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Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation

Hesperetin (HES) is a weakly acidic flavonoid of topical interest owing to its antiviral properties. Despite the presence of HES in many dietary supplements, its bioavailability is hindered by poor aqueous solubility (1.35 µg ml(−1)) and rapid first-pass metabolism. Cocrystallization has evolved as...

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Autores principales: Jin, Shasha, Haskins, Molly M., Deng, Cheng-Hua, Matos, Catiúcia R. M. O., Zaworotko, Michael J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: International Union of Crystallography 2023
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10161764/
https://www.ncbi.nlm.nih.gov/pubmed/37079399
http://dx.doi.org/10.1107/S205225252300266X
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author Jin, Shasha
Haskins, Molly M.
Deng, Cheng-Hua
Matos, Catiúcia R. M. O.
Zaworotko, Michael J.
author_facet Jin, Shasha
Haskins, Molly M.
Deng, Cheng-Hua
Matos, Catiúcia R. M. O.
Zaworotko, Michael J.
author_sort Jin, Shasha
collection PubMed
description Hesperetin (HES) is a weakly acidic flavonoid of topical interest owing to its antiviral properties. Despite the presence of HES in many dietary supplements, its bioavailability is hindered by poor aqueous solubility (1.35 µg ml(−1)) and rapid first-pass metabolism. Cocrystallization has evolved as a promising approach to generate novel crystal forms of biologically active compounds and enhance the physicochemical properties without covalent modification. In this work, crystal engineering principles were employed to prepare and characterize various crystal forms of HES. Specifically, two salts and six new ionic cocrystals (ICCs) of HES involving sodium or potassium salts of HES were studied using single-crystal X-ray diffraction (SCXRD) or powder X-ray diffraction and thermal measurements. Structures of seven of the new crystalline forms were elucidated by SCXRD, which revealed two families of isostructural ICCs in terms of their crystal packing and confirmed the presence of phenol⋯phenolate (PhOH⋯PhO(−)) supramolecular heterosynthons. Diverse HES conformations were observed amongst these structures, including unfolded and folded (previously unreported) conformations. One ICC, HES with the sodium salt of HES (NESNAH), was scalable to the gram scale and found to be stable after accelerated stability testing (exposure to elevated heat and humidity). HESNAH reached C (max) after 10 min in PBS buffer 6.8 compared with 240 min in pure HES. In addition, relative solubility was observed to be 5.5 times greater, offering the possibility of improved HES bioavailability.
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spelling pubmed-101617642023-05-06 Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation Jin, Shasha Haskins, Molly M. Deng, Cheng-Hua Matos, Catiúcia R. M. O. Zaworotko, Michael J. IUCrJ Research Papers Hesperetin (HES) is a weakly acidic flavonoid of topical interest owing to its antiviral properties. Despite the presence of HES in many dietary supplements, its bioavailability is hindered by poor aqueous solubility (1.35 µg ml(−1)) and rapid first-pass metabolism. Cocrystallization has evolved as a promising approach to generate novel crystal forms of biologically active compounds and enhance the physicochemical properties without covalent modification. In this work, crystal engineering principles were employed to prepare and characterize various crystal forms of HES. Specifically, two salts and six new ionic cocrystals (ICCs) of HES involving sodium or potassium salts of HES were studied using single-crystal X-ray diffraction (SCXRD) or powder X-ray diffraction and thermal measurements. Structures of seven of the new crystalline forms were elucidated by SCXRD, which revealed two families of isostructural ICCs in terms of their crystal packing and confirmed the presence of phenol⋯phenolate (PhOH⋯PhO(−)) supramolecular heterosynthons. Diverse HES conformations were observed amongst these structures, including unfolded and folded (previously unreported) conformations. One ICC, HES with the sodium salt of HES (NESNAH), was scalable to the gram scale and found to be stable after accelerated stability testing (exposure to elevated heat and humidity). HESNAH reached C (max) after 10 min in PBS buffer 6.8 compared with 240 min in pure HES. In addition, relative solubility was observed to be 5.5 times greater, offering the possibility of improved HES bioavailability. International Union of Crystallography 2023-04-21 /pmc/articles/PMC10161764/ /pubmed/37079399 http://dx.doi.org/10.1107/S205225252300266X Text en © Shasha Jin et al. 2023 https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution (CC-BY) Licence, which permits unrestricted use, distribution, and reproduction in any medium, provided the original authors and source are cited.
spellingShingle Research Papers
Jin, Shasha
Haskins, Molly M.
Deng, Cheng-Hua
Matos, Catiúcia R. M. O.
Zaworotko, Michael J.
Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation
title Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation
title_full Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation
title_fullStr Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation
title_full_unstemmed Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation
title_short Crystal engineering of ionic cocrystals comprising Na/K salts of hesperetin with hesperetin molecules and solubility modulation
title_sort crystal engineering of ionic cocrystals comprising na/k salts of hesperetin with hesperetin molecules and solubility modulation
topic Research Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10161764/
https://www.ncbi.nlm.nih.gov/pubmed/37079399
http://dx.doi.org/10.1107/S205225252300266X
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