Synergistic therapeutic effect of combined PDGFR and SGK1 inhibition in metastasis-initiating cells of breast cancer

被引：33

作者：

Yang, Lu ^{[1
,2
,3
,4
]}

Li, Ning ^{[1
,2
,3
,4
]}

Xue, Zhicheng ^{[1
,2
,3
,4
]}

Liu, Ling-Rui ^{[1
,2
,3
,4
]}

Li, Jian ^{[5
]}

Huang, Xiaojia ^{[1
,2
,3
,4
]}

Xie, Xinhua ^{[1
,2
,3
,4
]}

Zou, Yutian ^{[1
,2
,3
,4
]}

Tang, Hailin ^{[1
,2
,3
,4
]}

Xie, Xiaoming ^{[1
,2
,3
,4
]}

机构：

[1] Sun Yat Sen Univ, Dept Expt Res, Canc Ctr, Guangzhou, Peoples R China

[2] State Key Lab Oncol South China, Guangzhou, Peoples R China

[3] Collaborat Innovat Ctr Canc Med, Guangzhou, Peoples R China

[4] Sun Yat Sen Univ, Dept Breast Oncol, Canc Ctr, Guangzhou, Peoples R China

[5] Sun Yat Sen Univ, Dept Ultrasound, Canc Ctr, Guangzhou, Peoples R China

来源：

CELL DEATH AND DIFFERENTIATION | 2020年 / 27卷 / 07期

基金：

中国国家自然科学基金;

关键词：

RESISTANCE; PROGRESSION; ACTIVATION; GENES; LUNG;

D O I：

10.1038/s41418-019-0485-4

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

Lack of insight into the identity of the cells that initiate metastasis hampers the development of antimetastatic therapies. Only a tiny fraction of tumor cells termed metastasis-initiating cells (MICs) are able to successfully seed metastases, causing recurrence and therapeutic resistance. Using metastasis models, we describe a subpopulation of MIC derivates from lung metastases that do not have proliferation advantages, express high levels of the PDGF receptors and EMT/stemness-related genes, and are unique in their ability to initiate metastasis. PDGF factors specifically boost the metastatic potential of MIC populations in a PDGFR-dependent manner. However, PDGFR inhibition preferentially suppresses lung metastases, but does not reduce the primary tumor burden. Thus, we found that PDGFR inhibition blocks AKT activation, whereas SGK1, which shares high-similarity kinase domain and overlap substrates with AKT overexpression remains active in MICs. SGK1 and PDGF signaling act in concert to promote metastatic formation, and SGK1 inhibition confers vulnerability to PDGFR inhibitors, also eliciting a powerful antitumor effect. In vivo, SGK1 inhibitors sensitize xenograft tumors to PDGFR-targeted therapies by reducing primary tumor growth and lung metastasis. Consequently, dual inhibition of PDGFR and SGK1 exhibited strong antitumor activities in established breast cancer cell lines in vitro and in vivo. Therefore, this approach not only provides insight into MIC transformation but also aids the design of improved therapeutic strategies for advanced breast cancer.

引用

页码：2066 / 2080

页数：15

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