In silico screening of dicarboxylic acids for cocrystallization with phenylpiperazine derivatives based on both cocrystallization propensity and solubility advantage

Cysewski, Piotr

doi:10.1007/s00894-017-3287-y

Cited by 21 publications

(19 citation statements)

References 65 publications

(65 reference statements)

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“…As it was reported in our previous works Cysewski, 2017;Przybyłek et al, 2017), in silico methods can be quite successful in cocrystal screening and predicting cocrystal solubility advantage. Particularly, it was shown Przybyłek et al, 2017) that compounds containing polar OH and COOH groups are excellent methylxanthines solubility enhancers.…”

Section: Introductionmentioning

confidence: 53%

“…Recently there has been a growing interest in in-silico pharmaceutical excipients screening methods including bioavailability and solubility improvement agents such as soluble polymers, surfactants and nutraceutical cocrystals formers (Bergström et al, 2016;Christensen et al, 2017;Cysewski, 2017;Przybyłek et al, 2017). The major advantage of efficient theoretical approaches, important from the economic viewpoint, is reducing the time and reagents costs.…”

Section: Discussionmentioning

confidence: 99%

“…This indispensable additional criterion is a well-accepted measure of cocrystallization propensity. This kind of quantification of coformers affinity was successfully used for experimentally verified cocrystals screening (Cysewski, 2017(Cysewski, , 2016aCysewski et al, 2016;Klamt, 2012Klamt, , 2011Klamt et al, 2002;Klamt and Schüürmann, 1993;Loschen and Klamt, 2015; Przybyłek et al., 2016b). In order to demonstrate the usefulness of the screening procedure proposed here, the search for DSR enhancers was extended over a quite comprehensive set of coformers defined in the methodology part.…”

Section: Exemplary Applicationsmentioning

confidence: 99%

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Selection of effective cocrystals former for dissolution rate improvement of active pharmaceutical ingredients based on lipoaffinity index

Cysewski

Przybyłek

2017

European Journal of Pharmaceutical Sciences

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New theoretical screening procedure was proposed for appropriate selection of potential cocrystal formers possessing the ability of enhancing dissolution rates of drugs. The procedure relies on the training set comprising 102 positive and 17 negative cases of cocrystals found in the literature. Despite the fact that the only available data were of qualitative character, performed statistical analysis using binary classification allowed to formulate quantitative criterions. Among considered 3679 molecular descriptors the relative value of lipoaffinity index, expressed as the difference between values calculated for active compound and excipient, has been found as the most appropriate measure suited for discrimination of positive and negative cases. Assuming 5% precision, the applied classification criterion led to inclusion of 70% positive cases in the final prediction. Since lipoaffinity index is a molecular descriptor computed using only 2D information about a chemical structure, its estimation is straightforward and computationally inexpensive. The inclusion of an additional criterion quantifying the cocrystallization probability leads to the following conjunction criterions H<-0.18 and ΔLA>3.61, allowing for identification of dissolution rate enhancers. The screening procedure was applied for finding the most promising coformers of such drugs as Iloperidone, Ritonavir, Carbamazepine and Enthenzamide.

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Section: Introductionmentioning

confidence: 53%

Section: Discussionmentioning

confidence: 99%

Section: Exemplary Applicationsmentioning

confidence: 99%

See 1 more Smart Citation

Selection of effective cocrystals former for dissolution rate improvement of active pharmaceutical ingredients based on lipoaffinity index

Cysewski

Przybyłek

2017

European Journal of Pharmaceutical Sciences

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“…These include calculation of interaction energies [ 116 , 117 ], electrostatic potentials [ 118 ], molecular complementarity between API and coformers [ 119 , 120 ], solubility behavior [ 121 , 122 , 123 ], crystal energy landscapes of API-coformer pairs [ 124 ] and hydrogen bond propensities [ 125 ]. Table 6 presents the summary of various computational coformer screening methods [ 112 , 113 , 114 , 115 , 116 , 117 , 118 , 119 , 120 , 121 , 122 , 123 , 124 , 125 , 126 , 127 , 128 , 129 , 130 , 131 , 132 ] reported so far in the literature. Despite being less labor intensive, computational screening methods suffer from the requirement of large simulation times to perform molecular dynamic simulations.…”

Section: Screening Methods For Cocrystalsmentioning

confidence: 99%

Engineering Cocrystals of Poorly Water-Soluble Drugs to Enhance Dissolution in Aqueous Medium

2018

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Biopharmaceutics Classification System (BCS) Class II and IV drugs suffer from poor aqueous solubility and hence low bioavailability. Most of these drugs are hydrophobic and cannot be developed into a pharmaceutical formulation due to their poor aqueous solubility. One of the ways to enhance the aqueous solubility of poorlywater-soluble drugs is to use the principles of crystal engineering to formulate cocrystals of these molecules with water-soluble molecules (which are generally called coformers). Many researchers have shown that the cocrystals significantly enhance the aqueous solubility of poorly water-soluble drugs. In this review, we present a consolidated account of reports available in the literature related to the cocrystallization of poorly water-soluble drugs. The current practice to formulate new drug cocrystals with enhanced solubility involves a lot of empiricism. Therefore, in this work, attempts have been made to understand a general framework involved in successful (and unsuccessful) cocrystallization events which can yield different solid forms such as cocrystals, cocrystal polymorphs, cocrystal hydrates/solvates, salts, coamorphous solids, eutectics and solid solutions. The rationale behind screening suitable coformers for cocrystallization has been explained based on the rules of five i.e., hydrogen bonding, halogen bonding (and in general non-covalent bonding), length of carbon chain, molecular recognition points and coformer aqueous solubility. Different techniques to screen coformers for effective cocrystallization and methods to synthesize cocrystals have been discussed. Recent advances in technologies for continuous and solvent-free production of cocrystals have also been discussed. Furthermore, mechanisms involved in solubilization of these solid forms and the parameters influencing dissolution and stability of specific solid forms have been discussed. Overall, this review provides a consolidated account of the rationale for design of cocrystals, past efforts, recent developments and future perspectives for cocrystallization research which will be extremely useful for researchers working in pharmaceutical formulation development.

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“…This phenomenon can be used to design the new solid forms of an active pharmaceutical ingredient in order to improve physicochemical properties (Bartsch & Griesser, 2004). Therefore, data relating to interactions between solid compounds are essential in the formation of multicomponent solid forms of active pharmaceutical ingredient (Cysewski, 2017;Yamashita, Hirakura, Yuda, & Terada, 2014).…”

Section: Introductionmentioning

confidence: 99%

Analysis of Solid-State Interactions of Ketoprofen-Coformer Binary Mixtures by DSC and Hot Stage Microscopy

Wicaksono

Setyawan

Siswandono

2020

Molekul

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Ketoprofen is a non-steroidal anti-inflammatory drug with poor water solubility, so the absorption is less than optimal. One method to improve the solubility of ketoprofen is through the formation of multicomponent solid forms. The success of the formation of the multicomponent solid forms is strongly influenced by interactions between components in their solids. In this study, the analysis of the interactions in solid form of ketoprofen-coformers was carried out using the differential scanning calorimetry (DSC) and hot stage microscopy (HSM) with adipic acid and isonicotinamide as coformers. From the experimental results, the mixtures of ketoprofen-adipic acid show a solid-liquid phase diagram that indicates a simple eutectic system with eutectic points on the molar fraction of ketoprofen 0.9 and temperature at 92.9 °C. The ketoprofen-isonicotinamide mixtures have a eutectic system with the peritectic point. The solid-liquid phase diagram has indicated that the ketoprofen-adipic acid in eutectic composition forms a miscible liquid phase without interaction in its solid form, whereas the ketoprofen-isonicotinamide forms a miscible liquid phase accompanied by interaction with the excess component. The results of the HSM analysis showed the same phenomenon as the result of the DSC experiment and have confirmed with the FTIR analysis

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In silico screening of dicarboxylic acids for cocrystallization with phenylpiperazine derivatives based on both cocrystallization propensity and solubility advantage

Cited by 21 publications

References 65 publications

Selection of effective cocrystals former for dissolution rate improvement of active pharmaceutical ingredients based on lipoaffinity index

Selection of effective cocrystals former for dissolution rate improvement of active pharmaceutical ingredients based on lipoaffinity index

Engineering Cocrystals of Poorly Water-Soluble Drugs to Enhance Dissolution in Aqueous Medium

Analysis of Solid-State Interactions of Ketoprofen-Coformer Binary Mixtures by DSC and Hot Stage Microscopy

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