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首页> 外文期刊>Molecular cancer therapeutics >Serum PD-1 Is Elevated after Pembrolizumab Treatment but Has No Predictive Value
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Serum PD-1 Is Elevated after Pembrolizumab Treatment but Has No Predictive Value

机译:血清PD-1在Pembrozumab治疗后升高,但没有预测值

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摘要

Immune-checkpoint blockade (ICB) uses antibody targeting of specific inhibitory receptors and ligands. The major limitations of ICB, such as high cost, limited success rate, and immune-related adverse events (irAE), highlight the need for predictive biomarkers. We analyzed pre-immunotherapy and post-immunotherapy serum samples of 24 patients treated with pembrolizumab for changes in PD-1 and over 1,000 additional protein markers using a multiplex proximity extension assay (PEA) to identify potential predictive biomarkers of response and/or toxicity. Candidates were selected based on the criteria that at least 2 patients within any of 3 patient groups (responders without irAEs, responders with irAEs, or nonresponders with irAEs) had either a >= 4-fold increase or 4-fold decrease in expression post-immunotherapy. Female and male control samples were used as technical duplicates. A patient group with no response and no irAEs was used to exclude candidates. Following treatment with pembrolizwnab, there was a relative increase of PD-1 in the serum of all patients, compared with controls (average 4.4-fold). We identified 7 additional serum proteins that met our candidate selection criteria. These candidate markers did not have any significant association with response or toxicity to pembrolizumab. Overall, we show that serum PD-1 increases post-therapy with pembrolizumab treatment but has no predictive value for response or toxicity in this small set of patients.
机译:免疫检查点封闭(ICB)使用特异性抑制剂和配体的抗体靶向。 ICB的主要局限性,如高成本,有限的成功率和免疫相关的不良事件(IRAE),突出了对预测生物标志物的需求。我们分析了使用多重接近延伸测定(PEA)的PEMBROLIZUAB处理的24例患有PEMBROLIZUMAB的24例患者的预免疫疗法和免疫疗法血清样本,以鉴定响应和/或毒性的潜在预测生物标志物。基于标准选择候选者,即3例患者组中任一项的至少2名患者(没有伊拉斯的响应者,厄拉斯的反应者或与伊拉克的非反应者)具有> = 4倍的增加或表达后的4倍降低 - 免疫疗法。女性和男性对照样品用作技术重复。没有反应,没有伊拉斯的患者组被用来排除候选人。在用PembrolizWnab进行治疗后,所有患者的血清中的PD-1相对升高,与对照(平均为4.4倍)。我们确定了7种符合我们候选人选择标准的额外血清蛋白质。这些候选标记与Pembrolizumab的反应或毒性没有任何重要的关联。总体而言,我们表明,血清PD-1与Pembrolizumab治疗的治疗后疗法增加,但在这一小组患者中没有对响应或毒性的预测值。

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