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脂质化-阳离子化基序的引入赋予具有抗惊厥活性的系统生物可利用的神经肽 Y 和神经降压素类似物。

Introduction of lipidization-cationization motifs affords systemically bioavailable neuropeptide Y and neurotensin analogs with anticonvulsant activities.

机构信息

Department of Medicinal Chemistry, College of Pharmacy, University of Utah, Salt Lake City, UT 84108, USA.

出版信息

J Pept Sci. 2010 Sep;16(9):486-95. doi: 10.1002/psc.1266.

Abstract

The neuropeptides galanin (GAL), neuropeptide Y (NPY) or neurotensin (NT) exhibit anticonvulsant activities mediated by their respective receptors in the brain. To transform these peptides into potential neurotherapeutics, their systemic bioavailability and metabolic stability must be improved. Our recent studies with GAL analogs suggested that an introduction of lipoamino acids in the context of oligo-Lys residues (lipidization-cationization motif) significantly increases their penetration into the brain, yielding potent antiepileptic compounds. Here, we describe an extension of this strategy to NPY and NT. Rationally designed analogs of NPY and NT containing the lipidization-cationization motif were chemically synthesized and their physicochemical and pharmacological properties were characterized. The analogs NPY-BBB2 and NT-BBB1 exhibited increased serum stability, possessed log D > 1.1, retained high affinities toward their native receptors and produced potent antiseizure activities in animal models of epilepsy following intraperitoneal administration. Our results suggest that the combination of lipidization and cationization may be an effective strategy for improving systemic bioavailability and metabolic stability of various neuroactive peptides.

摘要

神经肽甘丙肽(GAL)、神经肽 Y(NPY)或神经降压素(NT)通过其在大脑中的相应受体表现出抗惊厥活性。为了将这些肽转化为潜在的神经治疗药物,必须提高它们的全身生物利用度和代谢稳定性。我们最近对 GAL 类似物的研究表明,在寡聚赖氨酸残基的背景下引入脂氨基酸(脂质化-阳离子化基序)可显著增加其进入大脑的能力,从而产生有效的抗癫痫化合物。在这里,我们将这一策略扩展到 NPY 和 NT。含有脂质化-阳离子化基序的 NPY 和 NT 的合理设计的类似物被化学合成,并对其物理化学和药理学性质进行了表征。类似物 NPY-BBB2 和 NT-BBB1 表现出增加的血清稳定性,具有 log D > 1.1,保留了对其天然受体的高亲和力,并在腹腔给药后产生了癫痫动物模型中的有效抗惊厥活性。我们的结果表明,脂质化和阳离子化的结合可能是提高各种神经活性肽的全身生物利用度和代谢稳定性的有效策略。

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