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ICAM-1 targeting, intracellular trafficking, and functional activity of polymer nanocarriers coated with a fibrinogen-derived peptide for lysosomal enzyme replacement

J Drug Target. 2017-02; 
GarnachoCarmen, MuroSi
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Peptide Synthesis … Methods Materials ICAM-1-targeting c3 peptide, whose sequence is derived from amino acids 117–133 of the fibrinogen gamma chain (NNQKIVNLKEKVAQLEA) [29], and a scrambled sequence peptide (c3S) were synthesised by GenScript (Piscataway, NJ) … Get A Quote

摘要

Enzyme replacement is a viable treatment for diseases caused by genetic deficiency of lysosomal enzymes. However, suboptimal access of enzymes to target sites limits this strategy. Polymer nanocarriers (NCs) coated with antibody against intercellular adhesion molecule 1 (ICAM-1), a protein overexpressed on most cells under disease states, enhanced biodistribution and lysosomal delivery of these therapeutics. Whether this can be achieved using more biocompatible ICAM-1-targeting moieties is unknown, since intracellular uptake via this route is sensitive to the receptor epitope being targeted. We examined this using polymer NCs coated with an ICAM-1-targeting peptide derived from the fibrinogen sequence. ... More

关键词

ICAM-1 targeting,Niemann–Pick disease,acid sphingomyelinase,enzyme replacement therapy,fibrinogen-derived peptide,lysosomal storage diseases,polymer nanocarr
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