Literature DB >> 34485684

The Combination of Morphology and Surface Chemistry Defines the Immunological Identity of Nanocarriers in Human Blood.

Michael P Vincent1, Nicholas B Karabin1, Sean D Allen2, Sharan Bobbala1, Molly A Frey2, Sijia Yi1, Yufan Yang1, Evan A Scott3.   

Abstract

Upon exposure to blood, a corona of proteins adsorbs to nanocarrier surfaces to confer a biological identity that interfaces with the immune system. While the nanocarrier surface chemistry has long been the focus of protein corona formation, the influence of nanostructure has remained unclear despite established influences on biodistribution, clearance, and inflammation. Here, combinations of nanocarrier morphology and surface chemistry are engineered to i) achieve compositionally distinct protein coatings in human blood and ii) control protein-mediated interactions with the immune system. A library of nine PEGylated nanocarriers differing in their combination of morphology (spheres, vesicles, and cylinders) and surface chemistry (methoxy, hydroxyl, and phosphate) are synthesized to represent properties of therapeutic and biomimetic delivery vehicles. Analysis by quantitative label-free proteomic techniques reveal that specific surface chemistry and morphology combinations adsorb unique protein signatures from human blood, resulting in differential complement activation and elicitation of distinct proinflammatory cytokine responses. Furthermore, nanocarrier morphology is shown to primarily influence uptake and clearance by human monocytes, macrophages, and dendritic cells. This comprehensive analysis provides mechanistic insights into rational design choices that impact the immunological identity of nanocarriers in human blood, which can be leveraged to engineer drug delivery vehicles for precision medicine and immunotherapy.

Entities:  

Keywords:  immunotherapy; morphology; nanocarrier; protein adsorption; rational design; surface chemistry

Year:  2021        PMID: 34485684      PMCID: PMC8411909          DOI: 10.1002/adtp.202100062

Source DB:  PubMed          Journal:  Adv Ther (Weinh)        ISSN: 2366-3987


  75 in total

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Review 5.  Employment of targeted nanoparticles for imaging of cellular processes in cardiovascular disease.

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7.  Aggregation behavior of poly(ethylene glycol-bl-propylene sulfide) di- and triblock copolymers in aqueous solution.

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9.  Effects of Protein Corona on Active and Passive Targeting of Cyclic RGD Peptide-Functionalized PEGylation Nanoparticles.

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Journal:  Mol Pharm       Date:  2018-10-01       Impact factor: 4.939

10.  The nanoparticle protein corona formed in human blood or human blood fractions.

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Authors:  Michael P Vincent; Trevor Stack; Amir Vahabikashi; Guorong Li; Kristin M Perkumas; Ruiyi Ren; Haiyan Gong; W Daniel Stamer; Mark Johnson; Evan A Scott
Journal:  ACS Appl Mater Interfaces       Date:  2021-07-07       Impact factor: 10.383

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