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qMSI 凸显的肿瘤微环境代谢相互作用:在免疫肿瘤学中色氨酸-犬尿氨酸途径的应用。

Microenvironment Tumor Metabolic Interactions Highlighted by qMSI: Application to the Tryptophan-Kynurenine Pathway in Immuno-Oncology.

机构信息

1 ImaBiotech, Lille, France.

2 iTeos Therapeutics SA, Gosselies, Belgium.

出版信息

SLAS Discov. 2017 Dec;22(10):1182-1192. doi: 10.1177/2472555217712659. Epub 2017 May 30.

DOI:10.1177/2472555217712659
PMID:28557618
Abstract

Inhibition of NK and effector T-cell functions and activation of regulatory cell populations are the main immunosuppressive effects of indoleamine-2,3-dioxygenase1 (IDO1). By converting tryptophan (Trp) into kynurenine (Kyn), IDO1 is involved in the immune response homeostasis, and its dysregulated expression is described in immune-related pathologies, as tumors that hijack it to evade immune destruction. Thereby, IDO1 inhibitors are being developed to stimulate antitumor immune responses. Existing and standard quantitation methods of IDO1 substrate and metabolite(s) are based on the total level of Trp and its metabolites determined by liquid chromatography tandem mass spectrometry analysis in human plasma, cerebrospinal fluid, and brain. Here, we describe the detection, localization, and absolute quantitation of Trp and Kyn by quantitative mass spectrometry imaging (qMSI) in transfected murine tumor models expressing various levels of IDO1. Myeloid, glycolysis metabolic signatures, and correlation between IDO1 expression and Trp to Kyn conversion are also shown. High-definition IDO1 and GCN2 immunostainings overlaid with Kyn molecular images underline the tumor metabolism and heterogeneity. The development of immunotherapies such as IDO1 inhibitors requires a deep understanding of the immune system, the interplay of cancer cells, and biomarker characterization. Our data underline that qMSI allows the study of the spatial distribution and quantitation of endogenous immune metabolites for biology and pharmacology studies.

摘要

吲哚胺 2,3-双加氧酶 1(IDO1)的主要免疫抑制作用是抑制 NK 和效应 T 细胞的功能以及激活调节性细胞群体。通过将色氨酸(Trp)转化为犬尿氨酸(Kyn),IDO1 参与免疫反应的动态平衡,其表达失调在免疫相关疾病中有所描述,如肿瘤利用其逃避免疫破坏。因此,正在开发 IDO1 抑制剂以刺激抗肿瘤免疫反应。IDO1 底物和代谢物的现有和标准定量方法基于液相色谱串联质谱分析在人血浆、脑脊液和大脑中测定的总 Trp 及其代谢物水平。在这里,我们描述了通过转染表达不同 IDO1 水平的鼠肿瘤模型的定量质谱成像(qMSI)对 Trp 和 Kyn 的检测、定位和绝对定量。还显示了髓样细胞、糖酵解代谢特征以及 IDO1 表达与 Trp 向 Kyn 转化之间的相关性。IDO1 和 GCN2 免疫染色与 Kyn 分子图像叠加突出了肿瘤代谢和异质性。IDO1 抑制剂等免疫疗法的发展需要深入了解免疫系统、癌细胞的相互作用以及生物标志物特征。我们的数据强调了 qMSI 允许研究内源性免疫代谢物的空间分布和定量,以进行生物学和药理学研究。

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