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17 results on '"Dalteparin metabolism"'

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1. Enhancement of vascularization and granulation tissue formation by growth factors in human platelet-rich plasma-containing fragmin/protamine microparticles.

2. Protamine neutralisation of low molecular weight heparins and their oligosaccharide components.

3. Fragmin/protamine microparticles as cell carriers to enhance viability of adipose-derived stromal cells and their subsequent effect on in vivo neovascularization.

4. Structural features of low-molecular-weight heparins affecting their affinity to antithrombin.

5. Fragmin/protamine microparticle-coated matrix immobilized cytokines to stimulate various cell proliferations with low serum media.

6. Anti-Xa activity after subcutaneous administration of dalteparin in ICU patients with and without subcutaneous oedema: a pilot study.

7. The factor IXa heparin-binding exosite is a cofactor interactive site: mechanism for antithrombin-independent inhibition of intrinsic tenase by heparin.

8. Human antithrombin III-derived heparin-binding peptide, a novel heparin antagonist.

9. The gelsolin/fragmin family protein identified in the higher plant Mimosa pudica.

10. Antithrombin binding of low molecular weight heparins and inhibition of factor Xa.

11. Physarum amoebae express a distinct fragmin-like actin-binding protein that controls in vitro phosphorylation of actin by the actin-fragmin kinase.

12. IL-12 is a heparin-binding cytokine.

13. Determination of low-molecular-weight heparins and their binding to protamine and a protamine analog using polyion-sensitive membrane electrodes.

14. In vivo phosphorylation of actin in Physarum polycephalum. Study of the substrate specificity of the actin-fragmin kinase.

15. The actin-binding properties of the Physarum actin-fragmin complex. Regulation by calcium, phospholipids, and phosphorylation.

16. Microfilament dynamics: regulation of actin polymerization by actin-fragmin kinase and phosphatases.

17. Control of actin assembly at filament ends.

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