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1. Kinetic modeling of the plasma pharmacokinetic profiles of ADAMTS13 fragment and its Fc-fusion counterpart in mice

2. A Novel Isoform of Met Receptor Tyrosine Kinase Blocks Hepatocyte Growth Factor/Met Signaling and Stimulates Skeletal Muscle Cell Differentiation

3. Global hemostatic assay of different target procoagulant activities of factor VIII and factor IX

4. Spartan deficiency causes accumulation of Topoisomerase 1 cleavage complexes and tumorigenesis

5. Pten regulates spindle pole movement through Dlg1-mediated recruitment of Eg5 to centrosomes

6. Cyclin A2 is an RNA binding protein that controls Mre11 mRNA translation

7. Mitotic kinase cascades orchestrating timely disjunction and movement of centrosomes maintain chromosomal stability and prevent cancer

8. The PI3K–Akt mediates oncogenic Met-induced centrosome amplification and chromosome instability

9. The ERK-RSK1 activation by growth factors at G2 phase delays cell cycle progression and reduces mitotic aberrations

10. Hepatocyte growth factor at S phase induces G2 delay through sustained ERK activation

11. Parkin Regulates Mitosis and Genomic Stability Through Cdc20/Cdh1

12. Centrosome dynamics as a source of chromosomal instability

13. Cyclin B2 and p53 control proper timing of centrosome separation

14. p90 ribosomal S6 kinase 1 (RSK1) isoenzyme specifically regulates cytokinesis progression

15. The p90 ribosomal S6 kinase 2 specifically affects mitotic progression by regulating the basal level, distribution and stability of mitotic spindles

16. Co-treatment with hepatocyte growth factor and TGF-beta1 enhances migration of HaCaT cells through NADPH oxidase-dependent ROS generation

17. Modulation of E-cadherin by hepatocyte growth factor induces aggressiveness of gastric carcinoma

19. The PI3K–Akt mediates oncogenic Met-induced centrosome amplification and chromosome instability.

20. Cyclin A2 is an RNA binding protein that controls Mre11 mRNA translation.

21. A Novel Isoform of Met Receptor Tyrosine Kinase Blocks Hepatocyte Growth Factor/Met Signaling and Stimulates Skeletal Muscle Cell Differentiation.

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