首页> 美国卫生研究院文献>Cancers >Relapse-Free Survival and PD-L1 Expression in First High- and Low-Grade Relapsed Luminal Basal and Double-Negative P53-Mutant Non-Muscular Invasive Bladder Cancer Depending on Previous Chemo- and Immunotherapy
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Relapse-Free Survival and PD-L1 Expression in First High- and Low-Grade Relapsed Luminal Basal and Double-Negative P53-Mutant Non-Muscular Invasive Bladder Cancer Depending on Previous Chemo- and Immunotherapy

机译:根据先前的化学和免疫疗法在首例高低度复发性管腔基底和双重阴性的P53突变型非肌肉浸润性膀胱癌中无复发生存率和PD-L1表达

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摘要

The goal of this study was to assess how PD-L1 expression in tissue specimens of patients with main molecular subtypes of NMIBC (luminal, basal and double-negative p53-mutant) associates with relapsed-free survival in dependence on the tumor grade and prior treatment of primary bladder cancer. PD-L1 expressions on the membrane of neoplastic and CD8+ immune cells were assessed in tumor specimens ( = 240) of primary and relapsed luminal, basal and double-negative p53-mutant NMIBC. Association between relapse-free survival and PD-L1 expression was estimated for high- and low-grade relapsed NMIBC according to previous treatment and their molecular profile, using the Kaplan–Meier method, and assessed by using the log-rank test. Potential confounders were adjusted by Cox regression models. In a group of patients who underwent only TUR without intravesical therapy, there were significant differences in relapse time between high- and low-grade tumors in basal and luminal molecular subtypes; for basal relapsed carcinoma, RFS was shorter in cases where tumors were less malignant. Both intravesical mitomycin and Bacillus Calmette–Guerin (BCG) therapy significantly extended the time of recurrence of low-grade luminal and basal bladder malignancies with no intergroup differences in double-negative NMIBC. PD-L1 expression status was associated with RFS for luminal relapsed NMIBCs in the group without previous frontline intervention, and with RFS in the group of patients with luminal relapsed bladder cancer previously utilized BCG. Obtained results may be considered as a promising approach for further clinical implementation.
机译:这项研究的目的是评估具有NMIBC主要分子亚型(管腔,基底和双阴性p53突变体)的患者组织样本中PD-L1的表达如何与无复发生存相关联,这取决于肿瘤的级别和先前的情况。原发性膀胱癌的治疗。在原发性和复发性管腔,基底和双阴性p53突变NMIBC的肿瘤样本(= 240)中评估了肿瘤和CD8 +免疫细胞膜上的PD-L1表达。使用Kaplan–Meier方法,根据先前的治疗方法和其分子特征,通过高阶和低阶复发NMIBC评估了无复发生存期与PD-L1表达之间的关联,并使用对数秩检验进行了评估。潜在的混杂因素通过Cox回归模型进行了调整。在仅接受TUR且未进行膀胱内治疗的一组患者中,基础和管腔分子亚型的高,低度肿瘤之间的复发时间存在显着差异。对于基底复发性癌,在恶性程度较低的情况下,RFS较短。膀胱丝裂霉素和卡介苗芽孢杆菌(BCG)治疗均显着延长了低度管腔和基底膀胱恶性肿瘤的复发时间,双阴性NMIBC组间无差异。 PD-L1的表达状态与先前未进行过一线干预的组中管腔复发的NMIBC的RFS相关,而与先前使用BCG的管腔复发的膀胱癌患者组的RFS相关。获得的结果可以被认为是进一步临床实施的有希望的方法。

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