Literature DB >> 7698245

Growth-inhibitory functions of a mutated gelsolin (His321) in NIH/3T3 mouse fibroblasts.

A Ishizaki1, H Fujita, N Kuzumaki.   

Abstract

We have previously established a murine flat revertant cell line R1 from an activated H-ras transformant EJ-NIH/3T3 by subjecting it to ethyl methanesulfonate. From the R1 cells, we cloned a mutated gelsolin gene His321 and have shown the inhibitory activity of His321 against EJ-NIH/3T3 tumors. Our present experiments were conducted to find out whether the His321 gene has any effects on untransformed NIH/3T3 fibroblasts. Rhodamine-phalloidin staining revealed that two NIH/3T3 clones expressing His321 (NIH/lambda 2S-3 and NIH/lambda 2S-6) form organized actin stress fibers as two clones transfected with the vector alone (NIH/neo-3 and NIH/neo-5). We also found that in a liquid medium, NIH/lambda 2S-3 and NIH/lambda 2S-6 grew more slowly than NIH/neo-3 and NIH/neo-5 and that the doubling times of the former were about 10 h slower than those of the latter. To investigate the effects of His321 on the signal transduction pathway necessary for cell growth, we stimulated the cell lines by prostaglandin E1 (PGE1), a platelet-derived growth factor (PDGF), or the epidermal growth factor (EGF). Although stimulation by PGE1 increased intercellular cyclic AMP in R1 cells, it did not do so in NIH/lambda 2S-3 and NIH/lambda 2S-6 cells. On the other hand, stimulation by PDGF or EGF induced far less DNA synthesis in NIH/lambda 2S-3 and NIH/lambda 2S-6 than in NIH/neo-3 and NIH/neo5. These results suggest that through the effects on the signal transduction pathway of PDGF and/or EGF His321-mutated gelsolin inhibits the growth of NIH/3T3.

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Year:  1995        PMID: 7698245     DOI: 10.1006/excr.1995.1108

Source DB:  PubMed          Journal:  Exp Cell Res        ISSN: 0014-4827            Impact factor:   3.905


  3 in total

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Authors:  Crystal G Pontrello; Iryna M Ethell
Journal:  Open Neurosci J       Date:  2009-01-01

2.  Gelsolin suppresses tumorigenicity through inhibiting PKC activation in a human lung cancer cell line, PC10.

Authors:  N Sagawa; H Fujita; Y Banno; Y Nozawa; H Katoh; N Kuzumaki
Journal:  Br J Cancer       Date:  2003-02-24       Impact factor: 7.640

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Journal:  Genome Biol       Date:  2008-01-30       Impact factor: 13.583

  3 in total

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