Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin

This study exploits the polymorphism and multi-component crystal formation of γ-amino butanoic acid (GABA) and its pharmaceutically active derivative, gabapentin. Two polymorphs of GABA and both polymorphs of gabapentin are structurally revisited, together with gabapentin monohydrate. Hereby, GABA f...

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Autores principales: Komisarek, Daniel, Demirbas, Fulya, Haj Hassani Sohi, Takin, Merz, Klaus, Schauerte, Carsten, Vasylyeva, Vera
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10536459/
https://www.ncbi.nlm.nih.gov/pubmed/37765268
http://dx.doi.org/10.3390/pharmaceutics15092299
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author Komisarek, Daniel
Demirbas, Fulya
Haj Hassani Sohi, Takin
Merz, Klaus
Schauerte, Carsten
Vasylyeva, Vera
author_facet Komisarek, Daniel
Demirbas, Fulya
Haj Hassani Sohi, Takin
Merz, Klaus
Schauerte, Carsten
Vasylyeva, Vera
author_sort Komisarek, Daniel
collection PubMed
description This study exploits the polymorphism and multi-component crystal formation of γ-amino butanoic acid (GABA) and its pharmaceutically active derivative, gabapentin. Two polymorphs of GABA and both polymorphs of gabapentin are structurally revisited, together with gabapentin monohydrate. Hereby, GABA form II is only accessible under special conditions using additives, whereas gabapentin converts to the monohydrate even in the presence of trace amounts of water. Different accessibilities and phase stabilities of these phases are still not fully clarified. Thus, indicators of phase stability are discussed involving intermolecular interactions, molecular conformations, and crystallization environment. Calculated lattice energy differences for polymorphs reveal their similar stability. Quantification of the hydrogen bond strengths with the atoms-in-molecules (AIM) model in conjunction with non-covalent interaction (NCI) plots also shows similar hydrogen bond binding energy values for all polymorphs. We demonstrate that differences in the interacting modes, in an interplay with the intermolecular repulsion, allow the formation of the desired phase under different crystallization environments. Salts and co-crystals of GABA and gabapentin with fumaric as well as succinic acid further serve as models to highlight how strongly HBs act as the motif-directing force in the solid-phase GABA-analogs. Six novel multi-component entities were synthesized, and structural and computational analysis was performed: GABA fumarate (2:1); two gabapentin fumarates (2:1) and (1:1); two GABA succinates (2:1) and (1:1); and a gabapentin:succinic acid co-crystal. Energetically highly attractive carboxyl/carboxylate interaction overcomes other factors and dominates the multi-component phase formation. Decisive commonalities in the crystallization behavior of zwitterionic GABA-derivatives are discussed, which show how they can and should be understood as a whole for possible related future products.
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spelling pubmed-105364592023-09-29 Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin Komisarek, Daniel Demirbas, Fulya Haj Hassani Sohi, Takin Merz, Klaus Schauerte, Carsten Vasylyeva, Vera Pharmaceutics Article This study exploits the polymorphism and multi-component crystal formation of γ-amino butanoic acid (GABA) and its pharmaceutically active derivative, gabapentin. Two polymorphs of GABA and both polymorphs of gabapentin are structurally revisited, together with gabapentin monohydrate. Hereby, GABA form II is only accessible under special conditions using additives, whereas gabapentin converts to the monohydrate even in the presence of trace amounts of water. Different accessibilities and phase stabilities of these phases are still not fully clarified. Thus, indicators of phase stability are discussed involving intermolecular interactions, molecular conformations, and crystallization environment. Calculated lattice energy differences for polymorphs reveal their similar stability. Quantification of the hydrogen bond strengths with the atoms-in-molecules (AIM) model in conjunction with non-covalent interaction (NCI) plots also shows similar hydrogen bond binding energy values for all polymorphs. We demonstrate that differences in the interacting modes, in an interplay with the intermolecular repulsion, allow the formation of the desired phase under different crystallization environments. Salts and co-crystals of GABA and gabapentin with fumaric as well as succinic acid further serve as models to highlight how strongly HBs act as the motif-directing force in the solid-phase GABA-analogs. Six novel multi-component entities were synthesized, and structural and computational analysis was performed: GABA fumarate (2:1); two gabapentin fumarates (2:1) and (1:1); two GABA succinates (2:1) and (1:1); and a gabapentin:succinic acid co-crystal. Energetically highly attractive carboxyl/carboxylate interaction overcomes other factors and dominates the multi-component phase formation. Decisive commonalities in the crystallization behavior of zwitterionic GABA-derivatives are discussed, which show how they can and should be understood as a whole for possible related future products. MDPI 2023-09-10 /pmc/articles/PMC10536459/ /pubmed/37765268 http://dx.doi.org/10.3390/pharmaceutics15092299 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Komisarek, Daniel
Demirbas, Fulya
Haj Hassani Sohi, Takin
Merz, Klaus
Schauerte, Carsten
Vasylyeva, Vera
Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin
title Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin
title_full Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin
title_fullStr Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin
title_full_unstemmed Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin
title_short Polymorphism and Multi-Component Crystal Formation of GABA and Gabapentin
title_sort polymorphism and multi-component crystal formation of gaba and gabapentin
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10536459/
https://www.ncbi.nlm.nih.gov/pubmed/37765268
http://dx.doi.org/10.3390/pharmaceutics15092299
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