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微凝胶酶:细胞色素 P450 BM3 在微凝胶中的 pH 不依赖固定化。

MicroGelzymes: pH-Independent Immobilization of Cytochrome P450 BM3 in Microgels.

机构信息

Institute of Biotechnology, RWTH Aachen University, Worringerweg 3, 52074 Aachen, Germany.

DWI-Leibniz-Institute for Interactive Materials e.V., Forckenbeckstraβe 50, 52074 Aachen, Germany.

出版信息

Biomacromolecules. 2020 Dec 14;21(12):5128-5138. doi: 10.1021/acs.biomac.0c01262. Epub 2020 Nov 18.

DOI:10.1021/acs.biomac.0c01262
PMID:33206503
Abstract

Microgels are an emerging class of "ideal" enzyme carriers because of their chemical and process stability, biocompatibility, and high enzyme loading capability. In this work, we synthesized a new type of permanently positively charged poly(-vinylcaprolactam) (PVCL) microgel with 1-vinyl-3-methylimidazolium (quaternization of nitrogen by methylation of -vinylimidazole moieties) as a comonomer (PVCL/VimQ) through precipitation polymerization. The PVCL/VimQ microgels were characterized with respect to their size, charge, swelling degree, and temperature responsiveness in aqueous solutions. P450 monooxygenases are usually challenging to immobilize, and often, high activity losses occur after the immobilization (in the case of P450 BM3 from up to 100% loss of activity). The electrostatic immobilization of P450 BM3 in permanently positively charged PVCL/VimQ microgels was achieved without the loss of catalytic activity at the pH optimum of P450 BM3 (pH 8; ∼9.4 nmol 7-hydroxy-3-carboxy coumarin ethyl ester/min for free and immobilized P450 BM3); the resulting P450-microgel systems were termed P450 MicroGelzymes (P450 μ-Gelzymes). In addition, P450 μ-Gelzymes offer the possibility of reversible ionic strength-triggered release and re-entrapment of the biocatalyst in processes (e.g., for catalyst reuse). Finally, a characterization of the potential of P450 μ-Gelzymes to provide resistance against cosolvents (acetonitrile, dimethyl sulfoxide, and 2-propanol) was performed to evaluate the biocatalytic application potential.

摘要

微凝胶是一类新兴的“理想”酶载体,因为它们具有化学和过程稳定性、生物相容性和高酶负载能力。在这项工作中,我们通过沉淀聚合合成了一种新型的永久性正电荷聚(-己内酯)(PVCL)微凝胶,其共聚单体为 1-乙烯基-3-甲基咪唑(-乙烯基咪唑部分的氮甲基化季铵化)(PVCL/VimQ)。研究了 PVCL/VimQ 微凝胶在水溶液中的粒径、电荷、溶胀度和温度响应。细胞色素 P450 单加氧酶通常难以固定,并且固定后通常会发生高活性损失(在 P450 BM3 的情况下,活性损失高达 100%)。通过静电固定化将 P450 BM3 固定在永久性正电荷的 PVCL/VimQ 微凝胶中,在 P450 BM3 的最佳 pH 值(pH 8;游离和固定化的 P450 BM3 的活性约为 9.4 nmol 7-羟基-3-羧酸香豆素乙酯/分钟)下不损失催化活性;所得的 P450-微凝胶体系被称为 P450 MicroGelzymes(P450 μ-Gelzymes)。此外,P450 μ-Gelzymes 提供了在过程中可逆离子强度触发释放和再捕获生物催化剂的可能性(例如,用于催化剂重复使用)。最后,对 P450 μ-Gelzymes 提供抗共溶剂(乙腈、二甲基亚砜和 2-丙醇)的能力进行了表征,以评估其生物催化应用潜力。

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