Seifert Alexander, Vomund Sandra, Grohmann Katrin, Kriening Sebastian, Urlacher Vlada B, Laschat Sabine, Pleiss Jürgen
Institute of Technical Biochemistry, University of Stuttgart, Allmandring 31, 70569 Stuttgart, Germany.
Chembiochem. 2009 Mar 23;10(5):853-61. doi: 10.1002/cbic.200800799.
A minimal CYP102A1 mutant library of only 24 variants plus wild type was constructed by combining five hydrophobic amino acids (alanine, valine, phenylalanine, leucine and isoleucine) in two positions. Both positions are located close to the centre of the haem group. The first, position 87, has been shown to mediate substrate specificity and regioselectivity in CYP102A1. The second hotspot, position 328, was predicted to interact with all substrates during oxidation and has previously been identified by systematic analysis of 31 crystal structures and 6300 sequences of cytochrome P450 monooxygenases. By systematically altering the size of the side chains, a broad range of binding site shapes was generated. All variants were functionally expressed in E. coli. The library was screened with four terpene substrates geranylacetone, nerylacetone, (4R)-limonene and (+)-valencene. Only three variants showed no activity towards all four terpenes, while eleven variants demonstrated either a strong shift or improved regio- or stereoselectivity during oxidation of at least one substrate as compared to CYP102A1 wild type.
通过在两个位置组合五个疏水氨基酸(丙氨酸、缬氨酸、苯丙氨酸、亮氨酸和异亮氨酸)构建了一个仅包含24个变体加野生型的最小CYP102A1突变体文库。这两个位置都靠近血红素基团的中心。第一个位置是87位,已被证明在CYP102A1中介导底物特异性和区域选择性。第二个热点位置是328位,预计在氧化过程中与所有底物相互作用,并且先前已通过对31个晶体结构和6300个细胞色素P450单加氧酶序列的系统分析确定。通过系统地改变侧链的大小,产生了广泛的结合位点形状。所有变体都在大肠杆菌中进行了功能表达。该文库用四种萜类底物香叶基丙酮、橙花基丙酮、(4R)-柠檬烯和(+)-瓦伦烯进行筛选。只有三个变体对所有四种萜类均无活性,而与CYP102A1野生型相比,有11个变体在至少一种底物的氧化过程中表现出强烈的偏移或改善的区域或立体选择性。
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