AI Article Synopsis

  • Prostate cancer cells must survive in the bloodstream for metastasis, and the study reveals that β1 integrins and FAK activation increase during their progression.
  • Highly metastatic PC3 and PC3-mm2 cells show continuous β1 integrin activation, correlating with their ability to resist anoikis, while low-metastatic cells like LNCaP and C4-2B4 have less activation.
  • Targeting β1 integrins with a specific antibody, mAb 33B6, significantly reduces adhesion and increases apoptosis in PC3-mm2 cells, indicating it could be a promising approach to prevent prostate cancer metastasis.

Article Abstract

Disseminated prostate cancer cells must survive in circulation for metastasis to occur. Mechanisms by which these cells survive are not well understood. By immunohistochemistry of human tissues, we found that levels of β1 integrins and integrin-induced autophosphorylation of FAK (pFAK-Y397) are increased in prostate cancer cells in primary prostate cancer and lymph node metastases, suggesting that β1 integrin activation occurs in metastatic progression of prostate cancer. A conformation-sensitive antibody, 9EG7, was used to examine β1 integrin activation. We found that β1 integrins are constitutively activated in highly metastatic PC3 and PC3-mm2 cells, with less activation in low metastatic LNCaP and C4-2B4 cells. Increased β1 integrin activation as well as the anoikis resistance in prostate cancer cells correlated with metastatic potential in vivo. Knockdown of β1 integrin abrogated anoikis resistance in PC3-mm2 cells. In agreement with β1 integrin activation, PC3-mm2 cells strongly adhered to type I collagen and fibronectin, a process inhibited by the β1 integrin-neutralizing antibody mAb 33B6. mAb 33B6 also inhibited the phosphorylation of β1 integrin downstream effectors, focal adhesion kinase (FAK) and AKT, leading to a 3-fold increase in PC3-mm2 apoptosis. Systemic delivery of mAb 33B6 suppressed spontaneous metastasis of PC3-mm2 from the prostate to distant lymph nodes following intraprostatic injection and suppressed metastasis of PC3-mm2 to multiple organs following intracardiac injection. Thus, constitutively activated β1 integrins play a role in survival of PC3-mm2 cells in circulation and represent a potential target for metastasis prevention.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3631285PMC
http://dx.doi.org/10.1158/1541-7786.MCR-12-0551DOI Listing

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