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一种增强肽体内半衰期的仿生方法。

A biomimetic approach for enhancing the in vivo half-life of peptides.

作者信息

Penchala Sravan C, Miller Mark R, Pal Arindom, Dong Jin, Madadi Nikhil R, Xie Jinghang, Joo Hyun, Tsai Jerry, Batoon Patrick, Samoshin Vyacheslav, Franz Andreas, Cox Trever, Miles Jesse, Chan William K, Park Miki S, Alhamadsheh Mamoun M

机构信息

Department of Pharmaceutics &Medicinal Chemistry, Thomas J. Long School of Pharmacy &Health Sciences, University of the Pacific, Stockton, California, USA.

Department of Chemistry, University of the Pacific, Stockton, California, USA.

出版信息

Nat Chem Biol. 2015 Oct;11(10):793-8. doi: 10.1038/nchembio.1907. Epub 2015 Sep 7.

Abstract

The tremendous therapeutic potential of peptides has not yet been realized, mainly owing to their short in vivo half-life. Although conjugation to macromolecules has been a mainstay approach for enhancing protein half-life, the steric hindrance of macromolecules often harms the binding of peptides to target receptors, compromising the in vivo efficacy. Here we report a new strategy for enhancing the in vivo half-life of peptides without compromising their potency. Our approach involves endowing peptides with a small molecule that binds reversibly to the serum protein transthyretin. Although there are a few molecules that bind albumin reversibly, we are unaware of designed small molecules that reversibly bind other serum proteins and are used for half-life extension in vivo. We show here that our strategy was effective in enhancing the half-life of an agonist for GnRH receptor while maintaining its binding affinity, which was translated into superior in vivo efficacy.

摘要

肽类巨大的治疗潜力尚未得到充分发挥,主要是由于其在体内的半衰期较短。尽管与大分子结合一直是延长蛋白质半衰期的主要方法,但大分子的空间位阻常常会损害肽与靶受体的结合,从而影响其体内疗效。在此,我们报告了一种在不影响肽效力的前提下延长其体内半衰期的新策略。我们的方法是赋予肽一个能与血清蛋白转甲状腺素蛋白可逆结合的小分子。虽然有一些分子能与白蛋白可逆结合,但我们尚未知晓有经过设计的可与其他血清蛋白可逆结合并用于体内延长半衰期的小分子。我们在此表明,我们的策略在延长促性腺激素释放激素(GnRH)受体激动剂半衰期的同时保持了其结合亲和力,进而转化为卓越的体内疗效。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/69e6/4575266/dc343ac41fc4/nihms714409f1.jpg

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