Taken together, autoantibodies against AIMP2-DX2 and AIMP2 are detectable in the human blood and the increased ratio of AIMP2-DX2/AIMP2 is related to poor clinical outcome of lung cancer.
机译:与氨酰基-tRNA合成酶相互作用的多功能蛋白2(AIMP2)可作为有效的肿瘤抑制因子,而缺少外显子2的剪接变体(AIMP2-DX2)与AIMP2竞争与靶蛋白的结合并损害其抗肿瘤活性。假设AIMP2及其变体AIMP2-DX2可以在病理条件下释放到人血清中,我们通过测量80例正常和肺癌样本中的血清对AIMP2和AIMP2-DX2的自身抗体的水平,研究了它们的诊断和预后价值年龄,性别和吸烟状况。 AIMP2-DX2,AIMP2和AIMP2-DX2 / AIMP2自身抗体比率曲线下的面积较低(分别为0.416、0.579和0.357),表明诊断价值有限。根据每个参数的中位数表达,将总共165位肺癌患者分为AIMP2-DX2,AIMP2和AIMP2-DX2 / AIMP2。高AIMP2-DX2组比低AIMP2-DX2组年龄更大,肿瘤更大(> 3 cm)。高AIMP2-DX2 / AIMP2组比低AIMP2-DX2 / AIMP2组具有更高的CYFRA-21水平,且总生存期明显缩短(18.6 vs. 48.9个月,P = 0.021,对数秩检验)。两者合计,在人类血液中可检测到针对AIMP2-DX2和AIMP2的自身抗体,并且AIMP2-DX2 / AIMP2比例的增加与肺癌的临床预后不良有关。

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