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Single-site iron-anchored amyloid hydrogels as catalytic platforms for alcohol detoxification

乙醛 戒毒(替代医学) 化学 乙醇 生物化学 医学 病理 替代医学
作者
Jiaqi Su,Pengjie Wang,Wei Zhou,Mohammad Peydayesh,Jiangtao Zhou,Tonghui Jin,Felix Donat,C. Jin,Lu Xia,Kaiwen Wang,Fazheng Ren,Paul Van der Meeren,F. Pelayo Garcı́a de Arquer,Raffaele Mezzenga
出处
期刊:Nature Nanotechnology [Nature Portfolio]
卷期号:19 (8): 1168-1177 被引量:39
标识
DOI:10.1038/s41565-024-01657-7
摘要

Abstract Constructing effective antidotes to reduce global health impacts induced by alcohol prevalence is a challenging topic. Despite the positive effects observed with intravenous applications of natural enzyme complexes, their insufficient activities and complicated usage often result in the accumulation of toxic acetaldehyde, which raises important clinical concerns, highlighting the pressing need for stable oral strategies. Here we present an effective solution for alcohol detoxification by employing a biomimetic-nanozyme amyloid hydrogel as an orally administered catalytic platform. We exploit amyloid fibrils derived from β-lactoglobulin, a readily accessible milk protein that is rich in coordinable nitrogen atoms, as a nanocarrier to stabilize atomically dispersed iron (ferrous-dominated). By emulating the coordination structure of the horseradish peroxidase enzyme, the single-site iron nanozyme demonstrates the capability to selectively catalyse alcohol oxidation into acetic acid, as opposed to the more toxic acetaldehyde. Administering the gelatinous nanozyme to mice suffering from alcohol intoxication significantly reduced their blood-alcohol levels (decreased by 55.8% 300 min post-alcohol intake) without causing additional acetaldehyde build-up. Our hydrogel further demonstrates a protective effect on the liver, while simultaneously mitigating intestinal damage and dysbiosis associated with chronic alcohol consumption, introducing a promising strategy in effective alcohol detoxification.
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