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1. RSK3 switches cell fate: from stress-induced senescence to malignant progression

2. The mitochondrially-localized nucleoside diphosphate kinase D (NME4) is a novel metastasis suppressor

3. Surface tension of model tissues during malignant transformation and epithelial–mesenchymal transition

4. Case report: Changes in the levels of stress hormones during Takotsubo syndrome

5. Inverted Takotsubo Syndrome With HELLP Syndrome: A Case Report

6. Meningococcal purpura fulminans and severe myocarditis with clinical meningitis but no meningeal inflammation: a case report

7. An updated evaluation of serum sHER2, CA15.3, and CEA levels as biomarkers for the response of patients with metastatic breast cancer to trastuzumab-based therapies.

8. The advantage of channeling nucleotides for very processive functions [version 2; referees: 3 approved]

9. The advantage of channeling nucleotides for very processive functions [version 1; referees: 3 approved]

12. En marche vers une oncologie personnalisée : l’apport des techniques génomiques et de l’intelligence artificielle dans l’usage des biomarqueurs tumoraux circulants

13. Supplementary Figure 3 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

14. Supplementary Figure 11 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

15. Supplementary Tables 1-4, Figure Legends 1-2 from Nm23-H1 Suppresses Tumor Cell Motility by Down-regulating the Lysophosphatidic Acid Receptor EDG2

16. Data from Nm23-H1 Suppresses Tumor Cell Motility by Down-regulating the Lysophosphatidic Acid Receptor EDG2

17. Supplementary Figure Legends 1-11, Methods from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

18. Supplementary Figure 9 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

19. Supplementary Figure 7 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

20. Supplementary Figure 6 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

21. Supplementary Movie 2 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

22. Supplementary Figure 2 from Nm23-H1 Suppresses Tumor Cell Motility by Down-regulating the Lysophosphatidic Acid Receptor EDG2

23. Supplementary Figure 8 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

24. Supplementary Figure 5 from Implication of Metastasis Suppressor NM23-H1 in Maintaining Adherens Junctions and Limiting the Invasive Potential of Human Cancer Cells

25. Supplementary Figure 1 from Nm23-H1 Suppresses Tumor Cell Motility by Down-regulating the Lysophosphatidic Acid Receptor EDG2

26. Force tuning through regulation of clathrin-dependent integrin endocytosis

27. Metastasis-suppressor NME1 controls the invasive switch of breast cancer by regulating MT1-MMP surface clearance

28. Extracellular Vesicle-Mediated Metastasis Suppressors NME1 and NME2 Modify Lipid Metabolism in Fibroblasts

29. The Function of NM23-H1/NME1 and Its Homologs in Major Processes Linked to Metastasis

30. [Clinical use and evolution of circulating biomarkers in the era of personalized oncology: From protein markers to bioclinical scores]

31. Nucleoside diphosphate kinase D (NME4) is the first mitochondrial metastasis suppressor

32. Loss of the Metastasis Suppressor NME1, But Not of Its Highly Related Isoform NME2, Induces a Hybrid Epithelial–Mesenchymal State in Cancer Cells

33. Massive lactic acidosis and ketoacidosis with glucagon deficiency in a chronic alcoholic patient

34. The mitochondrially-localized nucleoside diphosphate kinase D (NME4) is a novel metastasis suppressor

36. The nucleoside diphosphate kinase NDK-1/NME1 promotes phagocytosis in concert with DYN-1/Dynamin

37. Meningococcal purpura fulminans and severe myocarditis with clinical meningitis but no meningeal inflammation: a case report

38. NME4 Loss-of-Function Alters Mitochondria, Triggers Retrograde Signaling and Leads to Cellular Reprogramming

39. An updated evaluation of serum sHER2, CA15.3, and CEA levels as biomarkers for the response of patients with metastatic breast cancer to trastuzumab-based therapies

40. The mitochondrial nucleoside diphosphate kinase (NDPK-D/NME4), a moonlighting protein for cell homeostasis

41. The NDPK/NME superfamily: state of the art

42. NME4/nucleoside diphosphate kinase D in cardiolipin signaling and mitophagy

43. The extracellular domain of Her2 in serum as a biomarker of breast cancer

44. Metastasis suppressor NM23 limits oxidative stress in mammals by preventing activation of stress-activated protein kinases/JNKs through its nucleoside diphosphate kinase activity

45. The advantage of channeling nucleotides for very processive functions

46. NDPK-D (NM23-H4)-mediated externalization of cardiolipin enables elimination of depolarized mitochondria by mitophagy

47. Nm23-H1 homologs suppress tumor cell motility and anchorage independent growth

48. NM23 et les genès Suppresseurs de métastases

49. Nm23-H1 Suppresses Tumor Cell Motility by Down-regulating the Lysophosphatidic Acid Receptor EDG2

50. Nm23/NDP kinases in hepatocellular carcinoma

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