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首页> 外文期刊>Advances in Experimental Medicine and Biology >Structure-Function Relationship Study of Parathyroid Hormone (1-11) Analogues Containing D-AA
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Structure-Function Relationship Study of Parathyroid Hormone (1-11) Analogues Containing D-AA

机译:含D-AA的甲状旁腺激素(1-11)类似物的结构-功能关系研究

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摘要

In mammals, parathyroid hormone (PTH) [1], an 84 amino acid hormone, plays a vital role in regulating the concentrations of ionized calcium and phosphate in the blood and extracellular fluids. It has been shown that the first 34 amino acid fragment of PTH is sufficient to bind to and activate the PTH type I receptor (PTH1R), a heptahelical transmembrane G protein-coupled receptor. The molecular mechanisms by which PTH(l-34) binds to and activates the PTH1R have been extensively investigated [2]. The study of miniaturized PTH agonist and antagonist analogues has been the subject of extensive research [3], for the development of safer and non-parenteral bone anabolic drugs. Recent investigations focusing on the interaction of N-terminal fragments of PTH with PTH1R showed that certain modifications can increase signalling potency in peptides as short as 11 amino acids. To understand the role of the side-chains of all amino acid residues of the most active analogue of PTH(l-ll), H-Aib-Val-Aib-Glu-Ile-Gln-Leu-Nle-His-Gln-Har-NH2 (RP), we carried out a D-amino acid scan in which every L-AA was substituted with the corresponding D-AA, obtaining a library of PTH(l-ll) analogues which were tested for agonistic activity (Tab. 1).
机译:在哺乳动物中,甲状旁腺激素(PTH)[84]是一种84个氨基酸的激素,在调节血液和细胞外液中离子钙和磷酸盐的浓度中起着至关重要的作用。已经显示PTH的前34个氨基酸片段足以结合并激活PTH I型受体(PTH1R),PTH IR是七螺旋形跨膜G蛋白偶联受体。 PTH(1-34)结合并激活PTH1R的分子机制已得到广泛研究[2]。小型化的PTH激动剂和拮抗剂类似物的研究已成为广泛的研究主题[3],以开发更安全和非肠胃外的骨合成代谢药物。最近针对PTH N末端片段与PTH1R相互作用的研究表明,某些修饰可以增加短至11个氨基酸的肽的信号传导能力。要了解最活跃的PTH(1-3)类似物的所有氨基酸残基的侧链的作用,H-Aib-Val-Aib-Glu-Ile-Gln-Leu-Nle-His-Gln-Har -NH2(RP),我们进行了D-氨基酸扫描,其中每个L-AA被相应的D-AA取代,获得了PTH(3-1)类似物的文库,并测试了其激动活性(Tab。 1)。

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