SPARC Induces E-Cadherin Repression and Enhances Cell Migration through Integrin alpha v beta 3 and the Transcription Factor ZEB1 in Prostate Cancer Cells

Lopez-Moncada, Fernanda; Jose Torres, Maria; Lavanderos, Boris; Cerda, Oscar; Castellon, Enrique A.; Contreras, Hector R.

Abstract

Secreted protein acidic and rich in cysteine (SPARC), or osteonectin, is a matricellular protein that modulates interactions between cells and their microenvironment. SPARC is expressed during extracellular matrix remodeling and is abundant in bone marrow and high-grade prostate cancer (PCa). In PCa, SPARC induces changes associated with epithelial-mesenchymal transition (EMT), enhancing migration and invasion and increasing the expression of EMT transcriptional factor Zinc finger E-box-binding homeobox 1 (ZEB1), but not Zinc finger protein SNAI1 (Snail) or Zinc finger protein SNAI2 (Slug). It is unknown whether the SPARC-induced downregulation of E-cadherin in PCa cells depends on ZEB1. Several integrins are mediators of SPARC effects in cancer cells. Because integrin signaling can induce EMT programs, we hypothesize that SPARC induces E-cadherin repression through the activation of integrins and ZEB1. Through stable knockdown and the overexpression of SPARC in PCa cells, we demonstrate that SPARC downregulates E-cadherin and increases vimentin, ZEB1, and integrin beta 3 expression. Knocking down SPARC in PCa cells decreases the tyrosine-925 phosphorylation of FAK and impairs focal adhesion formation. Blocking integrin alpha v beta 3 and silencing ZEB1 revert both the SPARC-induced downregulation of E-cadherin and cell migration enhancement. We conclude that SPARC induces E-cadherin repression and enhances PCa cell migration through the integrin alpha v beta 3/ZEB1 signaling pathway.

Más información

Título según WOS: SPARC Induces E-Cadherin Repression and Enhances Cell Migration through Integrin alpha v beta 3 and the Transcription Factor ZEB1 in Prostate Cancer Cells
Título de la Revista: INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volumen: 23
Número: 11
Editorial: MDPI
Fecha de publicación: 2022
DOI:

10.3390/ijms23115874

Notas: ISI