(Panel A) Distributions of VHH–RTA interaction energy over ensembles of 5,000 computational models for V1C7, V5C1, and respective single-point mutants at VHH position 29, named V1C7G29R and V5C1R29G. The Gly29Arg mutation in V1C7G29R causes an average 2.5-REU shift to more favorable interaction energies, which become more similar to those of V5C1. Conversely, because of the Arg29Gly mutation, the interaction energies of V5C1R29G shift by 2.4 REU toward less favorable values, approximating more closely those of V1C7. (Panel B) Distributions of X29VHH–Glu67RTA interaction energy over the ensembles of models; X = Gly for V1C7 and V5C1R29G, X = Arg for V5C1 and V1C7G29R. The Arg29VHH–Glu67RTA interaction of V1C7G29R is as favorable as that of V5C1 (−3.1 and −3.2 REUs on average, respectively). Such an interaction is favorable enough to explain V1C7G29R’s enhancement in VHH–RTA interaction energy (−2.5 REUs on average) and, therefore, the prediction that V1C7G29R and V5C1 have similar RTA binding affinities. On the other hand, absence of the Gly29VHH–Glu67RTA interaction (μ = 0.0) can explain, for the most part, why V1C7 and V5C1R29G are predicted to bind RTA similarly weakly.