Dokumentdetails
ID

doi:10.1038/s42003-023-05757-3...

Autor
Cao, Yan Li, Jian Zhang, Gang Fang, Hao Du, Yongliang Liang, Yan
Langue
en
Editor

Nature

Kategorie

Life Sciences

Jahr

2024

Auflistungsdatum

31.01.2024

Schlüsselwörter
colorectal ptbp1 cancer klf15
Metrisch

Zusammenfassung

Colorectal cancer is a grievous health concern, we have proved long non-coding RNA LINC00689 is considered as a potential diagnosis biomarker for colorectal cancer, and it is necessary to further investigate its upstream and downstream mechanisms.

Here, we show that KLF15, a transcription factor, exhibits the reduced expression in colorectal cancer.

KLF15 suppresses the proliferative and metastatic capacities of colorectal cancer cells both in vitro and in vivo by transcriptionally activating LINC00689 .

Subsequently, LINC00689 recruits PTBP1 protein to enhance the stability of LATS2 mRNA in the cytoplasm.

This stabilization causes the suppression of the YAP1/β-catenin pathway and its target downstream genes.

Our findings highlight a regulatory network involving KLF15, LINC00689 , PTBP1, LATS2 , and the YAP1/β-catenin pathway in colorectal cancer, shedding light on potential therapeutic targets for colorectal cancer therapy.

KLF15 transcriptionally activates LINC00689 , leading to the stabilization of LATS2 mRNA by recruiting PTBP1, which in turn suppresses colorectal tumorigenesis by inhibiting oncogenes like YAP1 and β-catenin.

Cao, Yan,Li, Jian,Zhang, Gang,Fang, Hao,Du, Yongliang,Liang, Yan, 2024, KLF15 transcriptionally activates LINC00689 to inhibit colorectal cancer development, Nature

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