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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Differential membrane fluidization by active and inactive cannabinoid analogues
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Differential membrane fluidization by active and inactive cannabinoid analogues

机译:活性和非活性大麻素类似物的差异膜流化

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摘要

The effects of the two cannabinomimetic drugs (-)-2-(6a,7,10,10a-tetrahydro-6,6,9-trimethyl-1-hydroxy-6H-dibenzo[b,d]-pyranyl-2-(hexyl)-1,3-dithiolane (AMG-3) and its pharmacologically less active 1-methoxy analogue (AMG-18) on the thermotropic and structural properties of dipalmitoyl-sn-glycero-3-phosphorylcholine (DPPC) liposomes have been studied by X-ray diffraction and differential scanning calorimetry (DSC). DSC data revealed that the incorporation of the drugs affect differently the thermotropic properties of DPPC. The presence of the more active drug distinctly broadened and attenuated both the pretransition and main phase transition of DPPC bilayers, while the inactive analogue had only minor effects. Small and wide angle X-ray diffraction data showed that the two cannabinoids have different effects on the lipid phase structures and on the hydrocarbon chain packing. The pharmacologically active analogue, AMG-3, was found to efficiently fluidize domains of the lipids in the L_250L? gel phase, and to perturb the regular multibilayer lattice. In the liquid crystalline L_α phase, AMG-3 was also found to cause irregularities in packing, suggesting that the drug induces local curvature. At the same concentration, the inactive AMG-18 had only minor structural effects on the lipids. At about 10-fold or higher concentrations, AMG-18 was found to produce similar but still less pronounced effects in comparison to those observed by AMG-3. The dose-dependent, different thermotropic and structural effects by the two cannabinoid analogues suggest that these may be related to their biological activity.
机译:两种大麻素药物(-)-2-(6a,7,10,10a-四氢-6,6,9-三甲基-1-羟基-6H-二苯并[b,d]-吡喃基-2-(己基)-1,3-二硫杂环戊烷(AMG-3)及其药理学活性较低的1-甲氧基类似物(AMG-18)对二棕榈酰-sn-甘油-3-磷酸胆碱(DPPC)脂质体的热致和结构性质的研究通过X射线衍射和差示扫描量热法(DSC),DSC数据表明,药物的掺入对DPPC的热致性能有不同的影响,活性更高的药物的存在明显拓宽并减弱了DPPC的预转变和主相转变。小分子和广角X射线衍射数据表明,这两种大麻素对脂质相结构和烃链堆积具有不同的影响,其药理活性类似物AMG-3为被发现可以有效地流化L_中脂质的结构域250升?凝胶相,并扰动规则的多层晶格。在液晶L_α相中,还发现AMG-3会导致堆积不规则,这表明该药物会引起局部弯曲。在相同浓度下,无活性的AMG-18对脂质的结构影响很小。在约10倍或更高的浓度下,与AMG-3观察到的结果相比,发现AMG-18产生了相似但不那么明显的作用。两种大麻素类似物的剂量依赖性,不同的热致和结构效应表明,这可能与其生物学活性有关。

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