4.6 Article

Tunable Leuko-polymersomes That Adhere Specifically to Inflammatory Markers

Journal

LANGMUIR
Volume 26, Issue 17, Pages 14089-14096

Publisher

AMER CHEMICAL SOC
DOI: 10.1021/la1017032

Keywords

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Funding

  1. NCI NIH HHS [R01 CA115229, CA115229] Funding Source: Medline
  2. NHLBI NIH HHS [R01 HL085303, P01 HL018208] Funding Source: Medline
  3. NIBIB NIH HHS [R01 EB003457, EB003457] Funding Source: Medline

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The polymersome, a fully synthetic cell mimetic, is a tunable platform for drug delivery vehicles to detect and treat disease (theranostics). Here, we design a leuko-polymersome, a polymersome with the adhesive properties of leukocytes, which can effectively bind to inflammatory sites under flow. We hypothesize that optimal leukocyte adhesion can be recreated with ligands that mimic receptors of the two major leukocyte molecular adhesion pathways, the selectins and the integrins. Polymersomes functionalized with sialyl Lewis X and an antibody against ICAM-1 adhere avidly and selectively to surfaces coated with inflammatory adhesion molecules P-selectin and ICAM- I under flow. We find that maximal adhesion occurs at intermediate densities of both sialyl Lewis X and anti-ICAM- I, owing to synergistic binding effects between the two ligands. Leuko-polymersomes bearing these two receptor mimetics adhere under physiological shear rates to inflamed endothelium in an in vitro flow chamber at a rate 7.5 times higher than those to uninflamed endothelium. This work clearly demonstrates that polymersomes bearing only a single ligand bind less avidly and with lower selectivity, thus suggesting proper mimicry of leukocyte adhesion requires contributions from both pathways. This work establishes a basis for the design of polymersomes for targeted drug delivery in inflammation.

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