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Your search keyword '"T-Lymphoma Invasion and Metastasis-inducing Protein 1"' showing total 17 results

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17 results on '"T-Lymphoma Invasion and Metastasis-inducing Protein 1"'

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1. Phosphorylation and activation of the Rac1 and Cdc42 GEF Asef in A431 cells stimulated by EGF

2. Rac2D57N, a dominant inhibitory Rac2 mutant that inhibits p38 kinase signaling and prevents surface ruffling in bone-marrow-derived macrophages

3. Nm23-H1 regulates contact inhibition of locomotion, which is affected by ephrin-B1

4. Tiam1-regulated osteopontin in senescent fibroblasts contributes to the migration and invasion of associated epithelial cells

5. The Rac activator Tiam1 prevents keratinocyte apoptosis by controlling ROS-mediated ERK phosphorylation

6. The RacGEF Tiam1 inhibits migration and invasion of metastatic melanoma via a novel adhesive mechanism

7. eNOS-derived nitric oxide regulates endothelial barrier function through VE-cadherin and Rho GTPases

8. Lamellipodia are crucial for haptotactic sensing and response.

9. A novel high-content analysis tool reveals Rab8-driven cytoskeletal reorganization through Rho GTPases, calpain and MT1-MMP.

10. Rab5 is required in metastatic cancer cells for Caveolin-1-enhanced Rac1 activation, migration and invasion.

11. eNOS-derived nitric oxide regulates endothelial barrier function through VE-cadherin and Rho GTPases.

12. Nm23-H1 regulates contact inhibition of locomotion, which is affected by ephrin-B1.

13. Tiam1-regulated osteopontin in senescent fibroblasts contributes to the migration and invasion of associated epithelial cells.

14. Phosphorylation and activation of the Rac1 and Cdc42 GEF Asef in A431 cells stimulated by EGF.

15. The Rac activator Tiam1 prevents keratinocyte apoptosis by controlling ROS-mediated ERK phosphorylation.

16. The RacGEF Tiam1 inhibits migration and invasion of metastatic melanoma via a novel adhesive mechanism.

17. Rac2D57N, a dominant inhibitory Rac2 mutant that inhibits p38 kinase signaling and prevents surface ruffling in bone-marrow-derived macrophages.

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