Abi1 loss drives prostate tumorigenesis through activation of EMT and non-canonical WNT signaling

Disharee Nath; Xiang Li; Claudia Mondragon; Dawn Post; Ming Chen; Julie R White; Anita Hryniewicz-Jankowska; Tiffany Caza; Vladimir A Kuznetsov; Heidi Hehnly; Tamara Jamaspishvili; David M Berman; Fan Zhang; Sonia H Y Kung; Ladan Fazli; Martin E Gleave; Gennady Bratslavsky; Pier Paolo Pandolfi; Leszek Kotula

doi:10.1186/s12964-019-0410-y

Abi1 loss drives prostate tumorigenesis through activation of EMT and non-canonical WNT signaling

Cell Commun Signal. 2019 Sep 18;17(1):120. doi: 10.1186/s12964-019-0410-y.

Authors

Disharee Nath^{1

2}, Xiang Li^{1

2}, Claudia Mondragon¹, Dawn Post¹, Ming Chen^{3

4

5}, Julie R White⁶, Anita Hryniewicz-Jankowska^{1

7}, Tiffany Caza⁸, Vladimir A Kuznetsov^{1

9}, Heidi Hehnly¹⁰, Tamara Jamaspishvili¹¹, David M Berman¹¹, Fan Zhang¹², Sonia H Y Kung¹², Ladan Fazli¹², Martin E Gleave¹², Gennady Bratslavsky¹, Pier Paolo Pandolfi³, Leszek Kotula^{13

14}

Affiliations

¹ Department of Urology, Upstate Cancer Center, SUNY Upstate Medical University, 750 East Adams Street, Syracuse, New York, 13210, USA.
² Department of Biochemistry and Molecular Biology, SUNY Upstate Medical University, Syracuse, NY, 13210, USA.
³ Cancer Research Institute, Beth Israel Deaconess Cancer Center, Department of Medicine and Pathology, Beth Israel Deaconess Medical Center, Harvard Medical School, Boston, MA, 02215, USA.
⁴ Present address: Department of Pathology, Duke University School of Medicine, Durham, NC, 27710, USA.
⁵ Duke Cancer Institute, Duke University, Durham, NC, 27710, USA.
⁶ Laboratory of Comparative Pathology, Memorial Sloan-Kettering Cancer Center, New York, NY, 10065, USA.
⁷ Department of Cytobiochemistry, Faculty of Biotechnology, University of Wroclaw, ul. F. Joliot-Curie 14a, 50-383, Wroclaw, Poland.
⁸ Department of Pathology and Medicine, SUNY Upstate Medical University, Syracuse, NY, 13210, USA.
⁹ Bioinformatics Institute, A-STAR, Singapore, 138671, Singapore.
¹⁰ Department of Cell and Developmental Biology, SUNY Upstate Medical University, Syracuse, NY, 13210, USA.
¹¹ Department of Pathology and Molecular Medicine and Division of Cancer Biology & Genetics, Queen's Cancer Research Institute, Queen's University, 10 Stuart St, Kingston, ON, K7L 3N6, Canada.
¹² Department of Urologic Sciences, Vancouver Prostate Centre, University of British Columbia, Vancouver, BC, V6H 3Z6, Canada.
¹³ Department of Urology, Upstate Cancer Center, SUNY Upstate Medical University, 750 East Adams Street, Syracuse, New York, 13210, USA. kotulal@upstate.edu.
¹⁴ Department of Biochemistry and Molecular Biology, SUNY Upstate Medical University, Syracuse, NY, 13210, USA. kotulal@upstate.edu.

Abstract

Background: Prostate cancer development involves various mechanisms, which are poorly understood but pointing to epithelial mesenchymal transition (EMT) as the key mechanism in progression to metastatic disease. ABI1, a member of WAVE complex and actin cytoskeleton regulator and adaptor protein, acts as tumor suppressor in prostate cancer but the role of ABI1 in EMT is not clear.

Methods: To investigate the molecular mechanism by which loss of ABI1 contributes to tumor progression, we disrupted the ABI1 gene in the benign prostate epithelial RWPE-1 cell line and determined its phenotype. Levels of ABI1 expression in prostate organoid tumor cell lines was evaluated by Western blotting and RNA sequencing. ABI1 expression and its association with prostate tumor grade was evaluated in a TMA cohort of 505 patients and metastatic cell lines.

Results: Low ABI1 expression is associated with biochemical recurrence, metastasis and death (p = 0.038). Moreover, ABI1 expression was significantly decreased in Gleason pattern 5 vs. pattern 4 (p = 0.0025) and 3 (p = 0.0012), indicating an association between low ABI1 expression and highly invasive prostate tumors. Disruption of ABI1 gene in RWPE-1 cell line resulted in gain of an invasive phenotype, which was characterized by a loss of cell-cell adhesion markers and increased migratory ability of RWPE-1 spheroids. Through RNA sequencing and protein expression analysis, we discovered that ABI1 loss leads to activation of non-canonical WNT signaling and EMT pathways, which are rescued by re-expression of ABI1. Furthermore, an increase in STAT3 phosphorylation upon ABI1 inactivation and the evidence of a high-affinity interaction between the FYN SH2 domain and ABI1 pY421 support a model in which ABI1 acts as a gatekeeper of non-canonical WNT-EMT pathway activation downstream of the FZD2 receptor.

Conclusions: ABI1 controls prostate tumor progression and epithelial plasticity through regulation of EMT-WNT pathway. Here we discovered that ABI1 inhibits EMT through suppressing FYN-STAT3 activation downstream from non-canonical WNT signaling thus providing a novel mechanism of prostate tumor suppression.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't
Research Support, U.S. Gov't, Non-P.H.S.

MeSH terms

Adaptor Proteins, Signal Transducing / deficiency*
Adaptor Proteins, Signal Transducing / genetics*
Cadherins / metabolism
Carcinogenesis / genetics*
Cell Adhesion / genetics
Cell Line, Tumor
Cell Movement / genetics
Cytoskeletal Proteins / deficiency*
Cytoskeletal Proteins / genetics*
Epithelial-Mesenchymal Transition / genetics*
Frizzled Receptors / metabolism
Gene Knockout Techniques*
Humans
Male
Neoplasm Grading
Phenotype
Prostatic Neoplasms / pathology*
Recurrence
STAT3 Transcription Factor / metabolism
Up-Regulation / genetics
Wnt Signaling Pathway / genetics*
beta Catenin / metabolism

Substances

ABI1 protein, human
Adaptor Proteins, Signal Transducing
Cadherins
Cytoskeletal Proteins
FZD2 protein, human
Frizzled Receptors
STAT3 Transcription Factor
beta Catenin

Abstract

Publication types

MeSH terms

Substances

Grants and funding