首页> 外文期刊>Chembiochem: A European journal of chemical biology >Biosynthesis of Xyrrolin, a New Cytotoxic Hybrid Polyketide/Non-ribosomal Peptide Pyrroline with Anticancer Potential, in Xylaria sp. BCC 1067
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Biosynthesis of Xyrrolin, a New Cytotoxic Hybrid Polyketide/Non-ribosomal Peptide Pyrroline with Anticancer Potential, in Xylaria sp. BCC 1067

机译:Xyrrolin,一种具有抗癌潜力的新型细胞毒性杂化聚酮/非核糖体肽吡咯啉的生物合成。密件副本1067

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摘要

A gene from Xylaria sp. BCC 1067, pks3, that encodes a putative 3660-residue hybrid polyketide synthase (PKS)on-ribosomal peptide synthetase (NRPS) was characterised by targeted gene disruption in combination with comprehensive product identification. Studies of the features of a corresponding mutant, YA3, allowed us to demonstrate that pks3 is responsible for the synthesis of a new pyrroline compound, named xyrrolin, in the wild-type Xylaria sp. BCC 1067. The structure of xyrrolin was established by extensive spectroscopic and spectrometric analyses, including low- and high-resolution MS, IR, ~1H NMR, ~(13)C NMR, ~(13)C NMR with Dept135, HMQC 2D NMR, HMBC 2D NMR and COSY 2D NMR. On the basis of the Pks3 domain organisation and the chemical structure of xyrrolin, we proposed that biosynthesis of this compound requires the condensation of a tetraketide and an L-serine unit, followed by Dieckmann or reductive cyclisation and enzymatic removal of ketone residue(s). Bioassays of the pure xyrrolin further displayed cytotoxicity against an oral cavity (KB) cancer cell line.
机译:Xylaria sp。的一个基因。编码假定的3660-残基杂合聚酮化合物合成酶(PKS)/非核糖体肽合成酶(NRPS)的BCC 1067 pks3的特征在于靶向基因破坏结合全面的产品鉴定。对相应突变体YA3的特征的研究使我们能够证明pks3负责在野生型Xylaria sp中合成名为吡咯啉的新吡咯啉化合物。 BCC1067。通过广泛的光谱和光谱分析,包括低和高分辨率MS,IR,〜1H NMR,〜(13)C NMR,〜(13)C NMR和Dept135,HMQC 2D NMR,确定了二甲苯咯啉的结构。 ,HMBC 2D NMR和COZY 2D NMR。基于Pks3结构域的结构和木糖醇的化学结构,我们建议该化合物的生物合成需要四酮化合物和L-丝氨酸单元的缩合,然后进行Dieckmann或还原环化和酶除去酮残基。 。纯粹的二甲苯甲酚的生物测定进一步显示出对口腔癌细胞系(KB)的细胞毒性。

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