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Clustering of discrete cell properties essential for tumorigenicity and metastasis. I. Studies of syrian hamster embryo fibroblasts spontaneously transformed in vitro

โœ Scribed by G. I. Deichman; T. E. Kluchareva; V. A. Matveeva; N. E. Kushlinsky; L. S. Bassalyk; E. L. Vendrov


Publisher
John Wiley and Sons
Year
1989
Tongue
French
Weight
431 KB
Volume
44
Category
Article
ISSN
0020-7136

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โœฆ Synopsis


The expression of two discrete cell properties related to the host natural effector mechanisms, i.e., resistance to damage by H2O2, a cytotoxic product of activated macrophages, and the ability to secrete PGE, which inhibits NK-cell cytotoxicity, has been examined in parental Syrian hamster embryo cells spontaneously transformed in vitro (STHE strain) and in 18 in vivo selected sublines. In all cell variants, resistance to H2O2 and PGE-releasing activity were either both expressed, or not expressed at all. Parental STHE cells and 5 variants selected in vivo, which were equally highly susceptible to H2O2-induced damage, did not release any detectable amount of PGE upon contact with NK cells. In contrast, 13 other STHE variants selected in vivo and characterized by their resistance to H2O2, all released PGE upon contact with NK cells. Thus, these two biochemically unrelated cell phenotypic characteristics are likely to be either simultaneously selected in vivo, or united in cluster which pre-exist or appear in rare cell variants of the parental cell population in the conditions of in vivo natural selection pressure.


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Clustering of discrete cell properties e
โœ G. I. Deichman; H. A. Kashleva; T. E. Kluchareva; V. A. Matveeva ๐Ÿ“‚ Article ๐Ÿ“… 1989 ๐Ÿ› John Wiley and Sons ๐ŸŒ French โš– 400 KB

Tumorigenic and metastasizing activities (TGA; MA) and susceptibility, or resistance to H,O, and PGE-releasing activity (HzO: + PGE'+ phenotype) have been examined in 6 Syrian hamster embryo cell strains transformed in vitro with Rous sarcoma viruses (Schmidt-Ruppin and Prague strains). Early observ