Cancer-associated fibroblast-specific lncRNA LINC01614 enhances glutamine uptake in lung adenocarcinoma

Tongyan Liu; Chencheng Han; Panqi Fang; Zhifei Ma; Xiaoxiao Wang; Hao Chen; Siwei Wang; Fanchen Meng; Cheng Wang; Erbao Zhang; Guozhang Dong; Hongyu Zhu; Wenda Yin; Jie Wang; Xianglin Zuo; Mantang Qiu; Jinke Wang; Qian Xu; Hongbing Shen; Lin Xu; Zhibin Hu; Rong Yin

doi:10.1186/s13045-022-01359-4

Cancer-associated fibroblast-specific lncRNA LINC01614 enhances glutamine uptake in lung adenocarcinoma

Tongyan Liu(Jiangsu Cancer Hospital), Chencheng Han(Jiangsu Cancer Hospital), Panqi Fang(Jiangsu Cancer Hospital), Zhifei Ma(Jiangsu Cancer Hospital), Xiaoxiao Wang(Nanjing University of Chinese Medicine), Hao Chen(Jiangsu Cancer Hospital), Siwei Wang(Jiangsu Cancer Hospital), Fanchen Meng(Jiangsu Cancer Hospital), Cheng Wang(Nanjing Medical University), Erbao Zhang(Nanjing Medical University), Guozhang Dong(Jiangsu Cancer Hospital), Hongyu Zhu(Jiangsu Cancer Hospital), Wenda Yin(Jiangsu Cancer Hospital), Jie Wang(Jiangsu Cancer Hospital), Xianglin Zuo(Jiangsu Cancer Hospital), Mantang Qiu(Peking University), Jinke Wang(Jiangsu Cancer Hospital), Qian Xu(Nanjing Medical University), Hongbing Shen(Nanjing Medical University), Lin Xu(Jiangsu Cancer Hospital), Zhibin Hu(Nanjing Medical University), Rong Yin(Università Campus Bio-Medico)

Journal of Hematology & Oncology

October 8, 2022

10.1186/s13045-022-01359-4

Cited by 181Open Access

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Abstract

BACKGROUND: Besides featured glucose consumption, recent studies reveal that cancer cells might prefer "addicting" specific energy substrates from the tumor microenvironment (TME); however, the underlying mechanisms remain unclear. METHODS: Fibroblast-specific long noncoding RNAs were screened using RNA-seq data of our NJLCC cohort, TCGA, and CCLE datasets. The expression and package of LINC01614 into exosomes were identified using flow cytometric sorting, fluorescence in situ hybridization (FISH), and quantitative reverse transcription polymerase chain reaction (RT-PCR). The transfer and functional role of LINC01614 in lung adenocarcinoma (LUAD) and CAFs were investigated using 4-thiouracil-labeled RNA transfer and gain- and loss-of-function approaches. RNA pull-down, RNA immunoprecipitation, dual-luciferase assay, gene expression microarray, and bioinformatics analysis were performed to investigate the underlying mechanisms involved. RESULTS: We demonstrate that cancer-associated fibroblasts (CAFs) in LUAD primarily enhance the glutamine metabolism of cancer cells. A CAF-specific long noncoding RNA, LINC01614, packaged by CAF-derived exosomes, mediates the enhancement of glutamine uptake in LUAD cells. Mechanistically, LINC01614 directly interacts with ANXA2 and p65 to facilitate the activation of NF-κB, which leads to the upregulation of the glutamine transporters SLC38A2 and SLC7A5 and eventually enhances the glutamine influx of cancer cells. Reciprocally, tumor-derived proinflammatory cytokines upregulate LINC01614 in CAFs, constituting a feedforward loop between CAFs and cancer cells. Blocking exosome-transmitted LINC01614 inhibits glutamine addiction and LUAD growth in vivo. Clinically, LINC01614 expression in CAFs is associated with the glutamine influx and poor prognosis of patients with LUAD. CONCLUSION: Our study highlights the therapeutic potential of targeting a CAF-specific lncRNA to inhibit glutamine utilization and cancer progression in LUAD.

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