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Human microglia convert l-tryptophan into the neurotoxin quinolinic acid.

机译:人小胶质细胞将L-色氨酸转化为神经毒素喹啉酸。

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摘要

Immune activation leads to accumulations of the neurotoxin and kynurenine pathway metabolite quinolinic acid within the central nervous system of human patients. Whereas macrophages can convert L-tryptophan to quinolinic acid, it is not known whether human brain microglia can synthesize quinolinic acid. Human microglia, peripheral blood macrophages and cultures of human fetal brain cells (astrocytes and neurons) were incubated with [13C6]L-tryptophan in the absence or presence of interferon gamma. [13C6]Quinolinic acid was identified and quantified by gas chromatography and electron-capture negative-chemical ionization mass spectrometry. Both L-kynurenine and [13C6]quinolinic acid were produced by unstimulated cultures of microglia and macrophages. Interferon gamma, an inducer of indoleamine 2,3-dioxygenase, increased the accumulation of L-kynurenine by all three cell types (to more than 40 microM). Whereas large quantities of [13C6]quinolinic acid were produced by microglia and macrophages (to 438 and 1410 nM respectively), minute quantities of [13C6]quinolinic acid were produced in human fetal brain cultures (not more than 2 nM). Activated microglia and macrophage infiltrates into the brain might be an important source of accelerated conversion of L-tryptophan into quinolinic acid within the central nervous system in inflammatory diseases.
机译:免疫激活导致人类患者中枢神经系统内神经毒素和犬尿氨酸途径代谢物喹啉酸的积累。尽管巨噬细胞可以将L-色氨酸转化为喹啉酸,但人脑小胶质细胞是否可以合成喹啉酸尚不清楚。在不存在或存在干扰素γ的情况下,将人类小胶质细胞,外周血巨噬细胞和人类胎儿脑细胞(星形细胞和神经元)培养物与[13C6] L-色氨酸一起孵育。 [13C6]喹啉酸通过气相色谱和电子捕获负化学电离质谱法鉴定和定量。 L-犬尿氨酸和[13C6]喹啉酸都是由无刺激的小胶质细胞和巨噬细胞培养产生的。吲哚胺2,3-二加氧酶的诱导剂干扰素γ通过所有三种细胞类型均增加了L-犬尿氨酸的积累(超过40 microM)。小胶质细胞和巨噬细胞产生大量的[13C6]喹啉酸(分别达到438和1410 nM),而人胎脑培养物中产生的微量[13C6]喹啉酸(不超过2 nM)。活化的小胶质细胞和巨噬细胞浸润进入大脑可能是炎症疾病中中枢神经系统内L-色氨酸加速转化为喹啉酸的重要来源。

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