Amino-Quat-Primer Polymer stabilized Silica-Nanoparticle-Dispersions

Brandt, Miriam

10 November 2015

Enhancing the colloidal stability of nanoparticles dispersions, in order to extend the utilization time without any loss of performance, is desired. Prior works have confirmed the electrosteric stabilization of colloidal particles by so-called “amino-quat-primer” polymers, hyperbranched poly(ethylenimine) polymers containing amino groups and quaternized groups. In this work, a systematic investigation on the factors influencing the polymer-particle-interactions was carried out. Hence, aqueous silica-nanoparticle-dispersions were polymer-functionalized; their dispersions stability was studied using turbidity analysis; and the particle surface charge was examined employing electrophoretic measurements. Five key factors influencing the polymer-particle-interaction were defined, including: the polymer-particle-ratio, the degree of polymerization and the degree of functionalization of the polymer, the dispersion pH and the salt concentration. Alternatingly occurring areas of stable, unstable and again stable dispersions with an increasing polymer-particle-ratio occurred due to a charge reversal of bare, negatively charged to polymer-covered, positively charged particles. An additional area of unstable dispersions at very high polymer concentrations was assumed to arise from depletion forces of non-adsorbed free polymer. Stable, positively charged, polymer-covered silica nanoparticles were obtained for optimized conditions regarding the five key factors. After the dispersion stability enhancement, the new amino-functionalized surface could be used for further modifications, e.g. to result in a compatibility with a polymer matrix to fabricate highly functional polymer / inorganic hybrid materials.

hyperbranched poly(ethylenimine)

Amino-Quat-Primer

silica nanoparticles

dispersion

colloidal stability

surface modification

ddc:540

Mass Spectrometry Interfaced with Ion Mobility or Liquid Chromatography Separation for the Analysis of Complex Mixtures

Smiljanic, Danijela

06 December 2011

No description available.

Analytical Chemistry

non-covalent complexes

polyplexes, terplexes

ion mobility mass spectrometry

poly(ethylenimine)

LC-MS

Mechanisms of Cytotoxicity and Intracellular Trafficking for Gene Delivery Polymers

Grandinetti, Giovanna

18 August 2011

Herein, different polymer libraries were examined to determine the effect polymer structure has on intracellular events. The effect of different polyamine lengths in copolymers on cellular uptake, the effect of modifying end groups of trehalose-containing polymers on transfection efficiency, and the effect of different linker lengths between galactose and a hepatocyte-targeted polymer on transfection efficiency were studied. Furthermore, it was demonstrated that polymers with terbium chelated in their repeat units could potentially be used for Förster resonance energy transfer (FRET) studies to monitor pDNA release from the polymer. Much of the work in this dissertation focuses on elucidating the intracellular mechanisms of linear poly(ethylenimine) (PEI) and how it compares to poly(L-tartaramidopentaethylenetetramine) (T4) and poly(galactaramidopentaethylenetetramine) (G4), two poly(glycoamidoamine)s synthesized by our group. The long-term goal of this project is to develop structure-function relationships between polymers and pDNA delivery efficacy that will result in the rational design of safe, efficient vehicles for therapeutic nucleic acid delivery. Many polymers used as DNA delivery vehicles display high cytotoxicity. Often, the polymers with the highest transfection efficiency are the most toxic, as demonstrated herein by PEI and T4 with varying polymer lengths. Therefore, it was of interest to study how polymer structure influences mechanisms of cytotoxicity. To this end, studies on several mechanisms of cytotoxicity, including nuclear envelope permeabilization, were conducted. Longer polymers induced more cytotoxic responses than shorter ones, and it appears that hydroxyl groups in the repeat unit of polymers play a role in polyplex formation. This research has also led us to a potential link between transfection efficiency and cytotoxicity; the polymers with the highest transfection efficiency were also the most toxic, and were also able to induce the most nuclear envelope permeability. It is possible that these polymers' ability to permeabilize the nuclear envelope is what causes their high transfection efficiency and high toxicity. In addition, flow cytometry and confocal microscopy studies revealed that polymer structure plays a role in nuclear trafficking; poly(glycoamidoamine)s G4 and T4 more dependent on intracellular machinery than PEI. This research demonstrates the impact that changes in polymer structure have on intracellular mechanisms. / Ph. D.

structure-bioactivity relationship

poly(glycoamidoamine)s

poly(ethylenimine)

transfection

intracellular trafficking

toxicity

polymer

Non-viral DNA delivery

Gene Vectors with Fluorescence Tracking Capabilities

Angelopoulos, Sophia Despina

01 June 2022

No description available.

Chemistry

Biology

Physical Chemistry

Organic Chemistry

Polymers

Polymer Chemistry

gene vectors

gene therapy

TADF

thermally activated delayed fluorescence

poly(ethylenimine)

benzothiazole

blue emitting

polymers

lower critical solution temperature

dual-stimuli responsiveness