Crystallizing the Un-crystallizable: Insights from Extensive Screening of PROTACs [dataset]

PROTACs are new drug molecules in the beyond Rule of Five (bRo5) chemical space with extremely poor aqueous solubility and poor crystallizability. This makes PROTACs particularly challenging to understand from a solid-state pre-formulation perspective. While several X-ray structures have been reported of PROTACs in ternary complexes, to date no structures have been published of single component densely packed PROTACs, from which an understanding of PROTACs’ intermolecular interactions, and therefore physical properties, can be developed. An extensive crystallisation protocol was applied to grow single crystals of a cereblon-recruiting PROTAC ‘AZ1’ resulting in structures of an anhydrous form and a non-stoichiometric p-xylene solvate using 3D electron diffraction and synchrotron X-ray crystallography, respectively. The lattice energies are dominated by dispersive interactions between AZ1 molecules despite the presence of multiple hydrogen-bond donors and acceptors and planar aromatic groups, and both structures are built on similar intermolecular interactions. Thermal and spectral characterization revealed another solvate form containing dichloromethane. Amorphous solids produced by mechanochemical grinding of anhydrous AZ1 crystals also differed in dissolution characteristics from an amorphous solid produced by desolvating the dichloromethane solvate crystals, indicating that AZ1 may demonstrate polyamorphism. This study paves the way for solid form screening and understanding in pharmaceutical systems that are far bRo5.