• 主题
高级搜索  >
历史搜索 清空历史
首页> 外文期刊>Toxicon: An International Journal Devoted to the Exchange of Knowledge on the Poisons Derived from Animals, Plants and Microorganisms >Evidence of in vitro glucuronidation and enzymatic transformation of paralytic shellfish toxins by healthy human liver microsomes fraction.
【24h】

Evidence of in vitro glucuronidation and enzymatic transformation of paralytic shellfish toxins by healthy human liver microsomes fraction.

机译:健康人肝微粒体对麻痹性贝类毒素进行体外葡萄糖苷酸化和酶促转化的证据。

获取原文
获取原文并翻译 | 示例
       
页面导航
  • 摘要
  • 著录项
  • 相似文献
  • 相关主题

摘要

Paralytic Shellfish Toxins (PST) are endemic components found in filter bivalves in Southern Chile. Post-mortems analysis of fluid and tissue samples has shown biotransformation of PST in humans. The Gonyautoxin 3 (GTX3) and Gonyautoxin 2 (GTX2) are the major PST components in the toxin profile found in Chilean shellfish extracts, being as much as 65% of the total content of PST in filter bivalves. Therefore, they are the major accountable components of the human intoxication by shellfish consumption. The aim of this study is to show in vitro glucuronidation and biotransformation of GTX3 and GTX2 when they are incubated with microsomal fraction isolated from healthy human livers. Microsomes fractions isolated from human livers were incubated with GTX3 and GTX2 purified from contaminated mussels. After different incubation times, incubated samples were extracted and analyzed by HPLC with fluorescent on line detection and HPLC-MS analysis. The results revealed that GTX3 and GTX2, only when they were incubated with microsomal fraction and appropriated cofactors, showed to be enzymatic transformed in vitro. The glucuronidation of GTX3 and GTX2 followed typical Michaelis-Menten kinetics, resulting in apparent kinetic parameters of Km=39.4+or-0.24 micro M and Vmax=6.0x10-3 pmol/min/mg protein. In addition, the microsomes fraction also oxidized GTX3 and GTX2 into Gonyautoxin 4 (GTX 4) and Gonyautoxin 1 (GTX 1) resulting in 0.339x10-3 pmol/min/mg protein. In conclusion, this study reports oxidation and glucuronidation of GTX3 and GTX2 when they are incubated with human liver microsomal fraction. The metabolism occurs via a glucuronidation reaction, the basis first step of biotransformation in human liver. Also it is showed that GTX4 and GTX1 came by biotransformation from GTX3 and GTX2 in humans. This data confirm human biotransformation found in human post-mortem fluid and tissue samples described previously. This data is the first evidence of in vitro glucuronidation of PST, given a metabolic pathway of detoxification and excretion of PST in human.
机译:麻痹性贝类毒素(PST)是智利南部双过滤器中的特有成分。体液和组织样本的验尸分析显示,人体中PST发生了生物转化。 Gonyautoxin 3(GTX3)和Gonyautoxin 2(GTX2)是智利贝类提取物中毒素谱中主要的PST成分,占滤嘴双壳类中PST总含量的65%。因此,它们是食用贝类引起人中毒的主要责任成分。这项研究的目的是显示将GTX3和GTX2与从健康人肝中分离出的微粒体一起孵育后的体外葡萄糖醛酸苷化和生物转化。从人肝脏分离的微粒体级分与从受污染的贻贝纯化的GTX3和GTX2孵育。在不同的温育时间之后,提取温育的样品并通过具有在线荧光检测和HPLC-MS分析的HPLC进行分析。结果表明,仅当它们与微粒体级分和适当的辅因子一起孵育时,GTX3和GTX2才显示出是酶转化的体外。 GTX3和GTX2的葡糖醛酸化遵循典型的Michaelis-Menten动力学,导致表观动力学参数为 K m = 39.4 +或-0.24 micro M和 V max = 6.0x10 -3 pmol / min / mg蛋白。此外,微粒体级分还将GTX3和GTX2氧化为Gonyautoxin 4(GTX 4)和Gonyautoxin 1(GTX 1),得到0.339x10 -3 pmol / min / mg蛋白。总而言之,这项研究报告了将GTX3和GTX2与人肝微粒体温育后的氧化和葡萄糖醛酸化作用。代谢通过葡萄糖醛酸化反应发生,这是人类肝脏中生物转化的第一步。还表明GTX4和GTX1是通过人中GTX3和GTX2的生物转化而来的。该数据证实了在先前描述的人类尸体液体和组织样本中发现的人类生物转化。考虑到人体内PST的解毒和排泄的代谢途径,该数据是PST体外葡萄糖醛酸化的第一个证据。

著录项

相似文献

  • 外文文献
  • 中文文献
  • 专利
获取原文

客服邮箱:kefu@zhangqiaokeyan.com

京公网安备:11010802029741号 ICP备案号:京ICP备15016152号-6 六维联合信息科技 (北京) 有限公司©版权所有

  • 客服微信

  • 服务号