상세 보기
- Park, Seong Joon;
- Yoo, Hee Chan;
- Ahn, Eunyong;
- Luo, Enzhi;
- Kim, Yeabeen;
- 외 10명
WEB OF SCIENCE
48SCOPUS
51초록
Pancreatic ductal adenocarcinoma (PDAC) exhibits severe hyp-oxia, which is associated with chemoresistance and worse patient outcome. It has been reported that hypoxia induces metabolic reprogramming in cancer cells. However, it is not well known whether metabolic reprogramming contributes to hypoxia. Here, we established that increased glutamine catabolism is a fundamental mechanism inducing hypoxia, and thus chemoresistance, in PDAC cells. An extracellular matrix component-based in vitro three-dimensional cell printing model with patient-derived PDAC cells that recapitulate the hypoxic status in PDAC tumors showed that chemoresistant PDAC cells exhibit markedly enhanced glutamine catabolism compared with chemoresponsive PDAC cells. The augmented glutamine metabolic flux increased the oxygen con-sumption rate via mitochondrial oxidative phosphorylation (OXPHOS), promoting hypoxia and hypoxia-induced chemoresis-tance. Targeting glutaminolysis relieved hypoxia and improved chemotherapy efficacy in vitro and in vivo. This work suggests that targeting the glutaminolysis-OXPHOS-hypoxia axis is a novel therapeutic target for treating patients with chemoresistant PDAC. Significance: Increased glutaminolysis induces hypoxia via oxidative phosphorylation-mediated oxygen consumption and drives chemoresistance in pancreatic cancer, revealing a potential therapeutic strategy of combining glutaminolysis inhibition and chemotherapy to overcome resistance.
키워드
- 제목
- Enhanced Glutaminolysis Drives Hypoxia-Induced Chemoresistance in Pancreatic Cancer
- 저자
- Park, Seong Joon; Yoo, Hee Chan; Ahn, Eunyong; Luo, Enzhi; Kim, Yeabeen; Sung, Yulseung; Yu, Ya Chun; Kim, Kibum; Min, Do Sik; Lee, Hee Seung; Hwang, Geum Sook; Ahn, TaeJin; Choi, Junjeong; Bang, Seungmin; Han, Jung Min
- 발행일
- 2023-03
- 유형
- Article
- 저널명
- Cancer Research
- 권
- 83
- 호
- 5
- 페이지
- 735 ~ 752