Domingo-Vidal Marina, Whitaker-Menezes Diana, Mollaee Mehri, Lin Zhao, Tuluc Madalina, Philp Nancy, Johnson Jennifer M, Zhan Tingting, Curry Joseph, Martinez-Outschoorn Ubaldo
Sidney Kimmel Cancer Center, Department of Medical Oncology, Thomas Jefferson University, Philadelphia, PA, United States.
Lewis Katz School of Medicine, Department of Pathology and Laboratory Medicine, Temple University, Philadelphia, PA, United States.
Front Oncol. 2022 Jun 22;12:906494. doi: 10.3389/fonc.2022.906494. eCollection 2022.
The most common cancers of the aerodigestive tract (ADT) are non-small cell lung cancer (NSCLC) and head and neck squamous cell carcinoma (HNSCC). The tumor stroma plays an important role in ADT cancer development and progression, and contributes to the metabolic heterogeneity of tumors. Cancer-associated fibroblasts (CAFs) are the most abundant cell type in the tumor stroma of ADT cancers and exert pro-tumorigenic functions. Metabolically, glycolytic CAFs support the energy needs of oxidative (OXPHOS) carcinoma cells. Upregulation of the monocarboxylate transporter 4 (MCT4) and downregulation of isocitrate dehydrogenase 3α (IDH3α) are markers of glycolysis in CAFs, and upregulation of the monocarboxylate transporter 1 (MCT1) and the translocase of the outer mitochondrial membrane 20 (TOMM20) are markers of OXPHOS in carcinoma cells. It is unknown if glycolytic metabolism in CAFs is a driver of ADT cancer aggressiveness. In this study, co-cultures and co-injections in mice of ADT carcinoma cells with fibroblasts were used as experimental models to study the effects of fibroblasts on metabolic compartmentalization, oxidative stress, carcinoma cell proliferation and apoptosis, and overall tumor growth. Glycolytic metabolism in fibroblasts was modulated using the HIF-1α inhibitor BAY 87-2243, the antioxidant N-acetyl cysteine, and genetic depletion of MCT4. We found that ADT human tumors express markers of metabolic compartmentalization and that co-culture models of ADT cancers recapitulate human metabolic compartmentalization, have high levels of oxidative stress, and promote carcinoma cell proliferation and survival. In these models, BAY 87-2243 rescues IDH3α expression and NAC reduces MCT4 expression in fibroblasts, and these treatments decrease ADT carcinoma cell proliferation and increase cell death. Genetic depletion of fibroblast MCT4 decreases proliferation and survival of ADT carcinoma cells in co-culture. Moreover, co-injection of ADT carcinoma cells with fibroblasts lacking MCT4 reduces tumor growth and decreases the expression of markers of metabolic compartmentalization in tumors. In conclusion, metabolic compartmentalization with high expression of MCT4 in CAFs drives aggressiveness in ADT cancers.
气道消化道(ADT)最常见的癌症是非小细胞肺癌(NSCLC)和头颈部鳞状细胞癌(HNSCC)。肿瘤基质在ADT癌症的发生和发展中起重要作用,并导致肿瘤的代谢异质性。癌症相关成纤维细胞(CAFs)是ADT癌症肿瘤基质中最丰富的细胞类型,并发挥促肿瘤功能。在代谢方面,糖酵解型CAFs支持氧化磷酸化(OXPHOS)癌细胞的能量需求。单羧酸转运蛋白4(MCT4)的上调和异柠檬酸脱氢酶3α(IDH3α)的下调是CAFs中糖酵解的标志物,单羧酸转运蛋白1(MCT1)和线粒体外膜转位酶20(TOMM20)的上调是癌细胞中OXPHOS的标志物。尚不清楚CAFs中的糖酵解代谢是否是ADT癌症侵袭性的驱动因素。在本研究中,将ADT癌细胞与成纤维细胞在小鼠中的共培养和共注射用作实验模型,以研究成纤维细胞对代谢区室化、氧化应激、癌细胞增殖和凋亡以及整体肿瘤生长的影响。使用缺氧诱导因子-1α抑制剂BAY 87-2243、抗氧化剂N-乙酰半胱氨酸和MCT4的基因敲除来调节成纤维细胞中的糖酵解代谢。我们发现ADT人类肿瘤表达代谢区室化的标志物,并且ADT癌症的共培养模型概括了人类代谢区室化,具有高水平的氧化应激,并促进癌细胞增殖和存活。在这些模型中,BAY 87-2243挽救了成纤维细胞中IDH3α的表达,NAC降低了MCT4的表达,并且这些处理降低了ADT癌细胞的增殖并增加了细胞死亡。成纤维细胞MCT4的基因敲除降低了共培养中ADT癌细胞的增殖和存活。此外,将ADT癌细胞与缺乏MCT4的成纤维细胞共注射可减少肿瘤生长并降低肿瘤中代谢区室化标志物的表达。总之,CAFs中高表达MCT4的代谢区室化驱动了ADT癌症的侵袭性。
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