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김지원 (Ji Won Kim)  |
제주대학교 약학대학 |
 150 KB CV updated 2022-11-11 08:59
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Capicua suppresses YAP1 to limit tumorigenesis and maintain drug sensitivity in human cancer
 Authors and Affiliations
 Authors and Affiliations
Ji Won Kim1,2, Cuyler Luck1, Wei Wu1, Rovingaile Kriska Ponce1, Yone Kawe Lin1, Nehal Gupta1, Ross A. Okimoto1,3,4
1Department of Medicine, University of California, San Francisco, San Francisco, CA, USA
2Jeju Research Institute of Pharmaceutical Sciences, College of Pharmacy, Jeju National University, Jeju, Republic of Korea
3Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, San Francisco, CA, USA
Corresponding author: Ross A Okimoto
Abstract Inactivation of Capicua (CIC) or upregulation of yes-associated protein 1, YAP1, leads to broad RAS-RAF-MEK-ERK inhibitor resistance and tumor progression in multiple human cancers. Despite these shared malignant phenotypes, it remains unclear whether CIC and YAP1 are mechanistically linked. Here, we show that the ERK-regulated transcription factor CIC can directly repress YAP1 expression through non-consensus GGAAGGAA DNA-binding motifs in a proximal YAP1 regulatory element. Through binding at GGAA repeats, CIC regulates YAP1 transcriptional output in both normal and human cancer cells. Silencing YAP1 in CIC-deficient cells restores MAPK inhibitor sensitivity and suppresses tumor growth. Thus, we uncover a molecular link between the MAPK-ERK effector CIC and YAP1 in human cells and established YAP inhibition as a strategy to target CIC-deficient cancers.
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관련 인터뷰 |
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1. 논문관련 분야의 소개, 동향, 전망을 설명, 연구과정에서 생긴 에피소드
이 논문에서는 전사억제인자인 Capicua (CIC)가 비소세포성폐암 (NSCLC)을 포함한 여러 인간의 고형암종에서 oncogenic한 기능을 보이는 YAP1 (Yes-Associated Protein 1) 유전자의 전사를 억제함을 최초로 확인하였습니다. CIC는 tumor suppressor gene으로 작용하며, CIC의 유전적 결핍이나 단백질 발현 이상에 의한 고형암의 전이... |
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먹뚜뚜 (2022-11-30 11:17) |
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