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吡咯里西啶生物碱在肝脏微粒体酶代谢中的种属差异。

Species differences in the hepatic microsomal enzyme metabolism of the pyrrolizidine alkaloids.

作者信息

Huan J Y, Miranda C L, Buhler D R, Cheeke P R

机构信息

Toxicology Program, Oregon State University, Corvallis 97311, USA.

出版信息

Toxicol Lett. 1998 Oct 15;99(2):127-37. doi: 10.1016/s0378-4274(98)00152-0.

Abstract

Species differences in pyrrolic metabolites and senecionine (SN) N-oxide formation among eight animal species (sheep, cattle, gerbils, rabbits, hamsters, Japanese quail, chickens, rats) varying in susceptibility to pyrrolizidine alkaloid (PA) intoxication were measured in vitro by hepatic microsomal incubations. The results suggested that there is not a strong correlation between the production of pyrrolic metabolites and susceptibility of animals to PA toxicity. The rate of PA activation in hamsters, a resistant species, measured by formation of (+/-)6,7-dihydro-7-hydroxy-1-hydroxymethyl-5H-pyrrolizine (DHP) far exceeded the rate of SN N-oxide formation (detoxification) (DHP/N-oxide = 2.29). In contrast, SN N-oxide was the major metabolite in sheep, another resistant species, with much lower production of DHP (DHP/N-oxide = 0.26). The roles of cytochrome P450s and flavin-containing monooxygenases (FMO) in bioactivation and detoxification of pyrrolizidine alkaloids (PA) were studied in vitro using sheep and hamster hepatic microsomes. Chemical and immunochemical inhibition data suggested that the conversion of SN to DHP is catalyzed mainly by cytochrome P450s (68-82%), whereas the formation of SN N-oxide is carried out largely by FMO (55-71%). There also appeared to be a high rate of glutathione-DHP conjugation in hamster (63%) and sheep (79%) liver microsomal incubation mixtures. Therefore, low rates of pyrrole metabolite production coupled with glutathione conjugation in sheep may explain the resistance of sheep to SN, whereas the high rate of GSH-DHP conjugation may be one of the factors contributing to the resistance of hamsters to intoxication by this PA.

摘要

通过肝微粒体体外孵育,测定了八种对吡咯里西啶生物碱(PA)中毒敏感性不同的动物物种(绵羊、牛、沙鼠、兔子、仓鼠、日本鹌鹑、鸡、大鼠)中吡咯代谢产物和千里光碱(SN)N - 氧化物形成的物种差异。结果表明,吡咯代谢产物的产生与动物对PA毒性的敏感性之间没有很强的相关性。通过(±)6,7 - 二氢 - 7 - 羟基 - 1 - 羟甲基 - 5H - 吡咯里嗪(DHP)的形成来衡量,抗性物种仓鼠中PA的活化速率远远超过SN N - 氧化物形成(解毒)的速率(DHP/N - 氧化物 = 2.29)。相比之下,SN N - 氧化物是另一个抗性物种绵羊中的主要代谢产物,DHP的产生量要低得多(DHP/N - 氧化物 = 0.26)。利用绵羊和仓鼠的肝微粒体在体外研究了细胞色素P450和含黄素单加氧酶(FMO)在吡咯里西啶生物碱(PA)生物活化和解毒中的作用。化学和免疫化学抑制数据表明,SN向DHP的转化主要由细胞色素P450催化(68 - 82%),而SN N - 氧化物的形成主要由FMO进行(55 - 71%)。在仓鼠(63%)和绵羊(79%)肝微粒体孵育混合物中,谷胱甘肽 - DHP结合率似乎也很高。因此,绵羊中吡咯代谢产物产生率低以及谷胱甘肽结合可能解释了绵羊对SN的抗性,而高GSH - DHP结合率可能是仓鼠对这种PA中毒具有抗性的因素之一。

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