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基于丹宁酸配位框架合成的类酪氨酸羟化酶球形多孔铁-氮-碳纳米酶用于制备 L-DOPA

Spherical porous iron-nitrogen-carbon nanozymes derived from a tannin coordination framework for the preparation of L-DOPA by emulating tyrosine hydroxylase.

机构信息

Department of Pharmaceutical and Biological Engineering, School of Chemical Engineering, Sichuan University, Chengdu 610065, China.

出版信息

J Mater Chem B. 2023 Dec 6;11(47):11235-11250. doi: 10.1039/d3tb01082a.

DOI:10.1039/d3tb01082a
PMID:37953738
Abstract

L-3,4-Dihydroxyphenylalanine (L-DOPA) is widely used in Parkinson's disease treatment and is therefore in high demand. Development of an efficient method for the production of L-DOPA is urgently required. Nanozymes emulating tyrosine hydroxylase have attracted enormous attention for biomimetic synthesis of L-DOPA, but suffered from heterogeneity. Herein, a spherical porous iron-nitrogen-carbon nanozyme was developed for production of L-DOPA. Tannic acid chelated with ferrous ions to form a tannin-iron coordination framework as a carbon precursor. Iron and nitrogen co-doped carbon nanospheres were assembled an evaporation-induced self-assembly process using urea as a nitrogen source, F127 as a soft template, and formaldehyde as a crosslinker. The nanozyme was obtained after carbonization and acid etching. The nanozyme possessed a dispersive iron atom anchored in the Fe-N coordination structure as an active site to mimic the active center of tyrosine hydroxylase. The material showed spherical morphology, uniform size, high specific surface area, a mesoporous structure and easy magnetic separation. The structural properties could promote the density and accessibility of active sites and facilitate mass transport and electron transfer. The nanozyme exhibited high activity to catalyze the hydroxylation of tyrosine to L-DOPA as tyrosine hydroxylase in the presence of ascorbic acid and hydrogen peroxide. The titer of DOPA reached 1.2 mM. The nanozyme showed good reusability and comparable enzyme kinetics to tyrosine hydroxylase with a Michaelis-Menten constant of 2.3 mM. The major active species was the hydroxyl radical. Biomimetic simulation of tyrosine hydroxylase using a nanozyme with a fine structure provided a new route for the efficient production of L-DOPA.

摘要

L-3,4-二羟基苯丙氨酸(L-DOPA)广泛用于治疗帕金森病,因此需求量很大。迫切需要开发一种有效的 L-DOPA 生产方法。模拟酪氨酸羟化酶的纳米酶因其仿生合成 L-DOPA 而引起了极大的关注,但存在异质性。本文开发了一种球形多孔铁氮碳纳米酶,用于生产 L-DOPA。单宁酸与亚铁离子螯合形成单宁酸-铁配位框架作为碳前体。采用蒸发诱导自组装法,以尿素为氮源,F127 为软模板,甲醛为交联剂,组装铁氮共掺杂碳纳米球。碳化和酸蚀后得到纳米酶。纳米酶具有分散的铁原子锚定在 Fe-N 配位结构中作为活性位点,模拟酪氨酸羟化酶的活性中心。该材料具有球形形貌、均匀的尺寸、高比表面积、介孔结构和易于磁分离的特点。结构特性可以促进活性位点的密度和可及性,促进质量传输和电子转移。纳米酶在抗坏血酸和过氧化氢存在下表现出高活性,可催化酪氨酸羟化为 L-DOPA,类似于酪氨酸羟化酶。多巴的产量达到 1.2mM。纳米酶表现出良好的可重复使用性和与酪氨酸羟化酶相当的酶动力学,米氏常数为 2.3mM。主要的活性物质是羟基自由基。使用具有精细结构的纳米酶模拟酪氨酸羟化酶为 L-DOPA 的高效生产提供了一条新途径。

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