A functional single-cell metabolic survey identifies Elovl1 as a target to enhance CD8+ T cell fitness in solid tumours

IF 18.9 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Samantha Pretto, Qian Yu, Pierre Bourdely, Sarah Trusso Cafarello, Heleen H. Van Acker, Joren Verelst, Elena Richiardone, Lotte Vanheer, Amir Roshanzadeh, Franziska Schneppenheim, Charlotte Cresens, Maria Livia Sassano, Jonas Dehairs, Martin Carion, Shehab Ismail, Patrizia Agostinis, Susana Rocha, Tobias Bald, Johan Swinnen, Cyril Corbet, Sophia Y. Lunt, Bernard Thienpont, Mario Di Matteo, Massimiliano Mazzone
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Abstract

Reprogramming T cell metabolism can improve intratumoural fitness. By performing a CRISPR/Cas9 metabolic survey in CD8+ T cells, we identified 83 targets and we applied single-cell RNA sequencing to disclose transcriptome changes associated with each metabolic perturbation in the context of pancreatic cancer. This revealed elongation of very long-chain fatty acids protein 1 (Elovl1) as a metabolic target to sustain effector functions and memory phenotypes in CD8+ T cells. Accordingly, Elovl1 inactivation in adoptively transferred T cells combined with anti-PD-1 showed therapeutic efficacy in resistant pancreatic and melanoma tumours. The accumulation of saturated long-chain fatty acids in Elovl1-deficient T cells destabilized INSIG1, leading to SREBP2 activation, increased plasma membrane cholesterol and stronger T cell receptor signalling. Elovl1-deficient T cells increased mitochondrial fitness and fatty acid oxidation, thus withstanding the metabolic stress imposed by the tumour microenvironment. Finally, ELOVL1 in CD8+ T cells correlated with anti-PD-1 response in patients with melanoma. Altogether, Elovl1 targeting synergizes with anti-PD-1 to promote effective T cell responses. Through a functional CRISPR/Cas9 screening, Pretto et al. identify Elovl1 as a target to improve antitumour immunity by remodelling T cell lipid metabolism.

Abstract Image

Abstract Image

一项功能性单细胞代谢调查发现,Elovl1是实体肿瘤中增强CD8+ T细胞适应度的靶标
重编程T细胞代谢可以改善肿瘤内适应性。通过在CD8+ T细胞中进行CRISPR/Cas9代谢调查,我们确定了83个靶点,并应用单细胞RNA测序来揭示胰腺癌背景下与每种代谢扰动相关的转录组变化。这表明,在CD8+ T细胞中,超长链脂肪酸蛋白1 (Elovl1)的延长是维持效应功能和记忆表型的代谢靶点。因此,在过继转移的T细胞中,Elovl1失活联合抗pd -1显示出对耐药胰腺和黑色素瘤肿瘤的治疗效果。elovl1缺陷T细胞中饱和长链脂肪酸的积累破坏了INSIG1的稳定,导致SREBP2激活,质膜胆固醇升高,T细胞受体信号传导增强。缺乏elovl1的T细胞增加了线粒体适应性和脂肪酸氧化,从而承受了肿瘤微环境施加的代谢应激。最后,CD8+ T细胞中的ELOVL1与黑色素瘤患者的抗pd -1反应相关。总之,Elovl1靶向与抗pd -1协同促进有效的T细胞反应。
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来源期刊
Nature metabolism
Nature metabolism ENDOCRINOLOGY & METABOLISM-
CiteScore
27.50
自引率
2.40%
发文量
170
期刊介绍: Nature Metabolism is a peer-reviewed scientific journal that covers a broad range of topics in metabolism research. It aims to advance the understanding of metabolic and homeostatic processes at a cellular and physiological level. The journal publishes research from various fields, including fundamental cell biology, basic biomedical and translational research, and integrative physiology. It focuses on how cellular metabolism affects cellular function, the physiology and homeostasis of organs and tissues, and the regulation of organismal energy homeostasis. It also investigates the molecular pathophysiology of metabolic diseases such as diabetes and obesity, as well as their treatment. Nature Metabolism follows the standards of other Nature-branded journals, with a dedicated team of professional editors, rigorous peer-review process, high standards of copy-editing and production, swift publication, and editorial independence. The journal has a high impact factor, has a certain influence in the international area, and is deeply concerned and cited by the majority of scholars.
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