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Tailored Mutants of Phenylalanine Ammonia‐Lyase from Petroselinum crispum for the Synthesis of Bulky l‐ and d‐Arylalanines

机译:定制的Petroselinum crispum苯丙氨酸氨化酶突变体用于合成大体积的l-和d-芳基丙氨酸

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摘要

Tailored mutants of phenylalanine ammonia‐lyase from Petroselinum crispum (PcPAL) were created and tested in ammonia elimination from various sterically demanding, non‐natural analogues of phenylalanine and in ammonia addition reactions into the corresponding (E)‐arylacrylates. The wild‐type PcPAL was inert or exhibited quite poor conversions in both reactions with all members of the substrate panel. Appropriate single mutations of residue F137 and the highly conserved residue I460 resulted in PcPAL variants that were active in ammonia elimination but still had a poor activity in ammonia addition onto bulky substrates. However, combined mutations that involve I460 besides the well‐studied F137 led to mutants that exhibited activity in ammonia addition as well. The synergistic multiple mutations resulted in substantial substrate scope extension of PcPAL and opened up new biocatalytic routes for the synthesis of both enantiomers of valuable phenylalanine analogues, such as (4‐methoxyphenyl)‐, (napthalen‐2‐yl)‐, ([1,1′‐biphenyl]‐4‐yl)‐, (4′‐fluoro‐[1,1′‐biphenyl]‐4‐yl)‐, and (5‐phenylthiophene‐2‐yl)alanines.
机译:创建了量身定制的来自Petroselinum crispum(PcPAL)的苯丙氨酸解氨酶突变体,并进行了测试,测试了各种空间需求的非天然苯丙氨酸类似物的氨消除作用,以及将氨加成反应成相应的(E)-芳基丙烯酸酯的反应。在与底物面板所有成员的两个反应中,野生型PcPAL均呈惰性或转化非常差。残基F137和高度保守的残基I460的适当单突变导致PcPAL变异体具有消除氨的活性,但向大体积底物上添加氨的活性仍然很差。但是,除了经过充分研究的F137外,涉及I460的组合突变还导致了在氨添加方面也具有活性的突变体。协同多重突变导致PcPAL的底物范围大大扩展,并开辟了新的生物催化路线,用于合成有价值的苯丙氨酸类似物的两种对映异构体,例如(4-甲氧基苯基)-,(萘甲基-2-基)-,([1 ,1'-联苯基] -4-基),(4'-氟-[1,1'-联苯基] -4-基)-和(5-苯基噻吩-2-基)丙氨酸。

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