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首页> 外文期刊>Journal of Translational Medicine >Clinicopathologic implication of PD-L1 and phosphorylated STAT3 expression in diffuse large B cell lymphoma
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Clinicopathologic implication of PD-L1 and phosphorylated STAT3 expression in diffuse large B cell lymphoma

机译:弥漫性大B细胞淋巴瘤中PD-L1和磷酸化STAT3表达的临床病理意义

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摘要

Antitumor immune response of programmed cell death ligand (PD-L1) has shown clinical value not only in Hodgkin lymphoma and EBV-associated lymphomas but also in EBV-negative diffuse large B cell lymphoma (DLBCL) of non-germinal center B cell-like (non-GCB) subtype. Signal transducer and activator of transcription 3 (STAT3) is known to induce PD-L1 in immune cells and its activated form, phosphorylated STAT3 (pSTAT3), is also frequently expressed in non-GCB DLBCL. Herein, we investigated associations between PD-L1 expression/gene alteration, pSTAT3 expression and clinicopathologic variables in EBV-negative DLBCL. In 107 cases of DLBCLs with non-GCB subtype (67%; 72/107), GCB subtype (25%; 27/107) and unclassifiable cases (8%; 8/107), we performed PD-L1 and pSTAT3 immunohistochemistry and fluorescence in situ hybridization for PD-L1 gene translocation and copy number gain/amplification. PD-L1 was expressed in tumor cells (PD-L1t) in 21% (23/107; 30% cutoff), immune cells (PD-L1i) in 36% (38/107; 20% cutoff), and pSTAT3 in tumor nuclei in 41% (44/107; 40% cutoff). PD-L1 gene alteration was observed in 10% (10/102) including translocation in 6% (6/102) and copy number gain/amplification in 4% (4/102). Non-GCB subtype was associated with PD-L1t and pSTAT3 (p?=?0.006 and p?=?0.042), and tended to have PD-L1 gene alteration (p?=?0.058). Tumoral PD-L1 expression without gene alteration (PD-L1t+ GA?) correlated with pSTAT3-positive tumor cell proportions (%) (p?=?0.033). In survival analysis, pSTAT3 expression independently predicted shorter PFS in total cohort (p?=?0.017) and R-CHOP-treated group (p?=?0.007), and in pSTAT3-negative R-CHOP-treated subset, PD-L1 expression in immune cells (PD-L1i) correlated with shorter PFS (p?=?0.042). Gene alteration and protein expression of PD-L1 and pSTAT3 expression were closely related in DLBCL and constituted features of non-GCB subtype. In addition to known clinical significance of pSTAT3, immune cell expression of PD-L1 (PD-L1i) had also clinical value in pSTAT3-dependent manner. These findings may provide an insight into immunotherapeutic strategy and risk stratification in DLBCL patients.
机译:程序性细胞死亡配体(PD-L1)的抗肿瘤免疫反应不仅在霍奇金淋巴瘤和EBV相关淋巴瘤中表现出临床价值,而且在非生发性中心B细胞样EBV阴性弥漫性大B细胞淋巴瘤(DLBCL)中也具有临床价值(非GCB)子类型。已知信号转导和转录激活因子3(STAT3)在免疫细胞中诱导PD-L1,其激活形式磷酸化的STAT3(pSTAT3)也经常在非GCB DLBCL中表达。在这里,我们调查了EB-阴性DLBCL中PD-L1表达/基因改变,pSTAT3表达与临床病理变量之间的关联。在107例具有非GCB亚型(67%; 72/107),GCB亚型(25%; 27/107)和无法分类的病例(8%; 8/107)的DLBCL中,我们进行了PD-L1和pSTAT3免疫组织化学分析, PD-L1基因易位和拷贝数增加/扩增的荧光原位杂交。 PD-L1在肿瘤细胞(PD-L1t)中以21%(23/107; 30%截止)表达,免疫细胞(PD-L1i)在36%(38/107; 20%截止)中表达,pSTAT3在肿瘤中表达核中41%(44/107;截断率40%)。 PD-L1基因改变的发生率为10%(10/102),包括6%的易位(6/102)和4%(4/102)的拷贝数增加/扩增。非GCB亚型与PD-L1t和pSTAT3有关(p = 0.006和p = 0.042),并且倾向于具有PD-L1基因改变(p = 0.058)。没有基因改变的肿瘤PD-L1表达(PD-L1t +GAα)与pSTAT3阳性肿瘤细胞比例(%)相关(p≤0.033)。在生存分析中,pSTAT3的表达独立预测总队列(p?=?0.017)和R-CHOP治疗组(p?=?0.007)以及pSTAT3阴性R-CHOP治疗亚组PD-L1中较短的PFS。免疫细胞(PD-L11)中的表达与较短的PFS相关(p≥0.042)。在DLBCL中,PD-L1和pSTAT3的基因改变和蛋白质表达密切相关,构成了非GCB亚型的特征。除了已知的pSTAT3的临床意义外,PD-L1(PD-L1i)的免疫细胞表达还具有pSTAT3依赖性的临床价值。这些发现可能为DLBCL患者的免疫治疗策略和风险分层提供见识。

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