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HAI Peptide and Backbone Analogs—Validation and Enhancement of Biostability and Bioactivity of BBB Shuttles

机译:HAI肽和骨干类似物— BBB穿梭飞机的生物稳定性和生物活性的验证和增强

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摘要

Low effectiveness and resistance to treatments are commonplace in disorders of the central nervous system (CNS). These issues concern mainly the blood-brain barrier (BBB), which preserves homeostasis in the brain and protects this organ from toxic molecules and biohazards by regulating transport through it. BBB shuttles—short peptides able to cross the BBB—are being developed to help therapeutics to cross this barrier. BBB shuttles can be discovered by massive exploration of chemical diversity (e.g. computational means, phage display) or rational design (e.g. derivatives from a known peptide/protein able to cross). Here we present the selection of a peptide shuttle (HAI) from several candidates and the subsequent in-depth in vitro and in vivo study of this molecule. In order to explore the chemical diversity of HAI and enhance its biostability, and thereby its bioactivity, we explored two new protease-resistant versions of HAI (i.e. the retro-D-version, and a version that was N-methylated at the most sensitive sites to enzymatic cleavage). Our results show that, while both versions of HAI are resistant to proteases, the retro-D-approach preserved better transport properties.
机译:低效和对治疗的抵抗力在中枢神经系统(CNS)疾病中很普遍。这些问题主要涉及血脑屏障(BBB),该血脑屏障可维持大脑的体内稳态,并通过调节通过该器官的运输来保护该器官免受毒性分子和生物危害的影响。正在开发BBB穿梭-能够穿过BBB的短肽-来帮助治疗剂突破这一障碍。 BBB穿梭蛋白可以通过大量探索化学多样性(例如计算手段,噬菌体展示)或合理设计(例如来自能够穿越的已知肽/蛋白质的衍生物)发现。在这里,我们介绍了从几种候选物中选择肽穿梭分子(HAI)以及随后对该分子进行的深入体内和体外研究。为了探索HAI的化学多样性并增强其生物稳定性,从而增强其生物活性,我们探索了HAI的两个新的蛋白酶抗性版本(即retro-D版本,以及最敏感的N-甲基化版本酶切位点)。我们的结果表明,尽管两种HAI都对蛋白酶具有抗性,但逆D途径保留了更好的运输特性。

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