Linc00673-V3 positively regulates autophagy by promoting Smad3-mediated LC3B transcription in NSCLC.
Heng NiSong TangGuang LuYuequn NiuJinming XuHonghe ZhangJian HuHan-Ming ShenYihua WuDajing XiaPublished in: Life science alliance (2024)
Since its first discovery, long noncoding RNA Linc00673 has been linked to carcinogenesis and metastasis of various human cancers. Linc00673 had five transcriptional isoforms and their biological functions remained to be explored. Here we have reported that Linc00673-V3, one of the isoforms of Linc00673, promoted non-small cell lung cancer chemoresistance, and increased Linc00673-V3 expression level was associated with enhanced autophagy. Mechanistically, we discerned the existence of a stem-loop configuration engendered by the 1-100-nt and 2200-2275-nt fragments within Linc00673-V3. This structure inherently interacted with Smad3, thereby impeding its ubiquitination and subsequent degradation orchestrated by E3 ligase STUB1. The accumulation of Smad3 contributed to autophagy via up-regulation of LC3B transcription and ultimately conferred chemoresistance in NSCLC. Our results revealed a novel transcriptional regulation network between Linc00673-V3, Smad3, and LC3B , which provided an important insight into the interplay between autophagy regulation and non-canonical function of Smad3. Furthermore, the results from in vivo experiments suggested Linc00673-V3 targeted antisense oligonucleotide as a promising therapeutic strategy to overcome chemotherapy resistance in NSCLC.
Keyphrases
- long noncoding rna
- long non coding rna
- cell proliferation
- poor prognosis
- epithelial mesenchymal transition
- transforming growth factor
- cell death
- small cell lung cancer
- signaling pathway
- endoplasmic reticulum stress
- oxidative stress
- transcription factor
- gene expression
- advanced non small cell lung cancer
- small molecule
- drug delivery
- radiation therapy
- locally advanced
- heat shock protein
- rectal cancer