E-selectin binding peptide-polymer-drug conjugates and their selective cytotoxicity against vascular endothelial cells.

Abstract:

:The hypothesis that E-selectin on activated endothelial cells could be exploited to selectively target drug delivery systems to tumor vasculature was investigated. HPMA copolymer-doxorubicin (DOX) conjugates displaying the high affinity E-selectin binding peptide (Esbp, primary sequence DITWDQLWDLMK) as targeting ligand were synthesized and tested for their cytotoxicity and intracellular fate in human immortalized vascular endothelial cells (IVECs). The targeted copolymers displaying multiple copies of Esbp are bound to surface-associated E-selectin with affinity at the low nano-molar range, three orders of magnitude stronger than the free Esbp. In addition, the binding affinity of the HPMA-Esbp copolymers to E-selectin expressing IVECs was found to be 10-fold superior relative to non-targeted copolymers. Once bound, E-selectin facilitated rapid internalization and lysosomal trafficking of the copolymers. This lysosomotropism of HPMA-Esbp-bound DOX copolymers was then correlated with a 150-fold higher cytotoxicity relative to non-targeted HPMA-DOX conjugates. These findings strongly support the emerging role of E-selectin as a viable target for controlled drug delivery in cancer therapy.

journal_name

Biomaterials

journal_title

Biomaterials

authors

Shamay Y,Paulin D,Ashkenasy G,David A

doi

10.1016/j.biomaterials.2009.08.013

subject

Has Abstract

pub_date

2009-11-01 00:00:00

pages

6460-8

issue

32

eissn

0142-9612

issn

1878-5905

pii

S0142-9612(09)00844-8

journal_volume

30

pub_type

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