4.3 Article

Acid-Mediated Tumor Proteolysis: Contribution of Cysteine Cathepsins

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NEOPLASIA
卷 15, 期 10, 页码 1111-1123

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ELSEVIER SCIENCE INC
DOI: 10.1593/neo.13946

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  1. National Institutes of Health [R01 CA131990, R01 CA077575, U54 CA143970]
  2. National Institutes of Health Cancer Center Support [P30 CA22453]
  3. Perinatology Research Branch of the National Institute of Child Health and Development
  4. Cancer Center Support grant [P30 CA076292]

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One of the noncellular microenvironmental factors that contribute to malignancy of solid tumors is acidic peritumoral pH. We have previously demonstrated that extracellular acidosis leads to localization of the cysteine protease cathepsin B on the tumor cell membrane and its secretion. The objective of the present study was to determine if an acidic extracellular pH such as that observed in vivo (i.e., pHe 6.8) affects the activity of proteases, e. g., cathepsin B, that contribute to degradation of collagen IV by tumor cells when grown in biologically relevant three-dimensional (3D) cultures. For these studies, we used 1) 3D reconstituted basement membrane overlay cultures of human carcinomas, 2) live cell imaging assays to assess proteolysis, and 3) in vivo imaging of active tumor proteases. At pHe 6.8, there were increases in pericellular active cysteine cathepsins and in degradation of dye-quenched collagen IV, which was partially blocked by a cathepsin B inhibitor. Imaging probes for active cysteine cathepsins localized to tumors in vivo. The amount of bound probe decreased in tumors in bicarbonate-treated mice, a treatment previously shown to increase peritumoral pHe and reduce local invasion of the tumors. Our results are consistent with the acid-mediated invasion hypothesis and with a role for cathepsin B in promoting degradation of a basement membrane protein substrate, i.e., type IV collagen, in an acidic peritumoral environment.

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