Literature DB >> 7720072

Hemostatic, inflammatory, and fibroblast responses are blunted in mice lacking gelsolin.

W Witke1, A H Sharpe, J H Hartwig, T Azuma, T P Stossel, D J Kwiatkowski.   

Abstract

Gelsolin, an 82 kDa actin-binding protein, has potent actin filament-severing activity in vitro. To investigate the in vivo function of gelsolin, transgenic gelsolin-null (Gsn-) mice were generated and found to have normal embryonic development and longevity. However, platelet shape changes are decreased in Gsn- mice, causing prolonged bleeding times. Neutrophil migration in vivo into peritoneal exudates and in vitro is delayed. Gsn- dermal fibroblasts have excessive actin stress fibers and migrate more slowly than wild-type fibroblasts, but have increased contractility in vitro. These observations establish the requirement of gelsolin for rapid motile responses in cell types involved in stress responses such as hemostasis, inflammation, and wound healing. Neither gelsolin nor other proteins with similar actin filament-severing activity are expressed in early embryonic cells, indicating that this mechanism of actin filament dynamics is not essential for motility during early embryogenesis.

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Year:  1995        PMID: 7720072     DOI: 10.1016/0092-8674(95)90369-0

Source DB:  PubMed          Journal:  Cell        ISSN: 0092-8674            Impact factor:   41.582


  130 in total

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2.  Equilibria and kinetics of folding of gelsolin domain 2 and mutants involved in familial amyloidosis-Finnish type.

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Authors:  J L McGrath; E A Osborn; Y S Tardy; C F Dewey; J H Hartwig
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Authors:  E L Bearer; M T Abraham
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Review 6.  Degeneracy and complexity in biological systems.

Authors:  G M Edelman; J A Gally
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9.  Profilin I is essential for cell survival and cell division in early mouse development.

Authors:  W Witke; J D Sutherland; A Sharpe; M Arai; D J Kwiatkowski
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10.  VASP protects actin filaments from gelsolin: an in vitro study with implications for platelet actin reorganizations.

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