Topology of Surface Ligands on Liposomes: Characterization Based on the Terms, Incorporation Ratio, Surface Anchor Density, and Reaction Yield

Lee, Shang-Hsuan; Sato, Yusuke; Hyodo, Mamoru; Harashima, Hideyoshi

doi:10.1248/bpb.b16-00462

Cited by 12 publications

(12 citation statements)

References 49 publications

(71 reference statements)

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“…The discrepancy in the extent of in vivo MTX release can likely be attributed to different PEGylation methods used in the two studies. Previously, 5% PEG was incorporated into both HSPC and EYPC based PEG liposomes using the pre-insertion method, which led to about half of the PEG being oriented outward from the membrane and the rest toward the inside of the liposomes [23]. In the current study, 4% PEG was post-inserted, leading to PEG being present mainly on the outer side of the liposomes, with around 4.5% PEG presented on the surface and 0.5% PEG facing inwards, including the 1% PEG pre-inserted.…”

Section: Discussionmentioning

confidence: 99%

Targeted brain delivery of methotrexate by glutathione PEGylated liposomes: How can the formulation make a difference?

Gaillard

Lange

et al. 2019

European Journal of Pharmaceutics and Biopharmaceutics

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License: Article 25fa pilot End User Agreement This publication is distributed under the terms of Article 25fa of the Dutch Copyright Act (Auteurswet) with explicit consent by the author. Dutch law entitles the maker of a short scientific work funded either wholly or partially by Dutch public funds to make that work publicly available for no consideration following a reasonable period of time after the work was first published, provided that clear reference is made to the source of the first publication of the work. This publication is distributed under The Association of Universities in the Netherlands (VSNU) 'Article 25fa implementation' pilot project. In this pilot research outputs of researchers employed by Dutch Universities that comply with the legal requirements of Article 25fa of the Dutch Copyright Act are distributed online and free of cost or other barriers in institutional repositories. Research outputs are distributed six months after their first online publication in the original published version and with proper attribution to the source of the original publication. You are permitted to download and use the publication for personal purposes. All rights remain with the author(s) and/or copyrights owner(s) of this work. Any use of the publication other than authorised under this licence or copyright law is prohibited. If you believe that digital publication of certain material infringes any of your rights or (privacy) interests, please let the Library know, stating your reasons.

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Section: Discussionmentioning

confidence: 99%

Targeted brain delivery of methotrexate by glutathione PEGylated liposomes: How can the formulation make a difference?

Gaillard

Lange

et al. 2019

European Journal of Pharmaceutics and Biopharmaceutics

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“…In our methodology, the term 'incorporation ratio' is introduced as a parameter that reflects the accurate surface ligand density. 33) In Chart 1, to analyze the incorporation ratio of the inserted (functionalized) liposomes a post-insertion procedure was employed using plain liposomes with a 5-FAM-PEG 2000 -DSPE conjugate lipid (5-FAM conj. ), in which the liposomal surface was modified with a fluorescently labeled functionalized conjugate.…”

Section: Analysis Of Liposomal Surface Ligand Densitymentioning

confidence: 99%

“…The calculation was based on the assumption that the conjugates are exposed outward/inward from the membrane with a theoretical ratio 55/45 on the pre-inserted liposomes, i.e., incorporation ratio=(incorporated 5-FAM conj.×(55/100))/(lipids mixture+incorporated 5-FAM conj.). 33) Surprisingly, small differences in the incorporation ratios in eight different sizes of fractional liposomes suggested the absence of any size-dependency trend during the formation of pre-inserted liposomes. This result may be caused by homogeneous lipid constituents in the initial hydrated liposomes that form the liposomes during the sonication process.…”

Section: Incorporation Ratio Of Pre-inserted Liposomesmentioning

confidence: 99%

“…36) The parameter, 'incorporation ratio,' is introduced to define this density. 33) In an analysis of these ratios, our new discovery shows that when liposome size decreases, the incorporation ratio is not constant but rapidly increases. Since liposomes with smaller sizes promise to become more important in the near future, a significant underestimation of the incorporation ratio may be misleading and lead to erroneous conclusions regarding their bioactivities.…”

mentioning

confidence: 94%

“…[17][18][19][20][21][22][23][24][25][26][27][28][29][30][31][32] To address this issue, a method for estimating and calculating these values is needed and the liposomal preparation should be standardized, since these factors affect the density of the ligand on the surface of a particle. 33) Considering the clinical aspects of regulatory science (medicine), the characterization of liposomal surfaces guarantees the quality of a medical application. An accurate value for the surface ligand density provides an accurate assessment of the degree of binding affinity for a modified liposome.…”

mentioning

confidence: 99%

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Size-Dependency of the Surface Ligand Density of Liposomes Prepared by Post-insertion

Lee

Sato

Hyodo

et al. 2017

Biological & Pharmaceutical Bulletin

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In the active targeting of a drug delivery system (DDS), the density of the ligand on the functionalized liposome determines its affinity for binding to the target. To evaluate these densities on the surface of different sized liposomes, 4 liposomes with various diameters (188, 137, 70, 40 nm) were prepared and their surfaces were modified with fluorescently labeled ligand-lipid conjugates by the post-insertion method. Each liposomal mixture was fractionated into a series of fractions using size exclusion chromatography (SEC), and the resulting liposome fractions were precisely analyzed and the surface ligand densities calculated. The data collected using this methodology indicate that the density of the ligand on a particle is greatly dependent on the size of the liposome. This, in turn, indicates that smaller liposomes (75-40 nm) tend to possess higher densities. For developing active targeting systems, size and the density of the ligands are two important and independent factors that can affect the efficiency of a system as it relates to medical use.

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Liposomes as Targeted Drug‐Delivery Systems

Mundargi

Taneja

Hadia

et al. 2022

Targeted Drug Delivery

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Topology of Surface Ligands on Liposomes: Characterization Based on the Terms, Incorporation Ratio, Surface Anchor Density, and Reaction Yield

Cited by 12 publications

References 49 publications

Targeted brain delivery of methotrexate by glutathione PEGylated liposomes: How can the formulation make a difference?

Targeted brain delivery of methotrexate by glutathione PEGylated liposomes: How can the formulation make a difference?

Size-Dependency of the Surface Ligand Density of Liposomes Prepared by Post-insertion

Liposomes as Targeted Drug‐Delivery Systems

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