单克隆抗体
抗体
计算生物学
黄曲霉毒素
配体(生物化学)
化学
生物
分子生物学
组合化学
生物化学
免疫学
受体
食品科学
作者
Changrui Xing,Guanglei Li,Xin Zheng,Peng Li,Jian Yuan,Wenjing Yan
标识
DOI:10.1021/acs.jcim.4c00736
摘要
-GA) demonstrated a very weak binding affinity for Ab-4B5G6. The heavy chain was successfully isolated, and its sensitivity and specificity were consistent with those of the intact antibody. The homology models of variable heavy (VH) single-domain antibodies were established by RosettaAntibody, and the docking analysis revealed the same residues, including Ala, His, and Trp. Compared to the potential binding mode of fragment variable (FV) region, the results from a model of VH indicated that there are seven models involved in hydrophobic interaction with TYR32, which is usually referred to as polar amino acid and has both hydrophobic and hydrophilic features depending on the circumstances. Our work encompasses the entire process of Rosetta antibody-ligand computational simulation, highlighting the significance of variable heavy domain structural design in enhancing molecular interactions.
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