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3. Functionalized lipid nanoparticles for subcutaneous administration of mRNA to achieve systemic exposures of a therapeutic protein

8. pH-dependent structural transitions in cationic ionizable lipid mesophases are critical for lipid nanoparticle function

14. Lipid Nanoparticles Deliver the Therapeutic VEGFA mRNA In Vitro and In Vivo and Transform Extracellular Vesicles for Their Functional Extensions

19. The In VivoFate of Polycatecholamine Coated Nanoparticles Is Determined by a Fibrinogen Enriched Protein Corona

20. Lipid Nanoparticles Deliver the Therapeutic VEGFA mRNA In Vitro and In Vivo and Transform Extracellular Vesicles for Their Functional Extensions

21. Selecting Counterions to Improve Ionized Hydrophilic Drug Encapsulation in Polymeric Nanoparticles

24. Interaction Kinetics of Individual mRNA-Containing Lipid Nanoparticles with an Endosomal Membrane Mimic: Dependence on pH, Protein Corona Formation, and Lipoprotein Depletion

29. Quantitative intracellular retention of delivered RNAs through optimized cell fixation and immunostaining

30. Endosomal escape of delivered mRNA from endosomal recycling tubules visualized at the nanoscale

31. Quantitative intracellular retention of delivered RNAs through optimized cell fixation and immuno-staining

32. Apolipoprotein E Binding Drives Structural and Compositional Rearrangement of mRNA-Containing Lipid Nanoparticles

33. Screening of the binding affinity of serum proteins to lipid nanoparticles in a cell free environment

36. Apolipoprotein E Binding Drives Structural and Compositional Rearrangement of mRNA-Containing Lipid Nanoparticles

37. In silico prediction of drug solubility: 2: Free energy of solvation in pure melts

38. In silico prediction of drug solubility: 1: Free energy of hydration

39. Endosomal escape of delivered mRNA from endosomal recycling tubules visualized at the nanoscale

40. Quantitative intracellular retention of delivered RNAs through optimized cell fixation and immunostaining

41. Identification of RNA-binding proteins in exosomes capable of interacting with different types of RNA: RBP-facilitated transport of RNAs into exosomes

42. Successful reprogramming of cellular protein production through mRNA delivered by functionalized lipid nanoparticles

43. Nanocrystal formulations of a poorly soluble drug. 2. Evaluation of nanocrystal liver uptake and distribution after intravenous administration to mice

44. Secondary crystal nucleation:nuclei breeding factory uncovered

47. In Vivo Dog Intestinal Precipitation of Mebendazole : A Basic BCS Class II Drug

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