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1. Protocol for evaluating the effects of large gradient high magnetic fields on osteocyte function.

2. PTH 1-34 reduced apoptosis of MLO-Y4 osteocyte-like cells by activating autophagy and inhibiting ER stress under RPM conditions.

3. Connexin 43 Channels in Osteocytes Are Necessary for Bone Mass and Skeletal Muscle Function in Aged Male Mice.

4. Effect of High Static Magnetic Fields on Biological Activities and Iron Metabolism in MLO-Y4 Osteocyte-like Cells.

5. Osteocytic Connexin43 Channels Regulate Bone-Muscle Crosstalk.

6. Iron Overload-Induced Osteocyte Apoptosis Stimulates Osteoclast Differentiation Through Increasing Osteocytic RANKL Production In Vitro.

7. Blocking glucocorticoid signaling in osteoblasts and osteocytes prevents mechanical unloading-induced cortical bone loss.

8. Osteocytic connexin 43 channels affect fracture healing.

9. Biological responses of osteocytic connexin 43 hemichannels to simulated microgravity.

10. Blockage of hemichannels alters gene expression in osteocytes in a high magneto-gravitational environment.

11. Connexin 43 channels are essential for normal bone structure and osteocyte viability.

12. GeneChip expression profiling reveals the alterations of energy metabolism related genes in osteocytes under large gradient high magnetic fields.

13. Polycystin 2 is involved in the nitric oxide production in responding to oscillating fluid shear in MLO-Y4 cells.

14. Diamagnetic levitation causes changes in the morphology, cytoskeleton, and focal adhesion proteins expression in osteocytes.

15. Oscillatory fluid flow elicits changes in morphology, cytoskeleton and integrin-associated molecules in MLO-Y4 cells, but not in MC3T3-E1 cells.

16. Selection of suitable reference genes from bone cells in large gradient high magnetic field based on GeNorm algorithm.

17. Connexin 43 Channels in Osteocytes Regulate Bone Responses to Mechanical Unloading.

18. Connexin 43 Channels are Essential for Normal Bone Structure and Osteocyte Viability.

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