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M6A-modified lncRNA FAM83H-AS1 promotes colorectal cancer progression through PTBP1

Xiaojing Luo, Yun‐Xin Lu, Yun Wang, Runjie Huang, Jia Liu, Ying Jin, Ze-Kun Liu, Zexian Liu, Qitao Huang, Heng‐Ying Pu, Zhao-Lei Zeng, Rui‐Hua Xu, Qi Zhao, Qi‐Nian Wu

2024Cancer Letters24 citationsDOIOpen Access PDF

Abstract

LncRNA plays a crucial role in cancer progression and targeting, but it has been difficult to identify the critical lncRNAs involved in colorectal cancer (CRC) progression. We identified FAM83H-AS1 as a tumor-promoting associated lncRNA using 21 pairs of stage IV CRC tissues and adjacent normal tissues. In vitro and in vivo experiments revealed that knockdown of FAM83H-AS1 in CRC cells inhibited tumor proliferation and metastasis, and vice versa. M6A modification is critical for FAM83H-AS1 RNA stability through the writer METTL3 and the readers IGF2BP2/IGFBP3. PTBP1-an RNA binding protein-is responsible for the FAM83H-AS1 function in CRC. T4 (1770-2440 nt) and T5 (2440-2743 nt) on exon 4 of FAM83H-AS1 provide a platform for PTBP1 RRM2 interactions. Our results demonstrated that m6A modification dysregulated the FAM83H-AS1 oncogenic role by phosphorylated PTBP1 on its RNA splicing effect. In patient-derived xenograft models, ASO-FAM83H-AS1 significantly suppressed the growth of gastrointestinal (GI) tumors, not only CRC but also GC and ESCC. The combination of ASO-FAM83H-AS1 and oxaliplatin/cisplatin significantly suppressed tumor growth compared with treatment with either agent alone. Notably, there was pathological complete response in all these three GI cancers. Our findings suggest that FAM83H-AS1 targeted therapy would benefit patients primarily receiving platinum-based therapy in GI cancers.

Topics & Concepts

Cancer researchGene knockdownColorectal cancerBiologyLong non-coding RNARNA-binding proteinRNACancerCell cultureGeneGeneticsRNA modifications and cancerCancer-related molecular mechanisms researchRNA Research and Splicing