Structure, Self-Assembly, and Phase Behavior of Neuroactive N‑Acyl GABAs: Doxorubicin Encapsulation in NPGABA/DPPC Liposomes and Release Studies

N-Acylated amino acids and neurotransmitters in mammals exert significant biological effects on the nervous system, immune responses, and vasculature. N-Acyl derivatives of γ-aminobutyric acid (N-acyl GABA), which belong to both classes mentioned above, are prominent among them. In this work, a homo...

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Veröffentlicht in:Langmuir 2024-04, Vol.40 (15), p.7883-7895
Hauptverfasser: Chinapaka, Ravindar, Sivaramakrishna, Dokku, Choudhury, Suman Kumar, Manasa, Konga, Cheppali, Sudheer K., Swamy, Musti J.
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Sprache:eng
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Zusammenfassung:N-Acylated amino acids and neurotransmitters in mammals exert significant biological effects on the nervous system, immune responses, and vasculature. N-Acyl derivatives of γ-aminobutyric acid (N-acyl GABA), which belong to both classes mentioned above, are prominent among them. In this work, a homologous series of N-acyl GABAs bearing saturated N-acyl chains (C8–C18) have been synthesized and characterized with respect to self-assembly, thermotropic phase behavior, and supramolecular organization. Differential scanning calorimetric studies revealed that the transition enthalpies and entropies of N-acyl GABAs are linearly dependent on the acyl chain length. The crystal structure of N-tridecanoyl GABA showed that the molecules are packed in bilayers with the acyl chains aligned parallel to the bilayer normal and that the carboxyl groups from opposite layers associate to form dimeric structures involving strong O–H···O hydrogen bonds. In addition, N–H···O and C–H···O hydrogen bonds between amide moieties of adjacent molecules within each layer stabilize the molecular packing. Powder X-ray diffraction studies showed odd–even alternation in the d spacings, suggesting that the odd chain and even chain compounds pack differently. Equimolar mixtures of N-palmitoyl GABA and dipalmitoylphosphatidylcholine (DPPC) were found to form stable unilamellar vesicles with diameters of ∼300–340 nm, which could encapsulate doxorubicin, an anticancer drug, with higher efficiency and better release characteristics than DPPC liposomes at physiologically relevant pH. These liposomes exhibit faster release of doxorubicin at acidic pH (
ISSN:0743-7463
1520-5827
1520-5827
DOI:10.1021/acs.langmuir.3c03615