RRC ID 87185
著者 Li Y, Fujishita T, Mishiro-Sato E, Kojima Y, Niu Y, Taketo MM, Urano Y, Sakai T, Enomoto A, Nishida Y, Aoki M.
タイトル TGF-β signaling promotes desmoid tumor formation via CSRP2 upregulation.
ジャーナル Cancer Sci
Abstract Desmoid tumors (DTs), also called desmoid-type fibromatoses, are locally aggressive tumors of mesenchymal origin. In the present study, we developed a novel mouse model of DTs by inducing a local mutation in the Ctnnb1 gene, encoding β-catenin in PDGFRA-positive stromal cells, by subcutaneous injection of 4-hydroxy-tamoxifen. Tumors in this model resembled histologically clinical samples from DT patients and showed strong phosphorylation of nuclear SMAD2. Knockout of SMAD4 in the model significantly suppressed tumor growth. Proteomic analysis revealed that SMAD4 knockout reduced the level of Cysteine-and-Glycine-Rich Protein 2 (CSRP2) in DTs, and treatment of DT-derived cells with a TGF-β receptor inhibitor reduced CSRP2 RNA levels. Knockdown of CSRP2 in DT cells significantly suppressed their proliferation. These results indicate that the TGF-β/CSRP2 axis is a potential therapeutic target for DTs downstream of TGF-β signaling.
巻・号 115(2)
ページ 401-411
公開日 2024-2-1
DOI 10.1111/cas.16037
PMID 38041233
PMC PMC10859603
MeSH Animals Desmoid Tumors* / genetics Desmoid Tumors* / pathology Humans LIM Domain Proteins / genetics Mice Mice, Knockout Muscle Proteins / metabolism Nuclear Proteins / genetics Proteomics Transforming Growth Factor beta / metabolism Up-Regulation beta Catenin / genetics beta Catenin / metabolism
IF 4.966
リソース情報
実験動物マウス RBRC09616