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有机介质中的高活性生物催化剂:固态缓冲剂作为蛋白质包被微晶的固定基质。

High-activity biocatalysts in organic media: solid-state buffers as the immobilisation matrix for protein-coated microcrystals.

作者信息

Kreiner Michaela, Parker Marie Claire

机构信息

Department of Chemistry, University of Glasgow, Joseph Black Building, Glasgow G12 8QQ, Scotland, UK.

出版信息

Biotechnol Bioeng. 2004 Jul 5;87(1):24-33. doi: 10.1002/bit.20101.

Abstract

Recently, we reported a new high-activity biocatalyst for use in organic media termed protein-coated microcrystals (PCMC) (Kreiner et al. [2001] Chem Commun 12:1096-1097). These novel particles consist of water-soluble micron-sized crystalline particles coated with the given biocatalyst(s) and are prepared in a one-step rapid dehydration process. In this study we extended the choice of immobilisation matrix from a simple inorganic salt, K(2)SO(4), to other compounds, both inorganic and zwitterionic, that act as solid-state buffers for biocatalysis in organic media. The catalytic activity of serine proteases subtilisin Carlsberg (SC) and alpha-chymotrypsin (CT) were significantly increased when coated onto the surface of solid-state buffers, as measured in acetonitrile/1wt% H(2)O. SC-PCMC with both organic and inorganic buffer carriers (Na-AMPSO, Na(2)CO(3), and NaHCO(3)) showed a 3-fold greater activity than that observed when using the unbuffered system (PCMC-SC/K(2)SO(4)). In comparison with freeze-dried preparations, this represents an approximately 3,000-fold increase in catalytic activity. Importantly, there is no improvement in catalytic activity upon external addition of any of the solid-state buffers to the reaction mixture. When acting in a solid-state buffer capacity, good buffering capacity was observed with SC-PCMC (3 wt% protein loading) prepared from a 1:1 mixture of AMPSO and AMPSO-Na. Alternatively, increasing the amount of solid-state buffer in the system allows improvement of the buffering. This can be achieved either by decreasing the protein loading of the SC/Na-AMPSO-PCMC or by addition of further external solid-state buffer to the reaction mixture. The catalytic activity of lipase-PCMC prepared from solid-state buffers was found less responsive to immobilisation.

摘要

最近,我们报道了一种用于有机介质的新型高活性生物催化剂,称为蛋白质包被微晶(PCMC)(Kreiner等人,[2001]《化学通讯》12:1096 - 1097)。这些新型颗粒由涂有特定生物催化剂的水溶性微米级晶体颗粒组成,并通过一步快速脱水过程制备。在本研究中,我们将固定化基质的选择从简单的无机盐K₂SO₄扩展到其他化合物,包括无机化合物和两性离子化合物,它们在有机介质中作为生物催化的固态缓冲剂。当丝氨酸蛋白酶枯草芽孢杆菌蛋白酶(SC)和α-胰凝乳蛋白酶(CT)包被在固态缓冲剂表面时,其催化活性显著提高,这是在乙腈/1wt% H₂O中测量的。具有有机和无机缓冲载体(Na - AMPSO、Na₂CO₃和NaHCO₃)的SC - PCMC显示出比使用无缓冲系统(PCMC - SC/K₂SO₄)时观察到的活性高3倍。与冻干制剂相比,这代表催化活性提高了约3000倍。重要的是,向反应混合物中外部添加任何一种固态缓冲剂时,催化活性都没有提高。当以固态缓冲能力起作用时,由AMPSO和AMPSO - Na的1:1混合物制备的SC - PCMC(蛋白质负载量为3 wt%)观察到良好的缓冲能力。或者,增加系统中固态缓冲剂的量可以改善缓冲效果。这可以通过降低SC/Na - AMPSO - PCMC的蛋白质负载量或向反应混合物中添加更多外部固态缓冲剂来实现。发现由固态缓冲剂制备的脂肪酶 - PCMC的催化活性对固定化的响应较小。

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