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1. OptiMo‐LDLr: An Integrated In Silico Model with Enhanced Predictive Power for LDL Receptor Variants, Unraveling Hot Spot Pathogenic Residues

2. Contribution of APOE Genetic Variants to Dyslipidemia

3. Cholesterol Efflux Efficiency of Reconstituted HDL Is Affected by Nanoparticle Lipid Composition

4. MLb-LDLr

5. Leu22_Leu23 Duplication at the Signal Peptide of PCSK9 Promotes Intracellular Degradation of LDLr and Autosomal Dominant Hypercholesterolemia

7. Contributors

8. The Arg499His gain-of-function mutation in the C-terminal domain of PCSK9

11. Molecular mechanisms of lipotoxicity-induced pancreatic β-cell dysfunction

12. LDLR variants functional characterization: Contribution to variant classification

13. Molecular mechanisms of lipotoxicity-induced pancreatic β-cell dysfunction

14. miR-27b Modulates Insulin Signaling in Hepatocytes by Regulating Insulin Receptor Expression

15. Fast SARS-CoV-2 detection protocol based on RNA precipitation and RT-qPCR in nasopharyngeal swab samples

16. Boosting Cholesterol Efflux from Foam Cells by Sequential Administration of rHDL to Deliver MicroRNA and to Remove Cholesterol in a Triple‐Cell 2D Atherosclerosis Model

17. A Systematic Approach to Assess the Activity and Classification of PCSK9 Variants

18. Mutation type classification and pathogenicity assignment of sixteen missense variants located in the EGF-precursor homology domain of the LDLR

19. Pathophysiology of Type 2 Diabetes Mellitus

20. Cholesterol Efflux Efficiency of Reconstituted HDL Is Affected by Nanoparticle Lipid Composition

21. Statin Treatment-Induced Development of Type 2 Diabetes: From Clinical Evidence to Mechanistic Insights

23. Familial Hypercholesterolemia: The Most Frequent Cholesterol Metabolism Disorder Caused Disease

24. p.(Asp47Asn) and p.(Thr62Met): non deleterious LDL receptor missense variants functionally characterized in vitro

25. The leucine stretch length of PCSK9 signal peptide and its role in development of autosomal dominant hypercholesterolaemia: unravelling the activities of P.LEU23DEL AND P.LEU22_LEU23DUP variants

26. Replacement of cysteine at position 46 in the first cysteine-rich repeat of the LDL receptor impairs apolipoprotein recognition

27. Validation of LDLr Activity as a Tool to Improve Genetic Diagnosis of Familial Hypercholesterolemia: A Retrospective on Functional Characterization of LDLr Variants

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