Bier H, Hoffmann T, Haas I, van Lierop A
Department of Otorhinolaryngology/Head and Neck Surgery, Heinrich-Heine-University, Düsseldorf, Germany.
Cancer Immunol Immunother. 1998 May;46(3):167-73. doi: 10.1007/s002620050475.
Squamous cell carcinomas of the head and neck (SCCHN) frequently display high levels of the epidermal growth factor receptor (EGFR). Since EGFR is expressed on the cell surface it may form a suitable target for anticancer therapy with anti-receptor monoclonal antibodies (mAb). Besides the interference with receptor/ligand interactions, binding of mAb to EGFR leads to immunoglobulin-coated tumour cells that may induce or enhance non-specific immune effector mechanisms like antibody-dependent cell-mediated cytotoxicity (ADCC). In established cell lines of SCCHN (UM-SCC 11B, 14C, 22B, and 8029 NA) we investigated the antitumour activity of allogeneic peripheral blood mononuclear cells (PBMC) in combination with rat (ICR 62), mouse (EMD 55900), and humanized (EMD 72000) anti-EGFR mAb. In addition, autologous PBMC were available for tumour line UD-SCC 4. The EGFR protein content of the tumour cell lines ranged between 170 fmol/mg protein and 8100 fmol/mg protein, and MCF-7 cells served as receptor-negative controls. PBMC activity against SCCHN targets was determined in 96-well microtitre-plate monolayer cultures by the colorimetric 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay after coincubation for 4 h, 24 h and 72 h at effector target ratios of 1:1, 5:1, 10:1 and 20:1. PBMC subpopulations were obtained by macrophage depletion (plastic adherence) or natural killer (NK) cell enrichment (magnetic bead negative selection). Prolonged time of exposure and increased effector:target ratios revealed marked antitumour activity of PBMC alone. This non-specific immune destruction was enhanced considerably by humanized and rat, but not mouse anti-EGFR mAb. Increased EGFR protein in tumour cells partly correlated with an intensification of ADCC but was accompanied by decreased primary PBMC cytotoxicity. The utilization of PBMC subpopulations suggested a mainly NK-cell-mediated ADCC, which appeared to benefit directly or indirectly, e.g. via the secretion of cytokines, from other PBMC components. In conclusion, humanized (EMD 72000) and rat (ICR 62) anti-EGFR mAb were able to generate strong antitumour ADCC in target monolayers of SCCHN.
头颈部鳞状细胞癌(SCCHN)常常呈现高水平的表皮生长因子受体(EGFR)。由于EGFR在细胞表面表达,它可能成为用抗受体单克隆抗体(mAb)进行抗癌治疗的合适靶点。除了干扰受体/配体相互作用外,mAb与EGFR的结合会导致免疫球蛋白包被的肿瘤细胞,这可能诱导或增强非特异性免疫效应机制,如抗体依赖性细胞介导的细胞毒性(ADCC)。在已建立的SCCHN细胞系(UM-SCC 11B、14C、22B和8029 NA)中,我们研究了同种异体外周血单个核细胞(PBMC)与大鼠(ICR 62)、小鼠(EMD 55900)和人源化(EMD 72000)抗EGFR mAb联合使用时的抗肿瘤活性。此外,自体PBMC可用于肿瘤系UD-SCC 4。肿瘤细胞系中EGFR蛋白含量在170 fmol/mg蛋白至8100 fmol/mg蛋白之间,MCF-7细胞用作受体阴性对照。在96孔微量滴定板单层培养物中,通过比色法3-(4,5-二甲基噻唑-2-基)-2,5-二苯基四氮唑溴盐测定法,在效应细胞与靶细胞比例为1:1、5:1、10:1和20:1的情况下共同孵育4小时、24小时和72小时后,测定PBMC对SCCHN靶标的活性。通过巨噬细胞清除(塑料贴壁)或自然杀伤(NK)细胞富集(磁珠阴性选择)获得PBMC亚群。延长暴露时间和增加效应细胞:靶细胞比例显示PBMC单独具有显著的抗肿瘤活性。人源化和大鼠抗EGFR mAb可显著增强这种非特异性免疫破坏,但小鼠抗EGFR mAb则不能。肿瘤细胞中EGFR蛋白增加部分与ADCC增强相关,但同时原发性PBMC细胞毒性降低。PBMC亚群的利用表明主要是NK细胞介导的ADCC,它似乎直接或间接(例如通过细胞因子分泌)受益于其他PBMC成分。总之,人源化(EMD 72000)和大鼠(ICR 62)抗EGFR mAb能够在SCCHN的靶标单层中产生强大的抗肿瘤ADCC。
