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Understanding impact of pre-dissolved polymers on dissolution behavior of soluble carbamazepine cocrystal

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dc.contributor.author Ullah, Majeed
dc.contributor.author Khan, Saeed Ahmad
dc.contributor.author Shah, Syed Majid
dc.contributor.author Rabbani, Imran
dc.contributor.author Sadozai, Sajid Khan
dc.contributor.author Abbas, Naseer
dc.contributor.author Bin Asad, Muhammad Hasham Hassan
dc.contributor.author Badshah, Munair
dc.contributor.author Hasan, Syed Mohammad Farid
dc.contributor.author Hussain, Izhar
dc.date.accessioned 2022-12-13T04:38:54Z
dc.date.available 2022-12-13T04:38:54Z
dc.date.issued 2019-05-23
dc.identifier.citation Ullah, M., Khan, S. A., Shah, S. M., Rabbani, I., Sadozai, S. K., Abbas, N., ... & Hussain, I. (2019). Understanding impact of pre-dissolved polymers on dissolution behavior of soluble carbamazepine cocrystal. Pakistan Journal of Pharmaceutical Sciences, 32(3). en_US
dc.identifier.issn 1011-601X
dc.identifier.uri http://142.54.178.187:9060/xmlui/handle/123456789/14946
dc.description.abstract Cocrystallization is a novel approach for tackling the lower solubility concerns when they can yield solution concentration a lot better than their corresponding parent drug in crystalline form. To get the actual solubility and dissolution gains offered by the cocrystals, phase changes in solution (dissolution) has to be interrupted. In current study, we selected commonly used polymers in order to study their effects on the super saturation of carbamezepine-succinic acid (CBZ-SUC) cocrystal during dissolution studies. To observe solid phase changes during dissolution in situ Raman spectroscopy was used. At the completion of each test the solid phase was analyzed by Fourier-transform infrared spectroscopy (FTIR) and powder X-Ray diffractometry. In polymers absence, no dissolution improvement was achieved by the cocrystal owing to its quick transformation to the stable carbamazepine dihydrate (CBZDH). Pre-dissolved PVP at 2% w/v concentration did not inhibit CBZ crystallization as a dihydrate, whereas at 0.025% w/v pre-dissolved hydroxypropyl methyl cellulose acetate succinate (HPMCAS) did stabilize the cocrystal in buffer solution (pH 6.8) for the course of time studied. This cocrystal stabilization resulted in enhanced CBZ solubility ( ̴ 4fold) caused by cocrystal super saturation state. Seeding of this stable supersaturated state with 1% w/v CBZDH resulted in CBZ crystallization as dihydrate with ultimate loss of solubility advantage. en_US
dc.language.iso en en_US
dc.publisher Karachi: Faculty of Pharmacy & Pharmaceutical Sciences University of Karachi en_US
dc.subject Cocrystals en_US
dc.subject super saturation en_US
dc.subject crystallization inhibitor polymers en_US
dc.subject crystallization. en_US
dc.title Understanding impact of pre-dissolved polymers on dissolution behavior of soluble carbamazepine cocrystal en_US
dc.type Article en_US


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