Miersch Shane, Maruthachalam Bharathikumar Vellalore, Geyer C Ronald, Sidhu Sachdev S
Banting and Best Department of Medical Research and Donnelly Centre for Cellular and Biomolecular Research, University of Toronto , Toronto, Ontario, Canada M5S 3E1.
Department of Biochemistry, University of Saskatchewan , Saskatoon, Saskatchewan, Canada S7N 5E5.
ACS Chem Biol. 2017 May 19;12(5):1381-1389. doi: 10.1021/acschembio.6b00990. Epub 2017 Apr 4.
We tested whether grafting an interaction domain into the hypervariable loop of a combinatorial antibody library could promote targeting to a specific epitope. Formation of the epidermal growth factor receptor (EGFR) signaling heterodimer involves extensive contacts mediated by a "dimerization loop." We grafted the dimerization loop into the third hypervariable loop of a synthetic antigen-binding fragment (Fab) library and diversified other loops using a tailored diversity strategy. This structure-directed Fab library and a naı̈ve synthetic Fab library were used to select Fabs against EGFR. Both libraries yielded high affinity Fabs that bound to overlapping epitopes on cell-surface EGFR, inhibited receptor activation, and targeted epitopes distinct from those of cetuximab and panitumumab. Epitope mapping experiments revealed complex sites of interaction, comprised of domains I and II but not exclusively localized to the receptor dimerization loop. These results validate the grafting approach for designing Fab libraries and also underscore the versatility of naı̈ve synthetic libraries.
我们测试了将一个相互作用结构域嫁接到组合抗体文库的高变环中是否能够促进对特定表位的靶向作用。表皮生长因子受体(EGFR)信号异二聚体的形成涉及由一个“二聚化环”介导的广泛接触。我们将二聚化环嫁接到一个合成抗原结合片段(Fab)文库的第三个高变环中,并使用定制的多样化策略使其他环多样化。这个结构导向的Fab文库和一个天然合成Fab文库被用于筛选抗EGFR的Fab。两个文库都产生了高亲和力的Fab,它们与细胞表面EGFR上的重叠表位结合,抑制受体激活,并靶向与西妥昔单抗和帕尼单抗不同的表位。表位定位实验揭示了复杂的相互作用位点,由结构域I和II组成,但并非仅局限于受体二聚化环。这些结果验证了用于设计Fab文库的嫁接方法,也强调了天然合成文库的通用性。
