Abstract
Fab consist of a heavy and light chain and can be subdivided into a variable (VH and VL) and a constant region (CH1 and CL). The variable region contains the complementarity-determining region (CDR), which is formed by six hypervariable loops, shaping the antigen binding site, the paratope. Apart from the CDR loops, both the elbow angle and the relative interdomain orientations of the VH–VL and the CH1–CL domains influence the shape of the paratope. Thus, characterization of the interface and elbow angle dynamics is essential to antigen specificity. We studied nine antigen-binding fragments (Fab) to investigate the influence of affinity maturation, antibody humanization, and different light-chain types on the interface and elbow angle dynamics. While the CDR loops reveal conformational transitions in the micro-to-millisecond timescale, both the interface and elbow angle dynamics occur on the low nanosecond timescale. Upon affinity maturation, we observe a substantial rigidification of the VH and VL interdomain and elbow-angle flexibility, reflected in a narrower and more distinct distribution. Antibody humanization describes the process of grafting non-human CDR loops onto a representative human framework. As the antibody framework changes upon humanization, we investigated if both the interface and the elbow angle distributions are changed or shifted. The results clearly showed a substantial shift in the relative VH–VL distributions upon antibody humanization, indicating that different frameworks favor distinct interface orientations. Additionally, the interface and elbow angle dynamics of five antibody fragments with different light-chain types are included, because of their strong differences in elbow angles. For these five examples, we clearly see a high variability and flexibility in both interface and elbow angle dynamics, highlighting the fact that Fab interface orientations and elbow angles interconvert between each other in the low nanosecond timescale. Understanding how the relative interdomain orientations and the elbow angle influence antigen specificity, affinity, and stability has broad implications in the field of antibody modeling and engineering.
Highlights
Antibodies are key players as therapeutic agents because of their ability to bind the majority of targets and their suitability for protein engineering (Chiu et al, 2019; Kaplon and Reichert, 2019; Kaplon et al, 2020)
We investigate the dynamics of both relative VH–VL, CH1–CL interface angles and the elbow angle and their respective dependencies on different light-chain types and shifts upon antibody humanization and affinity maturation
While the other six discussed Fabs contribute to a better understanding of the interface and elbow angle flexibilities upon antibody humanization and affinity maturation (Cauerhff et al, 2004; Fransson et al, 2010)
Summary
Antibodies are key players as therapeutic agents because of their ability to bind the majority of targets and their suitability for protein engineering (Chiu et al, 2019; Kaplon and Reichert, 2019; Kaplon et al, 2020). Apart from the diversity in length, sequence, and structure of the CDR loops, the relative VH–VL interdomain orientation plays an important role in determining the shape of the antigenbinding site (Colman, 1988; Foote and Winter, 1992; Dunbar et al, 2013; Bujotzek et al, 2016). ABangle is a computational tool to characterize the relative orientations between the antibody variable domains (VH and VL) by using five angles and a distance and by comparing it to other known structures (Dunbar et al, 2013; Bujotzek et al, 2015, 2016)
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