4.8 Article

Tumor cell-organized fibronectin maintenance of a dormant breast cancer population

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SCIENCE ADVANCES
卷 6, 期 11, 页码 -

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AMER ASSOC ADVANCEMENT SCIENCE
DOI: 10.1126/sciadv.aaz4157

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资金

  1. NSF-NCI award [DMR-1234852]
  2. NIH [1DP2CA186573-01]
  3. Pew Charitable Trusts
  4. Barry and Afsaneh Siadat faculty award
  5. National Institutes of Health [T32 GM008515]
  6. National Science Foundation Graduate Research Fellowship [1451512]
  7. Cell and Tissue Engineering NIH Biotechnology Training Grant [T32-GM008433]
  8. NCI [R01 CA168464, 203439]

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Tumors can undergo long periods of dormancy, with cancer cells entering a largely quiescent, nonproliferative state before reactivation and outgrowth. To understand the role of the extracellular matrix (ECM) in regulating tumor dormancy, we created an in vitro cell culture system with carefully controlled ECM substrates to observe entrance into and exit from dormancy with live imaging. We saw that cell populations capable of surviving entrance into long-term dormancy were heterogeneous, containing quiescent, cell cycle-arrested, and actively proliferating cells. Cell populations capable of entering dormancy formed an organized, fibrillar fibronectin matrix via alpha(v)beta(3 )and alpha(5)beta(1) integrin adhesion, ROCK-generated tension, and TGF beta 2 stimulation, and cancer cell outgrowth after dormancy required MMP-2-mediated fibronectin degradation. We propose this approach as a useful, in vitro method to study factors important in regulating dormancy, and we used it here to elucidate a role for fibronectin deposition and MMP activation.

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