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FOXF2 reprograms breast cancer cells into bone metastasis seeds.


ABSTRACT: Bone metastases occur in most advanced breast cancer patients and cause serious skeletal-related complications. The mechanisms by which bone metastasis seeds develop in primary tumors and specifically colonize the bone remain to be elucidated. Here, we show that forkhead box F2 (FOXF2) functions as a master transcription factor for reprogramming cancer cells into an osteomimetic phenotype by pleiotropic transactivation of the BMP4/SMAD1 signaling pathway and bone-related genes that are expressed at early stages of bone differentiation. The epithelial-to-osteomimicry transition regulated by FOXF2 confers a tendency on cancer cells to metastasize to bone which leads to osteolytic bone lesions. The BMP antagonist Noggin significantly inhibits FOXF2-driven osteolytic bone metastasis of breast cancer cells. Thus, targeting the FOXF2-BMP/SMAD axis might be a promising therapeutic strategy to manage bone metastasis. The role of FOXF2 in transactivating bone-related genes implies a biological function of FOXF2 in regulating bone development and remodeling.

SUBMITTER: Wang S 

PROVIDER: S-EPMC6586905 | biostudies-literature | 2019 Jun

REPOSITORIES: biostudies-literature

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FOXF2 reprograms breast cancer cells into bone metastasis seeds.

Wang Shuo S   Li Gui-Xi GX   Tan Cong-Cong CC   He Rui R   Kang Li-Juan LJ   Lu Jun-Tao JT   Li Xiao-Qing XQ   Wang Qing-Shan QS   Liu Pei-Fang PF   Zhai Qiong-Li QL   Feng Yu-Mei YM  

Nature communications 20190620 1


Bone metastases occur in most advanced breast cancer patients and cause serious skeletal-related complications. The mechanisms by which bone metastasis seeds develop in primary tumors and specifically colonize the bone remain to be elucidated. Here, we show that forkhead box F2 (FOXF2) functions as a master transcription factor for reprogramming cancer cells into an osteomimetic phenotype by pleiotropic transactivation of the BMP4/SMAD1 signaling pathway and bone-related genes that are expressed  ...[more]

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