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Prognostic significance of L1CAM expression and its association with mutant p53 expression in high-risk endometrial cancer

机译:L1细胞粘附分子(L1Cam)表达的预后意义及其与突变型p53表达在高危子宫内膜癌中的关系。

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摘要

Studies in early-stage, predominantly low- and intermediate-risk endometrial cancer have demonstrated that L1 cell adhesion molecule (L1CAM) overexpression identifies patients at increased risk of recurrence, yet its prognostic significance in high-risk endometrial cancer is unclear. To evaluate this, its frequency, and the relationship of L1CAM with the established endometrial cancer biomarker p53, we analyzed the expression of both markers by immunohistochemistry in a pilot series of 116 endometrial cancers (86 endometrioid, 30 non-endometrioid subtype) with high-risk features (such as high tumor grade and deep myometrial invasion) and correlated results with clinical outcome. We used The Cancer Genome Atlas (TCGA) endometrial cancer series to validate our findings. Using the previously reported cutoff of 10% positive staining, 51/116 (44%) tumors were classified as L1CAM-positive, with no significant association between L1CAM positivity and the rate of distant metastasis (P=0.195). However, increasing the threshold for L1CAM positivity to 50% resulted in a reduction of the frequency of L1CAM-positive tumors to 24% (28/116), and a significant association with the rate of distant metastasis (P=0.018). L1CAM expression was strongly associated with mutant p53 in the high-risk and TCGA series (P10% does not predict prognosis in high-risk endometrial cancer, whereas an alternative threshold (50%) does. L1CAM expression is strongly, but not universally, associated with mutant p53, and may be strong enough for clinical implementation as prognostic marker in combination with p53. The high frequency of L1CAM expression in high-risk endometrial cancers suggests that it may also be a promising therapeutic target in this tumor subset.
机译:已经在早期阶段,主要是低和中度风险子宫内膜癌的研究表明,L1细胞粘附分子(L1CAM)过表达识别患者复发的风险增加,但在高风险的子宫内膜癌及其预后意义尚不清楚。为了评价这一点,它的频率,和L1CAM的与所建立的子宫内膜癌的生物标志物的p53的关系,我们分析了在具有高的导频系列的116个子宫内膜癌(86子宫内膜型,30个非子宫内膜样亚型)两种标记的通过免疫组织化学表达风险特征(如高肿瘤等级和深肌层浸润)和与临床结果相关的结果。我们使用的癌症基因组图谱(TCGA)子宫内膜癌系列来验证我们的研究结果。使用10%的阳性染色的先前报告的截止,51/116(44%)的肿瘤被归类为L1CAM阳性,与L1CAM阳性和远处转移(P = 0.195)的速率之间没有显著关联。然而,增加用于L1CAM积极性的阈值,以50%导致减少L1CAM阳性肿瘤的24%(​​116分之28)的频率,并与远处转移(P = 0.018)的速率的显著关联。 L1CAM表达与在高风险和TCGA系列(P10%不能预测在高风险的子宫内膜癌的预后突变型p53相关,而一种替代阈值(> 50%)一样。L1CAM表达是强烈的,但并不普遍,与突变型p53相关联,并且可以是用于临床实施中与p53结合的预后标志物足够强的。L1CAM表达的高风险子宫内膜癌的高频表明,它也可以是在该子集中的肿瘤有希望的治疗靶标。

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