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从头多胺合成支持激活的小鼠自然杀伤细胞的代谢和功能反应。

De novo polyamine synthesis supports metabolic and functional responses in activated murine NK cells.

机构信息

School of Biochemistry and Immunology, Trinity Biomedical Sciences Institute, Trinity College Dublin, Dublin, Ireland.

Institute of Functional Genomics, University of Regensburg, Regensburg, Germany.

出版信息

Eur J Immunol. 2021 Jan;51(1):91-102. doi: 10.1002/eji.202048784. Epub 2020 Nov 9.

DOI:10.1002/eji.202048784
PMID:32946110
Abstract

Cellular metabolism is dynamically regulated in NK cells and strongly influences their responses. Metabolic dysfunction is linked to defective NK cell responses in diseases such as obesity and cancer. The transcription factors, sterol regulatory element binding protein (SREBP) and cMyc, are crucial for controlling NK cell metabolic and functional responses, though the mechanisms involved are not fully understood. This study reveals a new role for SREBP in NK cells in supporting de novo polyamine synthesis through facilitating elevated cMyc expression. Polyamines have diverse roles and their de novo synthesis is required for NK cell glycolytic and oxidative metabolism and to support optimal NK cell effector functions. When NK cells with impaired SREBP activity were supplemented with exogenous polyamines, NK cell metabolic defects were not rescued but these NK cells displayed significant improvement in some effector functions. One role for polyamines is in the control of protein translation where spermidine supports the posttranslational hypusination of translation factor eIF5a. Pharmacological inhibition of hypusination also impacts upon NK cell metabolism and effector function. Considering recent evidence that cholesterol-rich tumor microenvironments inhibit SREBP activation and drive lymphocyte dysfunction, this study provides key mechanistic insight into this tumor-evasion strategy.

摘要

细胞代谢在 NK 细胞中是动态调节的,强烈影响其反应。代谢功能障碍与肥胖和癌症等疾病中 NK 细胞反应缺陷有关。转录因子固醇调节元件结合蛋白 (SREBP) 和 cMyc 对于控制 NK 细胞代谢和功能反应至关重要,尽管涉及的机制尚不完全清楚。本研究揭示了 SREBP 在 NK 细胞中的一个新作用,即通过促进 cMyc 表达的升高来支持从头多胺合成。多胺具有多种作用,其从头合成对于 NK 细胞糖酵解和氧化代谢以及支持最佳 NK 细胞效应功能是必需的。当 SREBP 活性受损的 NK 细胞补充外源性多胺时,NK 细胞的代谢缺陷并未得到挽救,但这些 NK 细胞在一些效应功能上显示出显著改善。多胺的一个作用是控制蛋白质翻译,其中 spermidine 支持翻译因子 eIF5a 的翻译后 hypusination。hypusination 的药理学抑制也会影响 NK 细胞代谢和效应功能。考虑到最近的证据表明富含胆固醇的肿瘤微环境抑制 SREBP 激活并导致淋巴细胞功能障碍,本研究为这种肿瘤逃避策略提供了关键的机制见解。

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