Interactions of epitopic variants of epidermal growth factor receptor with therapeutic anti- EGFR antibodies

SU Mahdiyah, T. Ahsan, K. Fatema, SS Shoily, AA Sajib
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Abstract

Epidermal growth factor receptor (EGFR) plays important roles in cancerous transformation of epithelial cells in many solid cancers. Due to the pivotal role of EGFR in cellular proliferation and metastasis, it is a promising molecular target for the treatment of various cancers. One of the major treatment approaches uses anti-EGFR monoclonal antibodies (mAbs) targeted to the extracellular domain of the receptor to competitively block the binding of its ligands. Cetuximab, necitumumab, nimotuzumab, and panitumumab are such approved mAbs which are commercially available and used to treat multiple types of cancers. The response rates to these expensive therapeutics in various cancers range from nearly 9% to 91%. Hence, the objective of this study was to indentify whether any of the missense single nucleotide polymorphisms (SNPs) in the EGFR gene impart any structural and functional impact on the receptor’s interaction with these antibodies. We used X-ray crystallographic structures (from Protein Data Bank) of the Fab fragments of these therapeutic antibodies in complex with EGFR to analyze the effects of the missense mutations on the antigen-antibody interactions. We also assessed the potential association of the destabilizing variants with pathogenicity and disease susceptibility. EGFR H433Q (rs1171743336), S464T (rs746763556), S492G (rs1057519760) and S492R (rs1057519860) variants appear to weaken interactions between EGFR and cetuximab, which is the most widely used anti-EGFR therapeutic antibody. Other epitopic variants do not appear to affect interactions between EGFR and relevant mAbs (necitumumab, nimotuzumab, and panitumumab). Prior to treatment of the EGFR mediated conditions with cetuximab, screening of variants that destabilize antibody-EGFR interaction may be considered as a companion diagnostic test for avoiding unresponsiveness and improving therapeutic outcomes. Dhaka Univ. J. Biol. Sci. 30(3 CSI): 393-403, 2022 (June)
表皮生长因子受体表位变异与治疗性抗EGFR抗体的相互作用
表皮生长因子受体(Epidermal growth factor receptor, EGFR)在多种实体癌上皮细胞的癌变过程中起重要作用。由于EGFR在细胞增殖和转移中的关键作用,它是治疗各种癌症的有希望的分子靶点。主要的治疗方法之一是使用靶向受体细胞外结构域的抗egfr单克隆抗体(mab)来竞争性地阻断其配体的结合。西妥昔单抗、尼妥珠单抗、尼妥珠单抗和帕尼珠单抗是经批准的单抗,可用于治疗多种类型的癌症。这些昂贵的治疗方法对各种癌症的反应率从近9%到91%不等。因此,本研究的目的是确定EGFR基因中的任何错义单核苷酸多态性(snp)是否对受体与这些抗体的相互作用产生任何结构和功能影响。我们使用这些治疗性抗体的Fab片段与EGFR复合物的x射线晶体结构(来自蛋白质数据库)来分析错义突变对抗原-抗体相互作用的影响。我们还评估了不稳定变异与致病性和疾病易感性的潜在关联。EGFR H433Q (rs1171743336)、S464T (rs746763556)、S492G (rs1057519760)和S492R (rs1057519860)变异体似乎减弱了EGFR与西妥昔单抗之间的相互作用,西妥昔单抗是最广泛使用的抗EGFR治疗性抗体。其他表位变异似乎不影响EGFR和相关单克隆抗体(necitumumab, nimotuzumab和panitumumab)之间的相互作用。在用西妥昔单抗治疗EGFR介导的疾病之前,筛选破坏抗体-EGFR相互作用的变异可能被认为是避免无反应和改善治疗结果的伴随诊断试验。达卡大学。科学30(3 CSI): 393- 403,2022(6月)
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