Characterization of the kynurenine pathway and quinolinic Acid production in macaque macrophages.

IF 2.7 Q3 NEUROSCIENCES

International Journal of Tryptophan Research Pub Date : 2013-05-15 Print Date: 2013-01-01 DOI:10.4137/IJTR.S11789

Chai K Lim, Margaret M C Yap, Stephen J Kent, Gabriel Gras, Boubekeur Samah, Jane C Batten, Robert De Rose, Benjamin Heng, Bruce J Brew, Gilles J Guillemin

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引用次数: 23

Abstract

The kynurenine pathway (KP) and one of its end-products, the excitotoxin quinolinic acid (QUIN), are involved in the pathogenesis of several major neuroinflammatory brain diseases. A relevant animal model to study KP metabolism is now needed to assess whether intervention in this pathway may improve the outcome of such diseases. Humans and macaques share a very similar genetic makeup. In this study, we characterized the KP metabolism in macaque primary macrophages of three different species in comparison to human cells. We found that the KP profiles in simian macrophages were very similar to those in humans when challenged with inflammatory cytokines. Further, we found that macaque macrophages are capable of producing a pathophysiological concentration of QUIN. Our data validate the simian model as a relevant model to study the human cellular KP metabolism in the context of inflammation.

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猕猴巨噬细胞犬尿氨酸途径和喹啉酸生成的表征。

犬尿氨酸途径(KP)及其最终产物之一兴奋毒素喹啉酸(QUIN)参与了几种主要的神经炎性脑疾病的发病机制。现在需要一个相关的动物模型来研究KP代谢，以评估干预这一途径是否可以改善此类疾病的预后。人类和猕猴有着非常相似的基因组成。在这项研究中，我们表征了三种不同种类猕猴原代巨噬细胞与人类细胞的KP代谢。我们发现，当受到炎症细胞因子的攻击时，猿类巨噬细胞的KP谱与人类非常相似。此外，我们发现猕猴巨噬细胞能够产生QUIN的病理生理浓度。我们的数据验证了类人猿模型作为研究炎症背景下人类细胞KP代谢的相关模型。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

International Journal of Tryptophan Research NEUROSCIENCES-

CiteScore

7.30

自引率

4.50%

发文量

审稿时长

8 weeks