化学
人血清白蛋白
领域(数学分析)
图像(数学)
血清白蛋白
白蛋白
生物化学
计算生物学
人工智能
数学
计算机科学
生物
数学分析
作者
Naoya Iwamoto,Takuma Kai,Shinsuke Inuki,Hiroaki Ohno,Hitoshi Maeda,Hiroshi Watanabe,Toru Maruyama,Shinya Oishi,Naoya Iwamoto,Takuma Kai,Shinsuke Inuki,Hiroaki Ohno,Hitoshi Maeda,Hiroshi Watanabe,Toru Maruyama,Shinya Oishi
标识
DOI:10.1021/acs.bioconjchem.4c00150
摘要
Human serum albumin (HSA) as a drug carrier can significantly improve the pharmacokinetic profiles of short-lived therapeutics. Conjugation of albumin-binding moieties (ABMs) to therapeutic agents may prolong their serum half-life by promoting their association with endogenous HSA. To discover a new molecular class of ABMs from mirror-image chemical space, a preparation protocol for bioactive HSA domain III and its d-enantiomer (d-HSA domain III) was established. Structural and functional analyses suggested that the synthetic protein enantiomers exhibited mirror-image structures and stereoselective neonatal fragement crystallizable receptor (FcRn) recognition. Additionally, the ligand-binding properties of synthetic l-HSA domain III were comparable with those of site II in native HSA, as confirmed using site II-selective fluorescent probes and an esterase substrate. Synthetic d-HSA domain III is an attractive tool for analyzing the site II-dependent molecular recognition properties of HSA.
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