甘露糖受体和CD163作为结直肠癌新生物标志物的鉴定

IF 1.9
Dongbing Ding, Yao Yao, Changming Yang, Songbai Zhang
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引用次数: 19

摘要

目的探讨甘露糖受体(MR)和CD163在结直肠癌(CRC)中的临床意义。采用酶联免疫吸附试验(ELISA)和免疫组织化学(IHC)进行分析。CRC患者术前血清MR和CD163水平分别为0.153 ~ 0.804 μg/ml(中位数为0.359 μg/ml)和0.319 ~ 1.314 μg/ml(中位数为0.685 μg/ml)。引人注目的是,CRC患者术前血清MR和CD163水平显著高于健康人(P< 0.0001)。ROC分析显示,血清MR和CD163的最佳诊断临界值分别为0.3485 μg/ml (AUC 0.7205,敏感性54.82%,特异性80.46%)和0.6111 μg/ml (AUC 0.7463,敏感性62.65%,特异性80.46%)。血清MR与CD163联合检测可显著提高诊断准确率(AUC 0.7968,灵敏度69.28%,特异性77.01%)。CRC患者术前血清MR、CD163水平与血清CEA、CA19-9、CA72-4浓度有显著相关性(P< 0.05)。血清中MR和CD163的高表达与总生存期缩短显著相关(P< 0.05),并被证明是不良预后因素(P< 0.05)。MR和CD163在结直肠癌组织中的表达显著高于癌旁组织(P< 0.001)。MR和CD163在结直肠癌组织中的高表达也与较短的总生存期显著相关(P< 0.05)。血清或结直肠癌组织中MR、CD163表达与淋巴转移程度均呈正相关(P< 0.0001)。综上所述,MR和CD163可能是结直肠癌患者的新型生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Identification of mannose receptor and CD163 as novel biomarkers for colorectal cancer.

The aim of present study was to investigate the clinical significances of mannose receptor (MR) and CD163 in colorectal cancer (CRC). Enzyme-linked immunosorbent assay (ELISA) and immunohistochemistry (IHC) were utilized for this analysis. Preoperative serum MR and CD163 levels ranged from 0.153 to 0.804 μg/ml (median = 0.359 μg/ml) and from 0.319 to 1.314 μg/ml (median = 0.685 μg/ml) in CRC patients respectively. Strikingly, preoperative serum levels of MR and CD163 were significantly increased in CRC patients than in healthy individuals (P< 0.0001). ROC analyses suggested that the optimum diagnostic cut-offs for serum MR and CD163 were 0.3485 μg/ml (AUC 0.7205, sensitivity 54.82%, and specificity 80.46%) and 0.6111 μg/ml (AUC 0.7463, sensitivity 62.65%, and specificity 80.46%) respectively. Detection of serum MR and CD163 together obviously enhanced the diagnostic accuracy (AUC 0.7968, sensitivity 69.28%, and specificity 77.01%). Then, preoperative serum MR and CD163 levels correlated significantly with serum CEA, CA19-9 and CA72-4 concentrations in CRC patients (P< 0.05). High MR and CD163 expression in serum was associated significantly with shorter overall survival (P< 0.05) and demonstrated as adversely prognostic factors (P< 0.05). Further, expression of MR and CD163 in CRC tissues was significantly higher than that in para-cancer tissues (P< 0.001). High expression of MR and CD163 in CRC tissues also correlated significantly with shorter overall survival (P< 0.05). MR and CD163 expression in serum or CRC tissues all correlated positively with the degree of lymphatic metastasis (P< 0.0001). In conclusion, MR and CD163 may be novel biomarkers for CRC patients.

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