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从耐盐粘细菌 Nannocystis pusilla B150 中生物合成苯并那罗酮 A,一种多药耐药逆转剂。

Biosynthesis of phenylnannolone A, a multidrug resistance reversal agent from the halotolerant myxobacterium Nannocystis pusilla B150.

出版信息

Chembiochem. 2014 Mar 21;15(5):757-65. doi: 10.1002/cbic.201300676.

Abstract

The myxobacterial strain Nannocystis pusilla B150 synthesizes the structurally new polyketides phenylnannolone A–C. Apart from some common volatiles and siderophores, these are the first natural products from the genus Nannocystis. Phenylnannolone A shows inhibitory activity towards the ABCB1 gene product P-glycoprotein and reverses daunorubicin resistance in cancer cells. To decipher the biochemical reactions leading to the formation of phenylnannolone A, the putative biosynthetic genes were identified (phn1, phn2). Phn2 is a polyketide synthase (PKS) with an NRPS-like loading module, and its domain order is consistent with the phenylnannolone A structure. The functionality and substrate selectivity of the loading module were determined by means of a γ-18O4-ATP pyrophosphate exchange and a phosphopantetheine ejection assay. A specific activation of cinnamic acid by the AMP-ligase was detected. Phn1 is a putative butyryl-CoA carboxylase (BCC), providing ethylmalonyl-CoA for the formation of the ethyl-substituted part of phenylnannolone A. Phn1 is the first BCC found in biosynthetic genes for an ethyl-substituted natural compound. Biosynthesis of phenylnannolone A, putatively encoded by phn1 and phn2, thus utilizes the first biosynthetic machinery in which both a BCC and a PKS are involved.

摘要

粘细菌菌株 Nannocystis pusilla B150 合成了结构新颖的聚酮类化合物苯基纳诺酮 A-C。除了一些常见的挥发性物质和铁载体外,这些是 Nannocystis 属的第一个天然产物。苯基纳诺酮 A 对 ABCB1 基因产物 P-糖蛋白具有抑制活性,并逆转癌细胞中的柔红霉素耐药性。为了解析导致苯基纳诺酮 A 形成的生化反应,鉴定了假定的生物合成基因(phn1、phn2)。Phn2 是一种具有 NRPS 样加载模块的聚酮合酶(PKS),其结构域顺序与苯基纳诺酮 A 的结构一致。通过 γ-18O4-ATP 焦磷酸交换和磷酸泛酰巯基乙胺排出测定,确定了加载模块的功能和底物选择性。检测到 AMP 连接酶对肉桂酸的特异性激活。Phn1 是一种假定的丁酰辅酶 A 羧化酶(BCC),为苯基纳诺酮 A 的乙基取代部分的形成提供乙基丙二酰辅酶 A。Phn1 是在乙基取代天然化合物生物合成基因中发现的第一个 BCC。苯基纳诺酮 A 的生物合成,推测由 phn1 和 phn2 编码,因此利用了第一个生物合成机制,其中涉及 BCC 和 PKS。

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