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In Vitro Membrane Permeation Studies and in Vivo Antinociception of Glycosylated Dmt1-DALDA Analogues

机译:糖基化Dmt1-DALDA类似物的体外膜渗透研究和体内抗伤害感受

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In this study the μ opioid receptor (MOR) ligands DALDA (Tyr-D-Arg-Phe-Lys-NH2) and Dmt1-DALDA (Dmt- D-Arg-Phe-Lys-NH2, Dmt = 2′,6′-dimethyltyrosine) were glycosylated at the N- or C-terminus. Subsequently, the modified peptides were subjected to in vitro and in vivo evaluation. In contrast to the N-terminally modified peptide (3), all peptide analogues derivatized at the C-terminus (4-7) proved to possess high affinity and agonist potency at both MOR and DOR (δ opioid receptor). Results of the Caco-2 monolayer permeation, as well as in vitro blood-brain barrier model experiments, showed that, in the case of compound 4, the glycosylation only slightly diminished the lumen-to-blood and blood-to-lumen transport. Altogether, these experiments were indicative of transcellular transport but not active transport. In vivo assays demonstrated that the peptides were capable of (i) crossing the blood-brain barrier (BBB) and (ii) activating both the spinal ascending as well as the descending opioid pathways, as determined by the tail-flick and hot-plate assays, respectively. In contrast to the highly selective MOR agonist Dmt1-DALDA 1, compounds 4-7 are mixed MOR/DOR agonists, expected to produce reduced opioid-related side effects.
机译:在这项研究中,μ阿片受体(MOR)配体DALDA(Tyr-D-Arg-Phe-Lys-NH2)和Dmt1-DALDA(Dmt-D-Arg-Phe-Lys-NH2,Dmt = 2',6'-二甲基酪氨酸)在N或C端被糖基化。随后,对修饰的肽进行体外和体内评估。与N末端修饰的肽(3)相比,在C端(4-7)衍生的所有肽类似物均被证明在MOR和DOR(δ阿片受体)上均具有高亲和力和激动剂效能。 Caco-2单层渗透的结果以及体外血脑屏障模型实验表明,在化合物4的情况下,糖基化仅略微减少了内腔至血液和血液至内腔的转运。总而言之,这些实验表明跨细胞转运,但不是主动转运。体内试验表明,该肽能够(i)穿越血脑屏障(BBB)和(ii)激活脊柱上升和下降的阿片样物质途径,这由甩尾法和热板法确定分析。与高度选择性的MOR激动剂Dmt1-DALDA 1相反,化合物4-7是MOR / DOR混合激动剂,预期会减少与阿片类药物有关的副作用。

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