Enhanced tumor growth in the NaS1 sulfate transporter null mouse : научное издание

Описание

Тип публикации: статья из журнала

Год издания: 2010

Идентификатор DOI: 10.1111/j.1349-7006.2009.01399.x

Аннотация: Sulfate plays an important role in maintaining normal structure and function of tissues, and its content is decreased in certain cancers including lung carcinoma. In this study, we investigated tumor growth in a mouse model of hyposulfatemia (Nas1-/-) and compared it to wild-type (Nas1+/+) mice. Lung epithelial tumor cells (TC-1 cell line) were injected subcutaneously into male Nas1-/- and Nas1+/+ mice on a mixed 129Sv and C57BL/6 genetic background. Tumor sections were stained with anti-glycosaminoglycan antibodies to assess the distribution of proteoglycans and Gomori's trichrome to detect collagen. After 14 days, tumor weights were markedly increased (by ~12-fold) in Nas1-/- mice when compared with Nas1+/+ mice. Histological analyses of tumors revealed increased (by ≈2.4-fold) vessel content, as well as markedly reduced collagen and immunoreactivity against glycosaminoglycan structural epitopes in the tumors from Nas1-/- mice. No significant differences were found for the growth of cultured TC-1 cells supplemented with Nas1-/- or Nas1+/+ serum, as determined by 3H-thymidine incorporation, implying that the cell culture conditions may not reflect the in vivo situation of enhanced tumor growth. This study has revealed increased tumor growth and an altered extracellular tumor matrix in hyposulfatemic Nas1-/- mice. These findings highlight the importance of blood sulfate levels as a possible modulator of tumor growth, and could lead to future cancer studies in humans with altered sulfate homeostasis. © 2009 Japanese Cancer Association.

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Издание

Журнал: Cancer Science

Выпуск журнала: Т. 101, 2

Номера страниц: 369-373

ISSN журнала: 13479032

Издатель: Oxford University Press

Персоны

  • Dawson P.A. (School of Biomedical Sciences,University of Queensland)
  • Markovich D. (School of Biomedical Sciences,University of Queensland)
  • Choyce A. (The University of Queensland Diamantina Institute for Cancer,Immunology and Metabolic Medicine,Princess Alexandra Hospital)
  • Leggatt G.R. (The University of Queensland Diamantina Institute for Cancer,Immunology and Metabolic Medicine,Princess Alexandra Hospital)
  • Chuang C. (Graduate School of Biomedical Engineering,University of New South Wales)
  • Whitelock J. (Graduate School of Biomedical Engineering,University of New South Wales)

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