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Literature DB >> 35449308

Therapeutic targeting of the mevalonate-geranylgeranyl diphosphate pathway with statins overcomes chemotherapy resistance in small cell lung cancer.

Chenchen Guo^1,2, Ruijie Wan^1,2, Yayi He³, Shu-Hai Lin⁴, Jiayu Cao^1,2, Ying Qiu^1,2, Tengfei Zhang^1,2, Qiqi Zhao^1,2,5, Yujia Niu⁴, Yujuan Jin¹, Hsin-Yi Huang¹, Xue Wang¹, Li Tan⁶, Roman K Thomas^7,8,9, Hua Zhang¹⁰, Luonan Chen^1,2,5, Kwok-Kin Wong¹⁰, Liang Hu¹¹, Hongbin Ji^12,13,14,15.

Abstract

Small cell lung cancer (SCLC) lacks effective treatments to overcome chemoresistance. Here we established multiple human chemoresistant xenograft models through long-term intermittent chemotherapy, mimicking clinically relevant therapeutic settings. We show that chemoresistant SCLC undergoes metabolic reprogramming relying on the mevalonate (MVA)-geranylgeranyl diphosphate (GGPP) pathway, which can be targeted using clinically approved statins. Mechanistically, statins induce oxidative stress accumulation and apoptosis through the GGPP synthase 1 (GGPS1)-RAB7A-autophagy axis. Statin treatment overcomes both intrinsic and acquired SCLC chemoresistance in vivo across different SCLC PDX models bearing high GGPS1 levels. Moreover, we show that GGPS1 expression is negatively associated with survival in patients with SCLC. Finally, we demonstrate that combined statin and chemotherapy treatment resulted in durable responses in three patients with SCLC who relapsed from first-line chemotherapy. Collectively, these data uncover the MVA-GGPP pathway as a metabolic vulnerability in SCLC and identify statins as a potentially effective treatment to overcome chemoresistance.

Entities: Chemical

Mesh：

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Year: 2022 PMID： 35449308 DOI： 10.1038/s43018-022-00358-1

Source DB: PubMed Journal: Nat Cancer ISSN： 2662-1347

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