Conformational changes drive protein function, including catalysis,
allostery, and signaling. X-ray diffuse scattering from protein crystals has
frequently been cited as a probe of these correlated motions, with significant
potential to advance our understanding of biological dynamics. However, recent
work challenged this prevailing view, suggesting instead that diffuse
scattering primarily originates from rigid body motions and could therefore be
applied to improve structure determination. To investigate the nature of the
disorder giving rise to diffuse scattering, and thus the potential applications
of this signal, a diverse repertoire of disorder models was assessed for its
ability to reproduce the diffuse signal reconstructed from three protein
crystals. This comparison revealed that multiple models of intramolecular
conformational dynamics, including ensemble models inferred from the Bragg
data, could not explain the signal. Models of rigid body or short-range
liquid-like motions, in which dynamics are confined to the biological unit,
showed modest agreement with the diffuse maps, but were unable to reproduce
experimental features indicative of long-range correlations. Extending a model
of liquid-like motions to include disorder across neighboring proteins in the
crystal significantly improved agreement with all three systems and highlighted
the contribution of intermolecular correlations to the observed signal. These
findings anticipate a need to account for intermolecular disorder in order to
advance the interpretation of diffuse scattering to either extract biological
motions or aid structural inference.Comment: 12 pages, 5 figures (not including Supplementary Information