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神经活性酰基 GABA 的结构、自组装和相行为:阿霉素在 NPGABA/DPPC 脂质体中的包封和释放研究。

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

机构信息

School of Chemistry, University of Hyderabad, Hyderabad 500046, India.

Department of Chemistry, School of Science, GITAM, Visakhapatnam 530045, India.

出版信息

Langmuir. 2024 Apr 16;40(15):7883-7895. doi: 10.1021/acs.langmuir.3c03615. Epub 2024 Apr 8.

Abstract

N-Acylated amino acids and neurotransmitters in mammals exert significant biological effects on the nervous system, immune responses, and vasculature. -Acyl derivatives of γ-aminobutyric acid (-acyl GABA), which belong to both classes mentioned above, are prominent among them. In this work, a homologous series of -acyl GABAs bearing saturated -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 -acyl GABAs are linearly dependent on the acyl chain length. The crystal structure of -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 spacings, suggesting that the odd chain and even chain compounds pack differently. Equimolar mixtures of -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 (<7.0), indicating their potential utility as drug carriers in cancer chemotherapy.

摘要

在哺乳动物中,N-酰基氨基酸和神经递质对神经系统、免疫反应和血管系统具有显著的生物学效应。-酰基衍生的γ-氨基丁酸(-酰基 GABA)属于上述两类物质,在其中尤为突出。在这项工作中,我们合成了一系列具有饱和-酰基链(C8-C18)的 -酰基 GABA 同系物,并对其自组装、热致相变行为和超分子组织进行了研究。差示扫描量热法研究表明,-酰基 GABA 的转变焓和熵与酰基链长度呈线性关系。-十三烷酰基 GABA 的晶体结构表明,分子以双层形式堆积,酰基链平行于双层法线排列,来自相反层的羧基基团相互作用形成涉及强 O-H···O 氢键的二聚体结构。此外,相邻分子酰胺部分之间的 N-H···O 和 C-H···O 氢键稳定了分子堆积。粉末 X 射线衍射研究表明,层间距存在奇-偶交替现象,表明奇数链和偶数链化合物的堆积方式不同。-棕榈酰基 GABA 和二棕榈酰磷脂酰胆碱(DPPC)的等摩尔混合物形成了直径约为 300-340nm 的稳定单层囊泡,能够包裹阿霉素这种抗癌药物,其在生理相关 pH 值下的包封效率和释放特性均优于 DPPC 脂质体。这些脂质体在酸性 pH(<7.0)下更快地释放阿霉素,表明它们在癌症化疗中作为药物载体的潜在应用价值。

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