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Dive into the research topics where Nicholas A. Peppas is active.

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Featured researches published by Nicholas A. Peppas.


Bioengineering & Translational Medicine | 2018

Uptake and Function of Membrane-destabilizing Cationic Nanogels for Intracellular Drug Delivery

William B. Liechty; Rebekah L. Scheuerle; Julia E. Vela Ramirez; Nicholas A. Peppas

Abstract The design of intracellular drug delivery vehicles demands an in‐depth understanding of their internalization and function upon entering the cell to tailor the physicochemical characteristics of these platforms and achieve efficacious treatments. Polymeric cationic systems have been broadly accepted to be membrane disruptive thus being beneficial for drug delivery inside the cell. However, if excessive destabilization takes place, it can lead to adverse effects. One of the strategies used to modulate the cationic charge is the incorporation of hydrophobic moieties, thus increasing the hydrophobic content. We have demonstrated the successful synthesis of nanogels based on diethylaminoethyl methacrylate and poly(ethylene glycol) methyl ether methacrylate. Addition of the hydrophobic monomers tert‐butyl methacrylate or 2‐(tert‐butylamino)ethyl methacrylate shows improved polymer hydrophobicity and modulation of the critical swelling pH. Here, we evaluate the cytocompatibility, uptake, and function of these membrane‐destabilizing cationic methacrylated nanogels using in vitro models. The obtained results suggest that the incorporation of hydrophobic monomers decreases the cytotoxicity of the nanogels to epithelial colorectal adenocarcinoma cells. Furthermore, analysis of the internalization pathways of these vehicles using inhibitors and imaging flow cytometry showed a significant decrease in uptake when macropinocytosis/phagocytosis inhibitors were present. The membrane‐disruptive abilities of the cationic polymeric nanogels were confirmed using three different models. They demonstrated to cause hemolysis in sheep erythrocytes, lactate dehydrogenase leakage from a model cell line, and disrupt giant unilamellar vesicles. These findings provide new insights of the potential of polymeric nanoformulations for intracellular delivery.


Archive | 2009

METHOD AND PROCESS FOR THE PRODUCTION OF MULTI-COATED RECOGNITIVE AND RELEASING SYSTEMS

Nicholas A. Peppas; Barbara Ekerdt; Marta Gómez-Burgaz


Archive | 2008

Highly porous, recognitive polymer systems

Nicholas A. Peppas; Aditya Durgam


Archive | 2006

Polymer network compositions and associated methods

James Zachary Hilt; Mark E. Byrne; Nicholas A. Peppas


Archive | 2014

DELIVERY OF SMALL INTERFERING RNA AND MICRO RNA THROUGH MEMBRANE-DISRUPTIVE, RESPONSIVE NANOSCALLE HYDROGELS

Nicholas A. Peppas; William Liechty


Archive | 2003

NOVEL BIOMIMETIC POLYMER NETWORKS: DEVELOPMENT AND APPLICATION AS SELECTIVE RECOGNITION ELEMENTS FOR BIOMOLECULES AT THE MICRO-/NANOSCALE

J. Zachary Hilt; Mark E. Byrne; Nicholas A. Peppas


Archive | 2015

POLYMERS FOR DELIVERY OF FACTOR VIII AND/OR FACTOR IX

Nicholas A. Peppas; Sarena D. Horava


Archive | 2010

Mimetic Drug Delivery Systems for Release with Specific Molecular Triggers

Nicholas A. Peppas


Archive | 2017

DELIVERY OF SMALL INTERFERING RNA AND MICRO RNA THROUGH NANOGELS CONTAINING HYDROPHOBIC PSEUDO-PEPTIDES

Nicholas A. Peppas; William Liechty


Archive | 2016

HYDROGELS FOR DELIVERY OF THERAPEUTIC COMPOUNDS

Jennifer M. Knipe; Laura E. Strong; Nicholas A. Peppas

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Sarena D. Horava

University of Texas at Austin

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William Liechty

University of Texas System

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Aditya Durgam

University of Texas System

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Barbara Ekerdt

University of Texas System

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Heidi Culver

University of Texas System

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