TGFBI公司
癌症研究
内皮糖蛋白
血管生成
转移
医学
癌症
结直肠癌
转化生长因子
生物
内科学
干细胞
细胞生物学
川地34
作者
Barbara Chiavarina,Brunella Costanza,Roberto Ronca,Arnaud Blomme,Sara Rezzola,Paola Chiodelli,Ambre Giguelay,Guillame Belthier,Gilles Doumont,Gaëtan Van Simaeys,Simon Lacroix,Takehiko Yokobori,Bilguun Erkhem‐Ochir,Patrick Balaguer,Vincent Cavaillès,Eric Fabbrizio,Emmanuel Di Valentin,Stéphanie Gofflot,Olivier Detry,Guy Jérusalem
出处
期刊:Theranostics
[Ivyspring International Publisher]
日期:2020-12-16
卷期号:11 (4): 1626-1640
被引量:63
摘要
Colorectal cancer (CRC) cells are traditionally considered unresponsive to TGFβ due to mutations in the receptors and/or downstream signaling molecules. TGFβ influences CRC cells only indirectly via stromal cells, such as cancer-associated fibroblasts. However, CRC cell ability to directly respond to TGFβ currently remains unexplored. This represents a missed opportunity for diagnostic and therapeutic interventions. Methods: We examined whether cancer cells from primary CRC and liver metastases respond to TGFβ by inducing TGFβ-induced protein ig-h3 (TGFBI) expression, and the contribution of canonical and non-canonical TGFβ signaling pathways to this effect. We then investigated in vitro and in vivo TGFBI impact on metastasis formation and angiogenesis. Using patient serum samples and an orthotopic mouse model of CRC liver metastases we assessed the diagnostic/tumor targeting value of novel antibodies against TGFBI. Results: Metastatic CRC cells, such as circulating tumor cells, directly respond to TGFβ. These cells were characterized by the absence of TGFβ receptor mutations and the frequent presence of p53 mutations. The pro-tumorigenic program orchestrated by TGFβ in CRC cells was mediated through TGFBI, the expression of which was positively regulated by non-canonical TGFβ signaling cascades. TGFBI inhibition was sufficient to significantly reduce liver metastasis formation in vivo. Moreover, TGFBI pro-tumorigenic function was linked to its ability to stimulate angiogenesis. TGFBI levels were higher in serum samples from untreated patients with CRC than in patients who were receiving chemotherapy. A radiolabeled anti-TGFBI antibody selectively targeted metastatic lesions in vivo, underscoring its diagnostic and therapeutic potential. Conclusions: TGFβ signaling in CRC cells directly contributes to their metastatic potential and stromal cell-independence. Proteins downstream of activated TGFβ, such as TGFBI, represent novel diagnostic and therapeutic targets for more specific anti-metastatic therapies.
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