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在杆菌肽生物合成中 BacA 和 BacB 对预苯酸的串联作用下的烯烃异构区域化学。

Olefin isomerization regiochemistries during tandem action of BacA and BacB on prephenate in bacilysin biosynthesis.

机构信息

Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, Boston, Massachusetts 02115, United States.

出版信息

Biochemistry. 2012 Apr 17;51(15):3241-51. doi: 10.1021/bi300254u. Epub 2012 Apr 6.

Abstract

BacA and BacB, the first two enzymes of the bacilysin pathway, convert prephenate to an exocylic regioisomer of dihydrohydroxyphenylpyruvate (ex-H(2)HPP) on the way to the epoxycyclohexanone warhead in the dipeptide antibiotic, bacilysin. BacA decarboxylates prephenate without aromatization, converting the 1,4-diene in prephenate to the endocyclic 1,3-diene in Δ(4),Δ(8)-dihydrohydroxyphenylpyruvate (en-H(2)HPP). BacB then performs an allylic isomerization to bring the diene into conjugation with the 2-ketone in the product Δ(3),Δ(5)-dihydrohydroxyphenylpyruvate (ex-H(2)HPP). To prove that BacA acts regiospecifically on one of the two prochiral olefins in prephenate, we generated 1,5,8-[(13)C]-chorismate from bacterial fermentation of 5-[(13)C]-glucose and in turn produced 2,4,6-[(13)C]-prephenate via chorismate mutase. Tandem action of BacA and BacB gave 2,4,8-[(13)C]-7R-ex-H(2)HPP, showing that BacA isomerizes only the pro-R double bond in prephenate. Nonenzymatic isomerization of the BacA product into conjugation gives only the Δ(3)E-geometric isomer of Δ(3),Δ(5)-ex-H(2)HPP. On the other hand, acceleration of the allylic isomerization by BacB gives a mixture of the E- and Z-geometric isomers of the 7R- product, indicating some rerouting of the flux, likely through dienolate geometric isomers.

摘要

BacA 和 BacB 是 bacilysin 途径的前两个酶,它们将预苯酸转化为二肽抗生素 bacilysin 中环己酮弹头的外环异构物二氢羟苯基丙酮酸(ex-H(2)HPP)。BacA 在没有芳构化的情况下脱羧预苯酸,将预苯酸中的 1,4-二烯转化为Δ(4),Δ(8)-二氢羟苯基丙酮酸(en-H(2)HPP)中的内环 1,3-二烯。BacB 然后进行烯丙基异构化,使二烯与产物Δ(3),Δ(5)-二氢羟苯基丙酮酸(ex-H(2)HPP)中的 2-酮共轭。为了证明 BacA 在预苯酸中的两个前手性烯烃之一上具有区域特异性作用,我们从细菌发酵 5-[(13)C]-葡萄糖生成 1,5,8-[(13)C]-分支酸,并依次通过分支酸变位酶生成 2,4,6-[(13)C]-预苯酸。BacA 和 BacB 的串联作用得到 2,4,8-[(13)C]-7R-ex-H(2)HPP,表明 BacA 仅异构化预苯酸中的 pro-R 双键。BacA 产物的非酶异构化进入共轭仅给出Δ(3)E-几何异构体的Δ(3),Δ(5)-ex-H(2)HPP。另一方面,BacB 的加速烯丙基异构化给出 7R-产物的 E-和 Z-几何异构体的混合物,表明通量的一些重路由,可能通过烯醇化物几何异构体。

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