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吲哚胺2,3-双加氧酶在恒河猴和普通狨猴中的表达。

Expression of indoleamine 2,3-dioxygenase in the rhesus monkey and common marmoset.

作者信息

Drenzek Jessica G, Breburda Edith E, Burleigh David W, Bondarenko Gennadiy I, Grendell Richard L, Golos Thaddeus G

机构信息

Wisconsin National Primate Research Center, University of Wisconsin-Madison, 1223 Capitol Court, Madison, WI 53715, USA.

出版信息

J Reprod Immunol. 2008 Jul;78(2):125-33. doi: 10.1016/j.jri.2008.03.005. Epub 2008 May 19.

Abstract

Indoleamine 2,3-dioxygenase (IDO) catalyzes the initial and rate-limiting step of tryptophan degradation along the kynurenine pathway, and is hypothesized to limit tryptophan availability at embryo implantation and prevent maternal T cell activation at the maternal-fetal interface. To determine if nonhuman primates are suitable models for investigating the role of IDO during pregnancy, we defined the expression of IDO in the rhesus monkey and common marmoset with particular attention to the female reproductive tract and placenta. IDO mRNA was detected by RT-PCR in the rhesus monkey term placenta, lung, small intestine, spleen, lymph node and nonpregnant uterus, and also in the common marmoset placenta. Immunohistochemical analysis of rhesus monkey tissues localized IDO to glandular epithelium of nonpregnant endometrium and first trimester decidua, vessel endothelium of nonpregnant myometrium, first trimester decidua and term decidua, and villous vessel endothelium and syncytiotrophoblast of term placenta. Western blot analysis confirmed IDO in rhesus monkey term placenta. In the common marmoset, IDO was detected in glandular epithelium of the nonpregnant uterus and in the decidua at day 60 and day 128 of gestation. IDO activity was higher in rhesus monkey and common marmoset decidua and placentas than in other tissues. Confirmation of IDO expression in rhesus monkey and common marmoset uterine and placental tissues supports the hypothesis that this enzyme regulates immune activation at the maternal-fetal interface and demonstrates that nonhuman primates may provide models with distinct similarities to human placentation to study the role of IDO in maternal-fetal immune dialogue.

摘要

吲哚胺2,3-双加氧酶(IDO)催化色氨酸沿犬尿氨酸途径降解的初始限速步骤,据推测它会限制胚胎着床时色氨酸的可利用性,并防止母胎界面处母体T细胞的激活。为了确定非人灵长类动物是否是研究IDO在妊娠期间作用的合适模型,我们确定了恒河猴和普通狨猴中IDO的表达,特别关注雌性生殖道和胎盘。通过RT-PCR在恒河猴足月胎盘、肺、小肠、脾脏、淋巴结和未孕子宫中检测到IDO mRNA,在普通狨猴胎盘中也检测到了该mRNA。对恒河猴组织的免疫组织化学分析将IDO定位到未孕子宫内膜和孕早期蜕膜的腺上皮、未孕子宫肌层、孕早期蜕膜和足月蜕膜的血管内皮,以及足月胎盘的绒毛血管内皮和合胞体滋养层。蛋白质印迹分析证实了恒河猴足月胎盘中存在IDO。在普通狨猴中,在未孕子宫的腺上皮以及妊娠60天和128天的蜕膜中检测到了IDO。恒河猴和普通狨猴蜕膜及胎盘中的IDO活性高于其他组织。恒河猴和普通狨猴子宫及胎盘组织中IDO表达的证实支持了这一假说,即该酶调节母胎界面处的免疫激活,并表明非人灵长类动物可能提供与人类胎盘形成有明显相似之处的模型,以研究IDO在母胎免疫对话中的作用。

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