Cathepsin B and tumor proteolysis: contribution of the tumor microenvironment
BF Sloane, S Yan, I Podgorski, BE Linebaugh… - Seminars in cancer …, 2005 - Elsevier
Seminars in cancer biology, 2005•Elsevier
Tumor–stromal interactions induce expression of matrix metalloproteinases and serine
proteases and, as shown recently, the cysteine protease cathepsin B. We speculate that
such interactions upregulate the transcription factor Ets1, resulting in increased cathepsin B
expression. This would be consistent with the observed concomitant upregulation of matrix
metalloproteinases and serine proteases as well as with the ability of extracellular matrices
and their binding partners to alter cathepsin B expression and secretion. Using a confocal …
proteases and, as shown recently, the cysteine protease cathepsin B. We speculate that
such interactions upregulate the transcription factor Ets1, resulting in increased cathepsin B
expression. This would be consistent with the observed concomitant upregulation of matrix
metalloproteinases and serine proteases as well as with the ability of extracellular matrices
and their binding partners to alter cathepsin B expression and secretion. Using a confocal …
Tumor–stromal interactions induce expression of matrix metalloproteinases and serine proteases and, as shown recently, the cysteine protease cathepsin B. We speculate that such interactions upregulate the transcription factor Ets1, resulting in increased cathepsin B expression. This would be consistent with the observed concomitant upregulation of matrix metalloproteinases and serine proteases as well as with the ability of extracellular matrices and their binding partners to alter cathepsin B expression and secretion. Using a confocal assay to analyze the contribution of tumor–stromal interactions to proteolysis, we have been able to confirm enhanced degradation of extracellular matrices by all three classes of proteases.
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