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柱孢藻 T3 毒素谱的再评估及推测的磺基转移酶在合成硫酸盐化和磺化 PSP 毒素中的作用。

Reassessment of the toxin profile of Cylindrospermopsis raciborskii T3 and function of putative sulfotransferases in synthesis of sulfated and sulfonated PSP toxins.

机构信息

Pontificia Universidad Católica de Chile, Alameda 340, 6513492 Santiago, Chile.

出版信息

Toxicon. 2010 Dec;56(8):1350-61. doi: 10.1016/j.toxicon.2010.07.022. Epub 2010 Aug 6.

Abstract

The toxigenic freshwater cyanobacterium Cylindrospermopsis raciborskii T3 has been used as a model to study and elucidate the biosynthetic pathway of tetrahydropurine neurotoxins associated with paralytic shellfish poisoning (PSP). There are nevertheless several inconsistencies and contradictions in the toxin profile of this strain as published by different research groups, and claimed to include carbamoyl (STX, NEO, GTX2/3), decarbamoyl (dcSTX), and N-sulfocarbamoyl (C1/2, B1) derivatives. Our analysis of the complete genome of another PSP toxin-producing cyanobacterium, Raphidiopsis brookii D9, which is closely related to C. raciborskii T3, resolved many issues regarding the correlation between biosynthetic pathways, corresponding genes and the T3 toxin profile. The putative sxt gene cluster in R. brookii D9 has a high synteny with the T3 sxt cluster, with 100% nucleotide identity among the shared genes. We also compared the PSP toxin profile of the strains by liquid chromatography coupled to mass spectrometry (LC-MS/MS). In contrast to published reports, our reassessment of the PSP toxin profile of T3 confirmed production of only STX, NEO and dcNEO. We gained significant insights via correlation between specific sxt genes and their role in PSP toxin synthesis in both D9 and T3 strains. In particular, analysis of sulfotransferase functions for SxtN (N-sulfotransferase) and SxtSUL (O-sulfotransferase) enzymes allowed us to propose an extension of the PSP toxin biosynthetic pathway from STX to the production of the derivatives GTX2/3, C1/2 and B1. This is a significantly revised view of the genetic mechanisms underlying synthesis of sulfated and sulfonated STX analogues in toxigenic cyanobacteria.

摘要

产毒淡水蓝藻柱孢鱼腥藻 Cylindrospermopsis raciborskii T3 已被用作研究和阐明与麻痹性贝类中毒 (PSP) 相关的四氢嘌呤神经毒素生物合成途径的模型。然而,不同研究小组发表的该菌株的毒素特征存在一些不一致和矛盾之处,并声称包括氨甲酰基 (STX、NEO、GTX2/3)、脱氨甲酰基 (dcSTX) 和 N-磺酰氨甲酰基 (C1/2、B1) 衍生物。我们对另一种产麻痹性贝类毒素的蓝藻 Raphidiopsis brookii D9 的完整基因组进行了分析,该藻与 C. raciborskii T3 密切相关,解决了与生物合成途径、相应基因和 T3 毒素特征之间相关性相关的许多问题。R. brookii D9 中的假定 sxt 基因簇与 T3 sxt 簇具有高度同源性,共享基因之间的核苷酸同一性为 100%。我们还通过液相色谱-质谱联用 (LC-MS/MS) 比较了这些菌株的 PSP 毒素特征。与已发表的报告相反,我们对 T3 的 PSP 毒素特征的重新评估证实仅产生 STX、NEO 和 dcNEO。我们通过在 D9 和 T3 菌株中特定 sxt 基因与它们在 PSP 毒素合成中的作用之间的相关性获得了重要的见解。特别是,对 SxtN(N-磺基转移酶)和 SxtSUL(O-磺基转移酶)酶的磺基转移酶功能的分析使我们能够提出 PSP 毒素生物合成途径从 STX 扩展到 GTX2/3、C1/2 和 B1 衍生物的生产。这是对产毒蓝藻中合成磺化和磺化 STX 类似物的遗传机制的重大修订观点。

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