Hyaluronic Acid Coated Chitosan Nanoparticles Reduced the Immunogenicity of the Formed Protein Corona

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作者
Abdulaziz Almalik
Hicham Benabdelkamel
Afshan Masood
Ibrahim O. Alanazi
Ibrahim Alradwan
Majed A. Majrashi
Assim A. Alfadda
Waleed M. Alghamdi
Haitham Alrabiah
Nicola Tirelli
Ali H. Alhasan
机构
[1] National Center for Biotechnology,NorthWest Centre for Advanced Drug Delivery (NoWCADD), Division of Pharmacy and Optometry
[2] Life science and Environment Research Institute,undefined
[3] King Abdulaziz City for Science and Technology (KACST),undefined
[4] Proteomics Resource Unit,undefined
[5] Obesity Research Center,undefined
[6] College of Medicine,undefined
[7] King Saud University,undefined
[8] The National Center for Genomic Technology (NCGT),undefined
[9] Life science and Environment Research Institute,undefined
[10] King Abdulaziz City for Science and Technology (KACST),undefined
[11] Department of Pharmaceutical Chemistry,undefined
[12] College of Pharmacy,undefined
[13] King Saud University,undefined
[14] School of Health Sciences,undefined
[15] University of Manchester,undefined
来源
Scientific Reports | / 7卷
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摘要
Studying the interactions of nanoparticles (NPs) with serum proteins is necessary for the rational development of nanocarriers. Optimum surface chemistry is a key consideration to modulate the formation of the serum protein corona (PC) and the resultant immune response. We investigated the constituent of the PC formed by hyaluronic acid-coated chitosan NPs (HA-CS NPs). Non-decorated chitosan NPs (CS NPs) and alginate-coated chitosan NPs (Alg-CS NPs) were utilized as controls. Results show that HA surface modifications significantly reduced protein adsorption relative to controls. Gene Ontology analysis demonstrates that HA-CS NPs were the least immunogenic nanocarriers. Indeed, less inflammatory proteins were adsorbed onto HA-CS NPs as opposed to CS and Alg-CS NPs. Interestingly, HA-CS NPs differentially adsorbed two unique anti-inflammatory proteins (ITIH4 and AGP), which were absent from the PC of both controls. On the other hand, CS and Alg-CS NPs selectively adsorbed a proinflammatory protein (Clusterin) that was not found on the surfaces of HA-CS NPs. While further studies are needed to investigate abilities of the PCs of only ITIH4 and AGP to modulate the interaction of NPs with the host immune system, our results suggest that this proof-of-concept could potentially be utilized to reduce the immunogenicity of a wide range of nanomaterials.
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