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1. Odd skipped-related 1 (Osr1) identifies muscle-interstitial fibro-adipogenic progenitors (FAPs) activated by acute injury.

2. Preface.

3. N-WASP is required for Amphiphysin-2/BIN1-dependent nuclear positioning and triad organization in skeletal muscle and is involved in the pathophysiology of centronuclear myopathy.

4. Defining skeletal muscle resident progenitors and their cell fate potentials.

5. Stem cells in the hood: the skeletal muscle niche.

6. Loss of a single allele for Ku80 leads to progenitor dysfunction and accelerated aging in skeletal muscle.

8. Identification and characterization of a non-satellite cell muscle resident progenitor during postnatal development.

9. Skeletal muscle phenotypically converts and selectively inhibits metastatic cells in mice.

10. Modulation of caspase activity regulates skeletal muscle regeneration and function in response to vasopressin and tumor necrosis factor.

11. Tumor necrosis factor-alpha inhibition of skeletal muscle regeneration is mediated by a caspase-dependent stem cell response.

12. Muscle cachexia is regulated by a p53-PW1/Peg3-dependent pathway.

13. Tumor necrosis factor-alpha gene transfer induces cachexia and inhibits muscle regeneration.

14. Embryonic deregulation of muscle stress signaling pathways leads to altered postnatal stem cell behavior and a failure in postnatal muscle growth.

15. TNFalpha inhibits skeletal myogenesis through a PW1-dependent pathway by recruitment of caspase pathways.

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