Filgotinib inhibits METTL3-mediated m6A of EIF3A by targeting ERG-TBP to suppress PDAC progression JAK-STAT3-independently
Zhang Chaolei, Ren Jianghao, Qiao Kexiong, Xu Chengjie, Pu Xiaofan, Chen Zongrong, Zhou Liangjing, Cao Liping, Jia Shengnan
Journal:npj Precision Oncology
IF:8
DOI:10.1038/s41698-026-01396-z
PMID:
Published:2026-04-01
research field:肿瘤学分子生物学癌症治疗学RNA生物学表观遗传学
Abstract
Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive tumor. EIF3A has been identified as a reader of N6-methyladenosine (m 6 A) modification, influencing the translation levels of various molecules and functioning as an oncogene. Our study presents novel findings demonstrating that the m 6 A of EIF3A, regulated by METTL3, influences the stability of EIF3A mRNA and its protein expression, ultimately impacting the progression of PDAC. Notably, through high-throughput drug screening targeting m 6 A of EIF3A, we identified filgotinib—a commercially rheumatism drug, Janus kinase (JAK) -STAT3 inhibitor—as an effective inhibitor of PDAC proliferation. Filgotinib increased DNA damage in PDAC cells via the ERG-TBP-METTL3-m 6 A-EIF3A axis. In contrast, other JAK-STAT3 inhibitors such as ruxolitinib and knockdown of STAT3 does not replicate this effect, indicating that the anti-tumor effect of filgotinib is independent of JAK-STAT3 signaling. This study offers innovative insights and potential therapeutic strategies for the treatment of PDAC through EIF3A m 6 A.
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