Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives
The purpose of this study is to confirm the impact of polar functional groups on inter and intra-molecular hydrogen bonding in haloperidol (HP) and droperidol (DP) and, hence, their effects on dissolution using a new approach. To confirm our theory, a new molecule: deshydroxy-haloperidol (DHP) was d...
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doaj-0c1bd88ecb604c80b98e68eeb6adda872020-11-24T22:47:25ZengMDPI AGMolecules1420-30492016-06-0121671910.3390/molecules21060719molecules21060719Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol DerivativesHardeep Saluja0Ahmed Mehanna1Riccardo Panicucci2Eman Atef3Department of Pharmaceutical Sciences, Southwestern Oklahoma State University, 100 Campus Drive, Weatherford, OK 73096-3098, USADepartment of Pharmaceutical Sciences, MCPHS-University-Boston, 179 Longwood Ave, Boston, MA 02115, USAWuXi AppTec, Cambridge, MA 02142, USADepartment of Pharmaceutical Sciences, MCPHS-University-Boston, 179 Longwood Ave, Boston, MA 02115, USAThe purpose of this study is to confirm the impact of polar functional groups on inter and intra-molecular hydrogen bonding in haloperidol (HP) and droperidol (DP) and, hence, their effects on dissolution using a new approach. To confirm our theory, a new molecule: deshydroxy-haloperidol (DHP) was designed and its synthesis was requested from a contract laboratory. The molecule was then studied and compared to DP and HP. Unlike DHP, both the HP and DP molecules have hydrogen donor groups, therefore, DHP was used to confirm the relative effects of the hydrogen donor group on solubility and crystal packing. The solid dispersions of the three structurally related molecules: HP, DP, and DHP were prepared using PVPK30, and characterized using XRPD and IR. A comparative dissolution study was carried out in aqueous medium. The absence of a hydrogen bonding donor group in DHP resulted in an unexpected increase in its aqueous solubility and dissolution rate from solid dispersion, which is attributed to weaker crystal pack. The increased dissolution rate of HP and DP from solid dispersions is attributed to drug-polymer hydrogen bonding that interferes with the drug-drug intermolecular hydrogen bonding and provides thermodynamic stability of the dispersed drug molecules. The drug-drug intermolecular hydrogen bond is the driving force for precipitation and crystal packing.http://www.mdpi.com/1420-3049/21/6/719drug crystal packinghydrogen bondingsolid dispersionhaloperidol-related compoundsmolecular interactionhydrophobic interactiondroperidoldeshydroxyhaloperidol |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Hardeep Saluja Ahmed Mehanna Riccardo Panicucci Eman Atef |
spellingShingle |
Hardeep Saluja Ahmed Mehanna Riccardo Panicucci Eman Atef Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives Molecules drug crystal packing hydrogen bonding solid dispersion haloperidol-related compounds molecular interaction hydrophobic interaction droperidol deshydroxyhaloperidol |
author_facet |
Hardeep Saluja Ahmed Mehanna Riccardo Panicucci Eman Atef |
author_sort |
Hardeep Saluja |
title |
Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives |
title_short |
Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives |
title_full |
Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives |
title_fullStr |
Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives |
title_full_unstemmed |
Hydrogen Bonding: Between Strengthening the Crystal Packing and Improving Solubility of Three Haloperidol Derivatives |
title_sort |
hydrogen bonding: between strengthening the crystal packing and improving solubility of three haloperidol derivatives |
publisher |
MDPI AG |
series |
Molecules |
issn |
1420-3049 |
publishDate |
2016-06-01 |
description |
The purpose of this study is to confirm the impact of polar functional groups on inter and intra-molecular hydrogen bonding in haloperidol (HP) and droperidol (DP) and, hence, their effects on dissolution using a new approach. To confirm our theory, a new molecule: deshydroxy-haloperidol (DHP) was designed and its synthesis was requested from a contract laboratory. The molecule was then studied and compared to DP and HP. Unlike DHP, both the HP and DP molecules have hydrogen donor groups, therefore, DHP was used to confirm the relative effects of the hydrogen donor group on solubility and crystal packing. The solid dispersions of the three structurally related molecules: HP, DP, and DHP were prepared using PVPK30, and characterized using XRPD and IR. A comparative dissolution study was carried out in aqueous medium. The absence of a hydrogen bonding donor group in DHP resulted in an unexpected increase in its aqueous solubility and dissolution rate from solid dispersion, which is attributed to weaker crystal pack. The increased dissolution rate of HP and DP from solid dispersions is attributed to drug-polymer hydrogen bonding that interferes with the drug-drug intermolecular hydrogen bonding and provides thermodynamic stability of the dispersed drug molecules. The drug-drug intermolecular hydrogen bond is the driving force for precipitation and crystal packing. |
topic |
drug crystal packing hydrogen bonding solid dispersion haloperidol-related compounds molecular interaction hydrophobic interaction droperidol deshydroxyhaloperidol |
url |
http://www.mdpi.com/1420-3049/21/6/719 |
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