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在大肠杆菌表达系统中工程化人类 PON1。

Engineering human PON1 in an E. coli expression system.

机构信息

Departments of Medicine (Div. of Medical Genetics) and Genome Sciences, University of Washington, Seattle, Washington, USA.

出版信息

Adv Exp Med Biol. 2010;660:37-45. doi: 10.1007/978-1-60761-350-3_5.

Abstract

Expression and purification of recombinant human paraoxonase-1 (rHuPON1) from bacterial systems have proven elusive. Most systems for successful production of recombinant PON1 have relied on either eukaryotic expression in baculovirus or prokaryotic expression of synthetic, gene-shuffled rabbit-mouse-human PON1 hybrid molecules. We review here methods and protocols for the production of pure, native rHuPON1 using an E. coli expression system followed by conventional column chromatographic purification. The resulting rHuPON1 is stable, active, and capable of protecting PON1 knockout mice (PON1(-/-)) from exposure to high levels of the organophosphorus (OP) compound diazoxon. Bacterially-derived rHuPON1 can be produced in large quantities and lacks the glycosylation of eukaryotic systems that produces immunogenic complications when used as a therapeutic. The rHuPON1 should be useful for treating insecticide OP exposures and reducing risks of other diseases resulting from low PON1 status. The ease of mutagenesis in bacterial systems will also allow for the generation and screening of rHuPON1 variants with enhanced catalytic efficiencies against nerve agents and other OP compounds.

摘要

从细菌系统中表达和纯化重组人对氧磷酶 1(rHuPON1)一直难以实现。大多数成功生产重组 PON1 的系统都依赖于杆状病毒中的真核表达或合成的、基因改组的兔-鼠-人 PON1 杂交分子的原核表达。我们在这里回顾了使用大肠杆菌表达系统生产纯的、天然的 rHuPON1 的方法和方案,然后进行常规的柱层析纯化。得到的 rHuPON1 稳定、活性高,能够保护 PON1 敲除小鼠(PON1(-/-))免受高浓度有机磷(OP)化合物敌敌畏的暴露。细菌衍生的 rHuPON1 可以大量生产,并且缺乏真核系统的糖基化,当用作治疗剂时会产生免疫原性并发症。rHuPON1 应该可用于治疗杀虫剂 OP 暴露,并降低由于 PON1 水平低而导致的其他疾病的风险。细菌系统中的突变容易进行,也允许生成和筛选具有增强的催化效率针对神经毒剂和其他 OP 化合物的 rHuPON1 变体。

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本文引用的文献

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Engineered recombinant human paraoxonase 1 (rHuPON1) purified from Escherichia coli protects against organophosphate poisoning.
Proc Natl Acad Sci U S A. 2008 Sep 2;105(35):12780-4. doi: 10.1073/pnas.0805865105. Epub 2008 Aug 18.
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