Integrin-targeted nano-sized polymeric systems for paclitaxel conjugation: a comparative study

Fecha de publicación: 01/01/2017

Autores de CIPF

Maria Jesus Vicent Docon

Autor

Participantes ajenos a CIPF

Eldar-Boock, A
Blau, R
Ryppa, C
Baabur-Cohen, H
Many, A
Kratz, F
Sanchis, J
Satchi-Fainaro, R

Grupos de Investigación

Laboratorio de Polímeros Terapéuticos

Jefe/a de Grupo

Maria Jesus Vicent Docon

Abstract

The generation of rationally designed polymer therapeutics via the conjugation of low molecular weight anti-cancer drugs to water-soluble polymeric nanocarriers aims to improve the therapeutic index. Here, we focus on applying polymer therapeutics to target two cell compartments simultaneously - tumour cells and angiogenic endothelial cells. Comparing different polymeric backbones carrying the same therapeutic agent and targeting moiety may shed light on any correlation between the choice of polymer and the anti-cancer activity of the conjugate. Here, we compared three paclitaxel (PTX)-bound conjugates with poly-l-glutamic acid (PGA, 4.9mol%), 2-hydroxypropylmethacrylamide (HPMA, 1.2mol%) copolymer, or polyethyleneglycol (PEG, 1:1 conjugate). PGA and HPMA copolymers are multivalent polymers that allow the conjugation of multiple compounds within the same polymer backbone, while PEG is a bivalent commercially available Food and Drug Administration (FDA)-approved polymer. We further conjugated PGA-PTX and PEG-PTX with the integrin alpha(v)beta(3)-targeting moiety RGD (5.5mol% and 1:1 conjugate, respectively). We based our selection on the overexpression of integrin alpha(v)beta(3) on angiogenic endothelial cells and several types of cancer cells. Our findings suggest that the polymer structure has major effect on the conjugate's activity on different tumour compartments. A multivalent PGA-PTX-E-[c(RGDfK)(2)] conjugate displayed a stronger inhibitory effect on the endothelial compartment, showing a 50% inhibition of the migration of human umbilical vein endothelial cell cells, while a PTX-PEG-E-[c(RGDfK)(2)] conjugate possessed enhanced anti-cancer activity on MDA-MB-231 tumour cells (IC50 = 20 nM versus IC50 300 nM for the PGA conjugate).

Datos de la publicación

ISSN/ISSNe:: 1061-186X, 1029-2330
Tipo:: Article
Páginas:: 829-844
DOI:: 10.1080/1061186X.2017.1358727
PubMed:: 28737432

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Métricas

Filiaciones

Eldar-Boock, A:: Tel Aviv Univ, Sackler Sch Med, Dept Physiol & Pharmacol, Tel Aviv, Israel
Blau, R:: Tel Aviv Univ, Sackler Sch Med, Dept Physiol & Pharmacol, Tel Aviv, Israel
Ryppa, C:: Tumor Biol Ctr, Freiburg, Germany
Baabur-Cohen, H:: Tel Aviv Univ, Sackler Sch Med, Dept Physiol & Pharmacol, Tel Aviv, Israel
Many, A:: Lis Matern Hosp, Sourasky Med Ctr, Tel Aviv, Israel
Vicent, MJ:: Ctr Invest Principe Felipe, Polymer Therapeut Lab, Av Eduardo Primo Yufera 3, E-46012 Valencia, Spain
Kratz, F:: Tumor Biol Ctr, Freiburg, Germany

CytRx Corp, Drug Discovery Branch, Engesserstr 4, D-79108 Freiburg, Germany
Sanchis, J:: Ctr Invest Principe Felipe, Polymer Therapeut Lab, Av Eduardo Primo Yufera 3, E-46012 Valencia, Spain

Monash Univ, Monash Inst Pharmaceut Sci, 399 Royal Parade, Parkville, Vic 3052, Australia
Satchi-Fainaro, R:: Tel Aviv Univ, Sackler Sch Med, Dept Physiol & Pharmacol, Tel Aviv, Israel