李翛然
(2023-03-28 21:41):
#paper A novel protein RASON encoded by a lncRNA controls oncogenic RAS signaling in KRAS mutant cancers doi: 10.1038/s41422-022-00726-7. Cell Research
. 这篇文章是我最近精读的一篇文章,作者我都认识,做的靶点恰恰是我们正在做的。所以聊了很多。 这是很有可能针对未来一个大癌症种类的核心解决方案。 只不过现在rason 的结构还没有解析出来。 我们看看今年怎么处理一下。
A novel protein RASON encoded by a lncRNA controls oncogenic RAS signaling in KRAS mutant cancers
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Abstract:
Mutations of the RAS oncogene are found in around 30% of all human cancers yet direct targeting of RAS is still considered clinically impractical except for the KRAS mutant. Here we report that RAS-ON (RASON), a novel protein encoded by the long intergenic non-protein coding RNA 00673 (LINC00673), is a positive regulator of oncogenic RAS signaling. RASON is aberrantly overexpressed in pancreatic ductal adenocarcinoma (PDAC) patients, and it promotes proliferation of human PDAC cell lines in vitro and tumor growth in vivo. CRISPR/Cas9-mediated knockout of Rason in mouse embryonic fibroblasts inhibits KRAS-mediated tumor transformation. Genetic deletion of Rason abolishes oncogenic KRAS-driven pancreatic and lung cancer tumorigenesis in LSL-Kras; Trp53 mice. Mechanistically, RASON directly binds to KRAS and inhibits both intrinsic and GTPase activating protein (GAP)-mediated GTP hydrolysis, thus sustaining KRAS in the GTP-bound hyperactive state. Therapeutically, deprivation of RASON sensitizes KRAS mutant pancreatic cancer cells and patient-derived organoids to EGFR inhibitors. Our findings identify RASON as a critical regulator of oncogenic KRAS signaling and a promising therapeutic target for KRAS mutant cancers.
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