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基于金属有机框架的氧载体,通过掺入金纳米酶而具有抗氧化活性。

Metal-organic framework-based oxygen carriers with antioxidant activity resulting from the incorporation of gold nanozymes.

作者信息

Liu Xiaoli, Domingues Nency Patricio, Oveisi Emad, Coll-Satue Clara, Jansman Michelle Maria Theresia, Smit Berend, Hosta-Rigau Leticia

机构信息

DTU Health Tech, Center for Nanomedicine and Theranostics, Technical University of Denmark, Nils Koppels Allé, Building 423, 2800 Kgs. Lyngby, Denmark.

Laboratory of Molecular Simulation (LSMO), Institute of Chemical Sciences and Engineering (ISIC), École Polytechnique Fédérale de Lausanne (EPFL)-Valais, CH-1950 Sion, Switzerland.

出版信息

Biomater Sci. 2023 Mar 28;11(7):2551-2565. doi: 10.1039/d2bm01405j.

Abstract

Blood transfusions are a life-saving procedure since they can preserve the body's oxygen levels in patients suffering from acute trauma, undergoing surgery, receiving chemotherapy or affected by severe blood disorders. Due to the central role of hemoglobin (Hb) in oxygen transport, so-called Hb-based oxygen carriers (HBOCs) are currently being developed for situations where donor blood is not available. In this context, an important challenge that needs to be addressed is the oxidation of Hb into methemoglobin (metHb), which is unable to bind and release oxygen. While several research groups have considered the incorporation of antioxidant enzymes to create HBOCs with minimal metHb conversion, the use of biological enzymes has important limitations related to their high cost, potential immunogenicity or low stability . Thus, nanomaterials with enzyme-like properties (, nanozymes (NZs)) have emerged as a promising alternative. Amongst the different NZs, gold (Au)-based metallic nanoparticles are widely used for biomedical applications due to their biocompatibility and multi-enzyme mimicking abilities. Thus, in this work, we incorporate Au-based NZs into a type of HBOC previously reported by our group (, Hb-loaded metal-organic framework (MOF)-based nanocarriers (NCs)) and investigate their antioxidant properties. Specifically, we prepare MOF-NCs loaded with Au-based NZs and demonstrate their ability to catalytically deplete over multiple rounds of two prominent reactive oxygen species (ROS) that exacerbate Hb's autoxidation (, hydrogen peroxide and the superoxide radical). Importantly, following loading with Hb, we show how these ROS-scavenging properties translate into a decrease in metHb content. All in all, these results highlight the potential of NZs to create novel HBOCs with antioxidant protection which may find applications as a blood substitute in the future.

摘要

输血是一种挽救生命的医疗手段,因为它可以维持遭受急性创伤、接受手术、进行化疗或患有严重血液疾病患者体内的氧含量。由于血红蛋白(Hb)在氧运输中起着核心作用,目前正在研发所谓的基于血红蛋白的氧载体(HBOCs),用于无法获得供血的情况。在这种背景下,一个需要解决的重要挑战是Hb氧化为高铁血红蛋白(metHb),而高铁血红蛋白无法结合和释放氧气。虽然几个研究小组考虑引入抗氧化酶来制备metHb转化率最低的HBOCs,但生物酶的使用存在一些重要局限性,如成本高、潜在的免疫原性或稳定性低。因此,具有类酶性质的纳米材料,即纳米酶(NZs),已成为一种有前途的替代方案。在不同的纳米酶中,基于金(Au)的金属纳米颗粒因其生物相容性和多酶模拟能力而被广泛用于生物医学应用。因此,在这项工作中,我们将基于Au的纳米酶整合到我们小组之前报道的一种HBOC中,即负载Hb的金属有机框架(MOF)基纳米载体(NCs),并研究它们的抗氧化性能。具体来说,我们制备了负载基于Au的纳米酶的MOF-NCs,并证明它们能够在多轮催化过程中消耗两种加剧Hb自氧化的主要活性氧(ROS),即过氧化氢和超氧阴离子自由基。重要的是,在负载Hb后,我们展示了这些ROS清除特性如何转化为metHb含量的降低。总而言之,这些结果突出了纳米酶在创建具有抗氧化保护作用的新型HBOCs方面的潜力,这些HBOCs未来可能会作为血液替代品得到应用。

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