Immunocamouflage of latex surfaces by grafted methoxypoly(ethylene glycol) (mPEG): Proteomic analysis of plasma protein adsorption

被引:0
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作者
Yevgeniya Le
Li Li
DunCheng Wang
Mark D. Scott
机构
[1] Canadian Blood Services,Centre for Blood Research
[2] University of British Columbia,Department of Pathology and Laboratory Medicine
[3] University of British Columbia,undefined
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关键词
PEGylation; immunocamouflage; iTRAQ; mass spectrometry; polystyrene latex; protein adsorption; proteomics; methoxypoly( ethylene glycol); polymer;
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摘要
Grafting of methoxypoly(ethylene glycol) (mPEG) to cells and biomaterials is a promising non-pharmacological immunomodulation technology. However, due to the labile nature of cells, surface-plasma interactions are poorly understood; hence, a latex bead model was studied. PEGylation of beads resulted in a density and molecular weight dependent decrease in total adsorbed protein with a net reduction from (159.9±6.4) ng cm−2 on bare latex to (18.4±0.8) and (52.3±5.3) ng cm−2 on PEGylated beads (1 mmol L−1 of 2 or 20 kD SCmPEG, respectively). SDS-PAGE and iTRAQ-MS analysis revealed differential compositions of the adsorbed protein layer on the PEGylated latex with a significant reduction in the compositional abundance of proteins involved in immune system activation. Thus, the biological efficacy of immunocamouflaged cells and materials is mediated by both biophysical obfuscation of antigens and reduced surface-macromolecule interactions.
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页码:191 / 201
页数:10
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