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使用拟肽研究 Kiss1r 选定十肽激动剂的血清稳定性。

Serum stability of selected decapeptide agonists of KISS1R using pseudopeptides.

机构信息

Pharmaceutical Research Division, Takeda Pharmaceutical Company Ltd, Fujisawa, Kanagawa, Japan.

出版信息

Bioorg Med Chem Lett. 2012 Oct 15;22(20):6391-6. doi: 10.1016/j.bmcl.2012.08.069. Epub 2012 Aug 23.

Abstract

Metastin/kisspeptin, a 54-amino acid peptide, is the ligand of the G-protein-coupled receptor KISS1R which plays a key role in pathways that regulate reproduction and cell migration in many endocrine and gonadal tissues. The N-terminally truncated decapeptide, metastin(45-54), has 3-10 times higher receptor affinity and intracellular calcium ion-mobilizing activity but is rapidly inactivated in serum. In this study we designed and synthesized stable KISS1R agonistic decapeptide analogs with selected substitutions at positions 47, 50, and 51. Replacement of glycine with azaglycine (azaGly) in which the α-carbon is replaced with a nitrogen atom at position 51 improved the stability of amide bonds between Phe(50)-Gly(51) and Gly(51)-Leu(52) as determined by in vitro mouse serum stability studies. Substitution for tryptophan at position 47 with other amino acids such as serine, threonine, β-(3-pyridyl)alanine, and D-tryptophan (D-Trp), produced analogs that were highly stable in mouse serum. D-Trp(47) analog 13 showed not only high metabolic stability but also excellent KISS1R agonistic activity. Other labile peptides may have increased serum stability using amino acid substitution.

摘要

Metastin/kisspeptin 是一种 54 个氨基酸的肽,是 G 蛋白偶联受体 KISS1R 的配体,在调节许多内分泌和性腺组织中的生殖和细胞迁移途径中发挥关键作用。N 端截断的十肽 metastin(45-54) 具有 3-10 倍更高的受体亲和力和细胞内钙离子动员活性,但在血清中迅速失活。在这项研究中,我们设计并合成了具有选定取代的稳定 KISS1R 激动剂十肽类似物在位置 47、50 和 51。用氮原子取代α-碳的氮杂甘氨酸(azaGly)取代位置 51 处的甘氨酸,提高了 Phe(50)-Gly(51) 和 Gly(51)-Leu(52) 之间酰胺键的稳定性,这通过体外小鼠血清稳定性研究确定。用其他氨基酸如丝氨酸、苏氨酸、β-(3-吡啶基)丙氨酸和 D-色氨酸(D-Trp)取代位置 47 处的色氨酸,产生了在小鼠血清中高度稳定的类似物。D-Trp(47)类似物 13 不仅表现出高代谢稳定性,而且还具有优异的 KISS1R 激动活性。其他不稳定的肽可能通过氨基酸取代增加了血清稳定性。

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