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1. Dual roles of mTORC1-dependent activation of the ubiquitin-proteasome system in muscle proteostasis

2. Distinct and additive effects of calorie restriction and rapamycin in aging skeletal muscle

3. Molecular and phenotypic analysis of rodent models reveals conserved and species-specific modulators of human sarcopenia

4. The neuromuscular junction is a focal point of mTORC1 signaling in sarcopenia

5. AIMTOR, a BRET biosensor for live imaging, reveals subcellular mTOR signaling and dysfunctions

6. mTORC1 signalling is not essential for the maintenance of muscle mass and function in adult sedentary mice

8. Distinct and additive effects of calorie restriction and rapamycin in aging skeletal muscle

9. Dual roles of mTORC1-dependent activation of the ubiquitin-proteasome system in muscle proteostasis

10. Molecular and phenotypic analysis of rodent models reveals conserved and species-specific modulators of human sarcopenia

11. mTORC1 signaling is not essential for the maintenance of muscle mass and function in adult sedentary mice

12. Regulation of glioma cell invasion by 3q26 gene products PIK3CA, SOX2 and OPA1

13. Regulation of Glioma Cell Invasion by 3q26 Gene Products PIK3CA, SOX2, and OPA1

14. Alterations to mTORC1 signaling in the skeletal muscle differentially affect whole-body metabolism

15. mTOR inactivation in myocardium from infant mice rapidly leads to dilated cardiomyopathy due to translation defects and p53/JNK-mediated apoptosis

16. Carboxy-Terminal Modulator Protein (CTMP) is a mitochondrial protein that sensitizes cells to apoptosis

17. eIF3-f function in skeletal muscles: To stand at the crossroads of atrophy and hypertrophy

18. The initiation factor eIF3-f is a major target for Atrogin1/MAFbx function in skeletal muscle atrophy

19. 0452 : MTOR inactivation during early postnatal development of mice myocardium leads to severe dilated cardiomyopathy due to altered translational efficiency and hypoxia-induced apoptosis

20. Mechanisms regulating neuromuscular junction development and function and causes of muscle wasting

21. Activation of mTORC1 in skeletal muscle regulates whole-body metabolism through FGF21

22. Degradation of MyoD Mediated by the SCF (MAFbx) Ubiquitin Ligase

23. Cyclin E–Cdk2 Phosphorylation Promotes Late G1-Phase Degradation of MyoD in Muscle Cells

24. Sustained Activation of mTORC1 in Skeletal Muscle Inhibits Constitutive and Starvation-Induced Autophagy and Causes a Severe, Late-Onset Myopathy

25. Myostatin inactivation increases myotube size through regulation of translational initiation machinery

26. The Carboxy-Terminal Modulator Protein (CTMP) regulates mitochondrial dynamics

27. PKB and the mitochondria: AKTing on apoptosis

28. MyoD undergoes a distinct G2/M-specific regulation in muscle cells

29. Protein kinase B/Akt at a glance

30. Critical role for lysine 133 in the nuclear ubiquitin-mediated degradation of MyoD

31. Dephosphorylation and subcellular compartment change of the mitotic Bloom's syndrome DNA helicase in response to ionizing radiation

32. Stabilization of MyoD by direct binding to p57(Kip2)

33. Differential response of skeletal muscles to mTORC1 signaling during atrophy and hypertrophy

34. The Translation Regulatory Subunit eIF3f Controls the Kinase-Dependent mTOR Signaling Required for Muscle Differentiation and Hypertrophy in Mouse

35. Sequential involvement of Cdk1, mTOR and p53 in apoptosis induced by the HIV-1 envelope

36. Mutant MyoD lacking Cdc2 phosphorylation sites delays M-phase entry

37. The translation regulatory subunit eIF3f controls the kinase-dependent mTOR signaling required for muscle differentiation and hypertrophy in mouse.

38. The Carboxy-Terminal Modulator Protein (CTMP) regulates mitochondrial dynamics.

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