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Fucosylated α1-acid glycoprotein as a biomarker to predict prognosis following tumor immunotherapy of patients with lung cancer

机译:岩氧化α1-酸糖蛋白作为生物标志物,以预测肺癌患者肿瘤免疫治疗后预后

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Immunotherapy targeting immune checkpoint molecules has provided remarkable clinical benefits in cancer patients but no clinically relevant biomarker for predicting treatment outcomes exists. Recently, we demonstrated that glycan structures of serum αsub1/sub-acid glycoprotein (AGP) changed dramatically in cancer patients and that α1,3fucosylated AGP (fAGP) levels increased along with disease progression and decreased responding to chemotherapy treatments. Here, the fAGP was analyzed in sera prospectively obtained from 39 patients with advanced lung cancer who underwent immunotherapy with anti-PD-1 antibody, nivolumab. Twenty-three patients had significantly high fAGP levels above the cut-off value (H-fAGP) at one month after starting the treatment and 20 patients in this group, whose tumor sizes did not decrease, maintained high fAGP levels continuously and subsequently died. However, the other 16 patients, whose fAGP levels decreased or maintained below the cut-off value (L-fAGP), survived during a 2-year observation even though 5 patients in this group had no tumor shrinkage. Accordingly, the overall survival rate was found to significantly correlate with the fAGP level. Multivariate analyses revealed that the H-fAGP was an independent risk factor for cancer progression. Therefore, the fAGP level appeared to be a reliable biomarker for predicting clinical efficacy of immunotherapy with nivolumab.
机译:靶向免疫检查点分子的免疫疗法在癌症患者提供了显着的临床益处,但没有临床相关的生物标志物用于预测治疗结果存在。最近,我们证明血清α<亚> 1 -Acid糖蛋白(AGP)的甘草结构在癌症患者中发生显着变化,并且α1,3汇曲糖基化的AGP(Fagp)水平随着疾病进展而增加,并降低了化疗治疗的响应响应。在这里,在从39名晚期肺癌患者中分析了FAGP,患有抗PD-1抗体Nivolumab的免疫疗法。在开始治疗后一个月的截止值(H-Fagp)在开始治疗后的一个月内具有显着高的Fagp水平,并且该组中的20名患者,其肿瘤尺寸没有减少,连续保持高的Fagp水平,随后死亡。然而,其他16名患者,其Fagp水平降低或维持在截止值(L-Fagp)下,即使该组5例患者没有肿瘤收缩,仍然存在于2年的观察中。因此,发现总存活率与Fagp水平显着相关。多变量分析显示H-Fagp是癌症进展的独立危险因素。因此,FAGP水平似乎是可靠的生物标志物,用于预测与Nivolumab的免疫疗法的临床疗效。

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