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The role of Cocrystallization-Mediated altered crystallographic properties on the tabletability of rivaroxaban and malonic acid

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dc.contributor.author Kale, D. P.
dc.contributor.author Puri, V.
dc.contributor.author Kumar, A.
dc.contributor.author Kumar, N.
dc.contributor.author Bansal, A. K.
dc.date.accessioned 2021-07-07T22:56:33Z
dc.date.available 2021-07-07T22:56:33Z
dc.date.issued 2021-07-08
dc.identifier.uri http://localhost:8080/xmlui/handle/123456789/2054
dc.description.abstract The present work aims to understand the crystallographic basis of the mechanical behavior of rivaroxaban-malonic acid cocrystal (RIV-MAL Co) in comparison to its parent constituents, i.e., rivaroxaban (RIV) and malonic acid (MAL). The mechanical behavior was evaluated at the bulk level by performing “out of die” bulk compaction and at the particle level by nanoindentation. The tabletability order for the three solids was MAL < RIV < RIV-MAL Co. MAL demonstrated “lower” tabletability because of its lower plasticity, despite it having reasonably good bonding strength (BS). The absence of a slip plane and “intermediate” BS contributed to this behavior. The “intermediate” tabletability of RIV was primarily attributed to the differential surface topologies of the slip planes. The presence of a primary slip plane (0 1 1) with flat-layered topology can favor the plastic deformation of RIV, whereas the corrugated topology of secondary slip planes (1 0 2) could adversely affect the plasticity. In addition, the higher elastic recovery of RIV crystal also contributed to its tabletability. The significantly “higher” tabletability of RIV-MAL Co among the three molecular solids was the result of its higher plasticity and BS. Flat-layered topology slip across the (0 0 1) plane, the higher degree of intermolecular interactions, and the larger separation between adjacent crystallographic layers contributed to improved mechanical behavior of RIV-MAL Co. Interestingly, a particle level deformation parameter H/E (i.e., ratio of mechanical hardness H to elastic modulus E) was found to inversely correlate with a bulk level deformation parameter σ0 (i.e., tensile strength at zero porosity). The present study highlighted the role of cocrystal crystallographic properties in improving the tabletability of materials. en_US
dc.language.iso en_US en_US
dc.subject cocrystal en_US
dc.subject compaction en_US
dc.subject nanoindentation en_US
dc.subject slip plane en_US
dc.subject tabletability en_US
dc.subject surface topology en_US
dc.subject interparticulate bonding area en_US
dc.subject interparticulate bonding strength en_US
dc.title The role of Cocrystallization-Mediated altered crystallographic properties on the tabletability of rivaroxaban and malonic acid en_US
dc.type Article en_US


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