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Reduced Cytokine Release in Ex Vivo Response to Cilengitide and Cetuximab Is a Marker for Improved Survival of Head and Neck Cancer Patients

机译:对西仑吉肽和西妥昔单抗的体内反应中细胞因子释放的减少是改善头颈癌患者生存的标志

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摘要

Targeting of αVβ3 and αVβ5 integrins by cilengitide may reduce growth of solid tumors including head and neck squamous cell carcinoma (HNSCC). Preclinical investigations suggest increased activity of cilengitide in combination with other treatment modalities. The only published trial in HNSCC (ADVANTAGE) investigated cisplatin, 5-fluorouracil, and cetuximab (PFE) without or with once (PFE+CIL1W) or twice weekly cilengitide (PFE+CIL2W) in recurrent/metastatic HNSCC. ADVANTAGE showed good tolerability of the cilengitide arms and even lower adverse events (AEs) compared to PFE but not the benefit in overall survival expected based on preclinical data. As we found in the FLAVINO assay, a short-time ex vivo assay for prediction of chemosensitivity, only a subgroup of HNSCC had an increased suppressive effect of cilengitide containing combination therapies on colony formation of epithelial cells (CFec) and release of pro-angiogenetic and pro-inflammatory cytokines, whereas other HNSCC failed to respond. Response to αVβ3 and αVβ5 integrin targeting by cilengitide classifies HNSCC regarding outcome. We present FLAVINO data arguing for further development of cilengitide plus cetuximab in treatment of a subgroup of HNSCC potentially identified by the FLAVINO assay using a set of biomarkers for response evaluation.
机译:西仑吉肽靶向αVβ3和αVβ5整合素可能会减少包括头颈部鳞状细胞癌(HNSCC)在内的实体瘤的生长。临床前研究表明,西仑吉肽与其他治疗方式联合使用可增加活性。 HNSCC(ADVANTAGE)中唯一发表的试验研究了在复发/转移性HNSCC中不加或联合使用一次(PFE + CIL1W)或每周两次西仑吉肽(PFE + CIL2W)的顺铂,5-氟尿嘧啶和西妥昔单抗(PFE)。与PFE相比,ADVANTAGE显示西仑吉肽具有良好的耐受性,甚至不良事件(AE)更低,但根据临床前数据预期的总生存期则没有益处。正如我们在FLAVINO测定法(一种用于预测化学敏感性的短期离体测定法)中所发现的那样,只有HNSCC的一个亚组具有含cilengitide的联合疗法对上皮细胞集落形成(CFec)和促血管生成的释放的抑制作用增强和促炎细胞因子,而其他HNSCC没有反应。西仑吉肽对靶向αVβ3和αVβ5整联蛋白的反应将HNSCC分类为预后。我们目前提出争论的FLAVINO数据,以进一步治疗西仑西肽加西妥昔单抗治疗可能通过FLAVINO测定法使用一组生物标记物进行反应评估的HNSCC亚组的治疗。

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