Departments of Biochemistry and Molecular Pharmacology and ‡Department of Pathology, New York University School of Medicine , New York, New York 10016, United States.
Biochemistry. 2013 Sep 10;52(36):6249-57. doi: 10.1021/bi400645e. Epub 2013 Aug 23.
The third variable region (V3) of HIV-1 gp120 plays a key role in viral entry into host cells; thus, it is a potential target for vaccine design. Human monoclonal antibody (mAb) 447-52D is one of the most broadly and potently neutralizing anti-V3 mAbs. We further characterized the 447-52D epitope by determining a high-resolution crystal structure of the Fab fragment in complex with a cyclic V3 and interrogated the antigen-antibody interaction by a combination of site-specific mutagenesis, isothermal titration calorimetry (ITC) and neutralization assays. We found that 447-52D's neutralization capability is correlated with its binding affinity and at 25 °C the Gibbs free binding energy is composed of a large enthalpic component and a small favorable entropic component. The large enthalpic contribution is due to (i) an extensive hydrogen bond network, (ii) a π-cation sandwiching the V3 crown apex residue Arg(315), and (iii) a salt bridge between the 447-52D heavy chain residue Asp(H95) and Arg(315). Arg(315) is often harbored by clade B viruses; thus, our data explained why 447-52D preferentially neutralizes clade B viruses. Interrogation of the thermodynamic signatures of residues at the antigen binding interface gives key insights into their contributions in the antigen-antibody interaction.
HIV-1 gp120 的第三可变区 (V3) 在病毒进入宿主细胞中起着关键作用;因此,它是疫苗设计的潜在目标。人类单克隆抗体 (mAb) 447-52D 是最广泛和最有效的抗 V3 mAb 之一。我们通过确定 Fab 片段与环状 V3 复合物的高分辨率晶体结构进一步表征了 447-52D 的表位,并通过定点突变、等温滴定量热法 (ITC) 和中和测定的组合来研究抗原-抗体相互作用。我们发现 447-52D 的中和能力与其结合亲和力相关,在 25°C 下,吉布斯自由结合能由较大的焓成分和较小的有利熵成分组成。较大的焓贡献归因于 (i) 广泛的氢键网络,(ii) 夹在 V3 冠顶残基 Arg(315) 之间的π-阳离子,以及 (iii) 447-52D 重链残基 Asp(H95) 和 Arg(315) 之间的盐桥。Arg(315) 通常存在于 B 型病毒中;因此,我们的数据解释了为什么 447-52D 优先中和 B 型病毒。对抗原结合界面残基的热力学特征的研究为它们在抗原-抗体相互作用中的贡献提供了关键见解。
