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1. The Calcified Vasculature in Chronic Kidney Disease Secretes Factors that Inhibit Bone Mineralization

2. Diurnal variation of magnesium and the mineral metabolism in patients with chronic kidney disease

3. Effect of NAD+ boosting on kidney ischemia-reperfusion injury.

4. Effect of inhibition of CBP-coactivated β-catenin-mediated Wnt signalling in uremic rats with vascular calcifications.

5. Exogenous BMP7 in aortae of rats with chronic uremia ameliorates expression of profibrotic genes, but does not reverse established vascular calcification.

6. Roles of NAD

7. Hypomorphic expression of parathyroid Bmal1 disrupts the internal parathyroid circadian clock and increases parathyroid cell proliferation in response to uremia

8. MO553: Impact of the Internal Parathyroid Clock on the Regulation of Parathyroid Gene Expression

9. Chronic Kidney Disease–Induced Vascular Calcification Impairs Bone Metabolism

10. Roles of NAD+ in Acute and Chronic Kidney Diseases

11. Diurnal variation of magnesium and the mineral metabolism in patients with chronic kidney disease

12. Extrarenal expression of α-klotho, the kidney related longevity gene, in Heterocephalus glaber, the long living Naked Mole Rat

13. Effect of NAD+ boosting on kidney ischemia-reperfusion injury

14. A molecular circadian clock operates in the parathyroid gland and is disturbed in chronic kidney disease associated bone and mineral disorder

16. MO054VASCULAR CALCIFICATION IMPAIRS BONE MINERALIZATION

17. Anastomotic leak after surgery for colon cancer and effect on long‐term survival

18. Fibroblast Growth Factor (FGF) 23 Regulates the Plasma Levels of Parathyroid Hormone In Vivo Through the FGF Receptor in Normocalcemia, But Not in Hypocalcemia

19. Kidney fibroblast growth factor 23 does not contribute to elevation of its circulating levels in uremia

20. Circadian rhythm of activin A and related parameters of mineral metabolism in normal and uremic rats

21. Effect of inhibition of CBP-coactivated β-catenin-mediated Wnt signalling in uremic rats with vascular calcifications

22. Klotho and activin A in kidney injury: plasma Klotho is maintained in unilateral obstruction despite no upregulation of Klotho biosynthesis in the contralateral kidney

26. Exogenous BMP7 in aortae of rats with chronic uremia ameliorates expression of profibrotic genes, but does not reverse established vascular calcification

27. A potential kidney - bone axis involved in the rapid minute-to-minute regulation of plasma Ca2+

28. Parathyroid hormone-related peptide plasma concentrations in patients on hemodialysis

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