4.6 Article

Lipid phosphate phosphatase-1 expression in cancer cells attenuates tumor growth and metastasis in mice

期刊

JOURNAL OF LIPID RESEARCH
卷 55, 期 11, 页码 2389-2400

出版社

ELSEVIER
DOI: 10.1194/jlr.M053462

关键词

autotaxin; breast cancer; thyroid cancer; cell migration; epidermal growth factor receptor; G-protein-coupled receptors; lysophosphatidate

资金

  1. Canadian Institutes of Health Research (CIHR)
  2. Canadian Breast Cancer Foundation (CBCF)
  3. Women and Children's Health Research Institute of the University of Alberta
  4. CIHR
  5. Alberta Cancer Foundation
  6. CBCF
  7. Vanier Canada Graduate Scholarship from the Government of Canada
  8. Killam Trust Award
  9. MD/PhD scholarship from Alberta Innovates-Health Solutions

向作者/读者索取更多资源

Lipid phosphate phosphatase-1 (LPP1) degrades lysophosphatidate (LPA) and attenuates receptor-mediated signaling. LPP1 expression is low in many cancer cells and tumors compared with normal tissues. It was hypothesized from studies with cultured cells that increasing LPP1 activity would decrease tumor growth and metastasis. This hypothesis has never been tested in vivo. To do this, we inducibly expressed LPP1 or a catalytically inactive mutant in cancer cells. Expressing active LPP1 increased extracellular LPA degradation by 5-fold. It also decreased the stimulation of Ca2+ transients by LPA, a nondephosphorylatable LPA(1/2) receptor agonist and a protease-activated receptor-1 peptide. The latter results demonstrate that LPP1 has effects downstream of receptor activation. Decreased Ca2+ mobilization and Rho activation contributed to the effects of LPP1 in attenuating the LPA-induced migration of MDA-MB-231 breast cancer cells and their growth in 3D culture. Increasing LPP1 expression in breast and thyroid cancer cells decreased tumor growth and the metastasis by up to 80% compared with expression of inactive LPP1 or green fluorescent protein in syngeneic and xenograft mouse models. The present work demonstrates for the first time that increasing the LPP1 activity in three lines of aggressive cancer cells decreases their abilities to produce tumors and metastases in mice.

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