Prevailingly Cationic Agmatine-based Amphoteric Polyamidoamine As a Nontoxic, Nonhemolytic, and "stealthlike" DNA Complexing Agent and Transfection Promoter

Overview

Journal Biomacromolecules

Publisher American Chemical Society

Specialties Biochemistry
Biology
Molecular Biology

Date 2007 Mar 29

PMID 17388564

Citations 10

Authors

Paolo Ferruti

Jacopo Franchini

Marco Bencini

Elisabetta Ranucci

Gian Paolo Zara

Loredana Serpe

Luca Primo

Roberta Cavalli

Affiliations

Soon will be listed here.

Abstract

AGMA1, a prevailingly cationic amphoteric polyamidoamine obtained by polyaddition of (4-aminobutyl)guanidine (agmatine) to 2,2-bis(acrylamido)acetic acid, was studied as a potential DNA carrier and transfection promoter. Fluorescein-labeled AGMA1 was prepared by conjugation with fluorescein isothiocyanate and its cell uptake, blood permanence, and body distribution studied. In spite of its cationic character, AGMA1 is neither toxic nor hemolytic in the pH range 4.0-7.4, circulates for a long time in the blood without preferentially localizing in the liver, easily enters HT-29 cells, gives stable complexes with DNA, and is endowed with good transfection efficiency, suggesting the ability to transport in the cytoplasm a DNA payload without any measurable membranolytic activity. If compared with other transfection promoters, including polyamidoamines of different structures, AGMA1 is apparently endowed with a unique combination of desirable requirements for a nonviral DNA polymer carrier and warrants potential as a transfection agent in vivo.

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