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Influence of Tryptophan Contained in 1-Methyl-Tryptophan on Antimicrobial and Immunoregulatory Functions of Indoleamine 23-Dioxygenase

机译:中所含的1-甲基色氨酸色氨酸的影响关于抗菌和吲哚胺23双加氧酶的免疫调节功能

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摘要

Indoleamine 2,3-dioxygenase (IDO) has been identified as an important antimicrobial and immunoregulatory effector molecule essential for the establishment of tolerance by regulating local tryptophan (Trp) concentrations. On the other hand, the immunosuppressive capacity of IDO can have detrimental effects for the host as it can lead to deleterious alterations of the immune response by promoting tolerance to some types of tumors. To suppress this disadvantageous IDO effect, the competitive inhibitor 1-Methyl-Tryptophan (1-MT) is being tested in clinical trials. However, it remains inconclusive which stereoisomer of 1-MT is the more effective inhibitor of IDO-mediated immunosuppression. While IDO enzyme activity is more efficiently inhibited by 1-L-MT in cell-free or in vitro settings, 1-D-MT is superior to 1-L-MT in the enhancement of anti-tumor responses in vivo.Here, we present new data showing that commercially available 1-L-MT lots contain tryptophan in amounts sufficient to compensate for the IDO-mediated tryptophan depletion in vitro. The addition of 1-L-MT abrogated IDO-mediated antimicrobial effects and permitted the growth of the tryptophan-auxotroph microorganisms Staphylococcus aureus and Toxoplasma gondii. Consistent with this, the tryptophan within 1-L-MT lots was sufficient to antagonize IDO-mediated inhibition of T cell responses. Mass spectrometry (MS) analysis revealed not only tryptophan within 1-L-MT, but also the incorporation of this tryptophan in bacterial and human proteins that were generated in the presence of 1-L-MT in otherwise tryptophan-free conditions. In summary, these data reveal that tryptophan within 1-L-MT can affect the results of in vitro studies in an L-stereospecific and IDO-independent way.
机译:吲哚胺2,3-二加氧酶(IDO)已被确认为重要的抗微生物和免疫调节效应分子,通过调节局部色氨酸(Trp)浓度来建立耐受性。另一方面,IDO的免疫抑制能力可能会对宿主产生不利影响,因为它可能通过增强对某些类型肿瘤的耐受性而导致免疫反应的有害改变。为了抑制这种不利的IDO效应,正在临床试验中测试竞争性抑制剂1-甲基色氨酸(1-MT)。但是,尚不确定1-MT的哪种立体异构体是IDO介导的免疫抑制的更有效抑制剂。在无细胞或体外条件下,1-L-MT可以更有效地抑制IDO酶的活性,但是1-D-MT在增强体内抗肿瘤反应方面优于1-L-MT。目前的新数据表明,市售的1-L-MT批次所含色氨酸的量足以补偿体外IDO介导的色氨酸消耗。 1-L-MT的添加消除了IDO介导的抗菌作用,并允许色氨酸营养缺陷型微生物金黄色葡萄球菌和弓形虫的生长。与此相一致,1-L-MT批次中的色氨酸足以拮抗IDO介导的T细胞应答抑制作用。质谱(MS)分析不仅显示了1-L-MT中的色氨酸,而且还将该色氨酸掺入了细菌和人的蛋白质中,而细菌和人蛋白质则是在1-L-MT存在下在无色氨酸的条件下生成的。总之,这些数据表明1-L-MT中的色氨酸可以以L-立体特异性和IDO独立的方式影响体外研究的结果。

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