Author:
Bang Yewon,Choi Yoon-Aa,Gu Jeonghyeon,Kwon Sohee,Lee Dohoon,Lee Eun Seo,Lee Myeong Sup,Lee Sangchoon,Lee Soyul,Lee Su Jung,Lim Jungsub,Maeng Jin Young,Nam Juno,Noh Jinsung,Oh Hyunjeong,Park Sun-Young,Park Taeyong,Seo Sumin,Seok Chaok,Song Moo Young,Won Jonghun,Woo Hyeonuk,Yang Jinsol,Yoon Min Ji,Bae Woong,Kim Jaehoon,Lee Dongjin,Lee Jaemyung,Lee Youhan,Yu Hasun
Abstract
AbstractProtein loops, characterized by their versatile structures with varying sizes and shapes, can recognize a wide range of targets with high specificity and affinity. The variable loops of the antibody complementarity-determining region (CDR) are particularly crucial for immune responses and therapeutic applications due to their effective target recognition capabilities. Accurate structure prediction of these antibody loops is essential for the efficientin silicodesign of target-binding antibodies for therapeutic or industrial use. However, predicting antibody loop structures is challenging due to the lack of evolutionary information from related proteins. Thus, a successfulab initiostructure prediction method, which operates without structural templates or related sequences, is crucial for the effective design of antibody loop-mediated interactions. This study demonstrates that highly accurate antibody loop structure prediction enables the effective zero-shot design of target-binding antibody loops. The performance of loop design has been shown to depend on the accuracy ofab initioloop structure prediction, as tested with two versions of our design model. The high affinity, diversity, novelty, and specificity of the antibody loops designed with these new methods were validated experimentally on four target proteins.
Publisher
Cold Spring Harbor Laboratory