The temporal relationship between butyrate-induced cellular flattening of murine sarcoma virus-transformed rat cells (MSV-NRK) and alterations in certain surface-associated biochemical markers of transformation, e.g., surface glycopeptides, glycolipids, fibronectin, hexose uptake, and cell-substrate adhesion was examined. The induction of elevated levels of the ganglioside GM3 and of a GDla-like ganglioside were observed to precede or to parallel cellular flattening. Likewise, enhanced incorporation of radioisotopically labeled fucose into a novel fucose-containing component, i.e., glucopyranosyl (1 leads to 3) fucopyranosyl-threonine, was also observed to occur at an early stage of cellular flattening. In contrast, a shift in the molecular weight distribution of trypsin-sensitive, surface fucopeptides was observed to occur at a late stage of cellular flattening. Moreover, surface fibronectin was not detectable in the butyrate-flattened MSV-NRK cells despite the fact that the cells manifested significantly enhanced cell-substrate adhesion. Thus, butyrate appears to be a useful tool for understanding the sequential changes associated with expression of the transformed phenotype of MSV-NRK cells.
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1 February 1980
Article|
February 01 1980
Effects of sodium butyrate on the membrane glycoconjugates of murine sarcoma virus-transformed rat cells.
D P Via
S Sramek
G Larriba
S Steiner
Online ISSN: 1540-8140
Print ISSN: 0021-9525
J Cell Biol (1980) 84 (2): 225–234.
Citation
D P Via, S Sramek, G Larriba, S Steiner; Effects of sodium butyrate on the membrane glycoconjugates of murine sarcoma virus-transformed rat cells.. J Cell Biol 1 February 1980; 84 (2): 225–234. doi: https://doi.org/10.1083/jcb.84.2.225
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