Potential prognostic value of PD-L1 and FOXP3 as predictors of relapse in breast cancer

R. Nagib, Sherine Refat, A. Eladl, Z. Emarah, K. Elnaghi
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Abstract

Background: Expression of PD-L1 detected by immunohistochemistry can represent a new hope for cancer management. The role of PD L1 in breast cancer is still unclear. Similarly, is the role of tumor-infiltrating FOXP3 +ve regulatory T (Treg) cells where literature data are conflicting. Our study aimed to evaluate the immunohistochemical expression of PD L1 and FOXP3 in breast cancer, correlate them with clinicopathological parameters as well as evaluating their relation.Methods: This is a retrospective study carried out on 136 breast cancer specimens. Only cases with proved pathological diagnosis of infiltrating duct carcinoma of no special type (NST) were included. Tissue microarray blocks were constructed and immunostained with the polyclonal antibody for PDL1 and monoclonal antibody for FOXP3.Results: Statistically significant correlation was found between high FOXP3 and nearly all adverse prognostic factors including; grade III tumors (p = .003), basal-like subtype(p = .001), high Ki67(p = .001), negative ER status(p = .001), negative PR(p = .028), HER2 expression(p = .04), advanced stage (p = .001), and LN metastases(p = .001). For PDL1, only statistically significant correlation with high Ki67 (p = .018) and advanced stage(p = .03) was found. A statistically significant positive correlation was found between PD L1 and FOXP3(p= .001). No statistically significant correlation was found between both PDL1 and FOXP3 in relation to disease-free survival (DFS) (p = .054). PDL1, age (≥ 50 years), nodal metastases were significant predictors of relapse in breast cancer.Conclusion: The current study supports PDL1 as a predictor of relapse in breast cancer. Additionally, it highlights the synergistic role between PDL1 and FOXP3 in breast cancer microenvironment. Each can be considered as a poor prognostic marker in breast cancer. This raises a concern about the benefit of breast cancer patients from blocking of PDL1 pathway.
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PD-L1和FOXP3作为乳腺癌复发预测因子的潜在预后价值
背景:免疫组织化学检测PD-L1的表达是癌症治疗的新希望。PD L1在乳腺癌中的作用尚不清楚。同样,肿瘤浸润性FOXP3 +ve调节性T (Treg)细胞的作用也是文献数据相互矛盾的。我们的研究旨在评估PD L1和FOXP3在乳腺癌中的免疫组织化学表达,以及它们与临床病理参数的相关性,并评估它们之间的关系。方法:对136例乳腺癌标本进行回顾性研究。仅纳入病理诊断为浸润性导管癌无特殊类型(NST)的病例。构建组织微阵列块并用PDL1多克隆抗体和FOXP3单克隆抗体进行免疫染色。结果:高FOXP3与几乎所有不良预后因素均有统计学意义相关,包括;III级肿瘤(p = 0.003)、基底样亚型(p = 0.001)、高Ki67(p = 0.001)、ER阴性(p = 0.001)、PR阴性(p = 0.028)、HER2表达(p = 0.04)、晚期(p = 0.001)和LN转移(p = 0.001)。对于PDL1,仅与高Ki67 (p = 0.018)和晚期(p = 0.03)有统计学意义的相关性。PD L1与FOXP3呈显著正相关(p= 0.001)。PDL1和FOXP3与无病生存(DFS)的相关性无统计学意义(p = 0.054)。PDL1、年龄(≥50岁)、淋巴结转移是乳腺癌复发的重要预测因素。结论:目前的研究支持PDL1作为乳腺癌复发的预测因子。此外,它强调了PDL1和FOXP3在乳腺癌微环境中的协同作用。每一个都可以被认为是乳腺癌预后不良的标志。这引起了人们对乳腺癌患者从阻断PDL1途径中获益的关注。
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