PLoS ONE (Jan 2015)

Cellular Adhesion Promotes Prostate Cancer Cells Escape from Dormancy.

  • Nazanin Ruppender,
  • Sandy Larson,
  • Bryce Lakely,
  • Lori Kollath,
  • Lisha Brown,
  • Ilsa Coleman,
  • Roger Coleman,
  • Holly Nguyen,
  • Peter S Nelson,
  • Eva Corey,
  • Linda A Snyder,
  • Robert L Vessella,
  • Colm Morrissey,
  • Hung-Ming Lam

DOI
https://doi.org/10.1371/journal.pone.0130565
Journal volume & issue
Vol. 10, no. 6
p. e0130565

Abstract

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Dissemination of prostate cancer (PCa) cells to the bone marrow is an early event in the disease process. In some patients, disseminated tumor cells (DTC) proliferate to form active metastases after a prolonged period of undetectable disease known as tumor dormancy. Identifying mechanisms of PCa dormancy and reactivation remain a challenge partly due to the lack of in vitro models. Here, we characterized in vitro PCa dormancy-reactivation by inducing cells from three patient-derived xenograft (PDX) lines to proliferate through tumor cell contact with each other and with bone marrow stroma. Proliferating PCa cells demonstrated tumor cell-cell contact and integrin clustering by immunofluorescence. Global gene expression analyses on proliferating cells cultured on bone marrow stroma revealed a downregulation of TGFB2 in all of the three proliferating PCa PDX lines when compared to their non-proliferating counterparts. Furthermore, constitutive activation of myosin light chain kinase (MLCK), a downstream effector of integrin-beta1 and TGF-beta2, in non-proliferating cells promoted cell proliferation. This cell proliferation was associated with an upregulation of CDK6 and a downregulation of E2F4. Taken together, our data provide the first clinically relevant in vitro model to support cellular adhesion and downregulation of TGFB2 as a potential mechanism by which PCa cells may escape from dormancy. Targeting the TGF-beta2-associated mechanism could provide novel opportunities to prevent lethal PCa metastasis.