Cryptococcosis, tuberculosis, and a kidney cancer fail to fit the atherosclerosis paradigm for foam cell lipid content.

Valentina Guerrini, Brendan Prideaux, Rehan Khan, Selvakumar Subbian, Yina Wang, Evita Sadimin, Siddhi Pawar, Rahul Ukey, Eric A Singer, Chaoyang Xue, Maria Laura Gennaro
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Abstract

Foam cells are dysfunctional, lipid-laden macrophages associated with chronic inflammation of diverse origin. The long-standing paradigm that foam cells are cholesterol-laden derives from atherosclerosis research. We previously showed that, in tuberculosis, foam cells surprisingly accumulate triglycerides. Here, we utilized bacterial ( Mycobacterium tuberculosis ), fungal ( Cryptococcus neoformans ), and human papillary renal cell carcinoma (pRCC) models to address the need for a new explanation of foam cell biogenesis. We applied mass spectrometry-based imaging to assess the spatial distribution of storage lipids relative to foam-cell-rich areas in lesional tissues, and we characterized lipid-laden macrophages generated under corresponding in vitro conditions. The in vivo data and the in vitro findings showed that cryptococcus-infected macrophages accumulate triglycerides, while macrophages exposed to pRCC- conditioned-medium accumulated both triglycerides and cholesterol. Moreover, cryptococcus- and mycobacterium-infected macrophages accumulated triglycerides in different ways. Collectively, the data show that the molecular events underlying foam cell formation are specific to disease and microenvironment. Since foam cells are potential therapeutic targets, recognizing that their formation is disease-specific opens new biomedical research directions.

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疾病间泡沫细胞生物发生的异质性。
泡沫细胞是功能失调的、富含脂质的巨噬细胞,与传染性和非传染性的慢性炎症有关。几十年来,泡沫细胞生物学的基本模式一直建立在动脉粥样硬化的基础上,动脉粥样硬化是一种巨噬细胞富含胆固醇的疾病。我们之前的研究表明,结核性肺部病变中的泡沫细胞意外地积累甘油三酯,这表明泡沫细胞的生物发生有多种方式。在本研究中,我们使用基质辅助激光解吸/电离质谱成像来评估在感染真菌病原体新型隐球菌的小鼠肺部和人类乳头状肾细胞癌切除组织中储存脂质相对于泡沫细胞富集区域的空间分布。我们还分析了中性脂质含量和在相应的体外条件下产生的脂质巨噬细胞的转录程序。体内数据与体外研究结果一致,表明新生隐球菌感染的巨噬细胞积累甘油三酯,而暴露于人类肾癌条件培养基的巨噬细胞同时积累甘油三酯和胆固醇。此外,巨噬细胞转录组分析为条件特异性代谢重塑提供了证据。体外数据还表明,尽管结核分枝杆菌和新生隐球菌感染都诱导巨噬细胞中甘油三酯积聚,但它们是通过不同的分子机制引起的,脂质积聚对雷帕霉素药物的敏感性不同以及巨噬细胞转录组重塑的特征就证明了这一点。总之,这些数据表明,泡沫细胞形成的机制是特定于疾病微环境的。由于泡沫细胞已被视为几种疾病的药物干预靶点,认识到它们的形成是疾病特异性的,开辟了具有生物医学意义的新的研究方向。
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