Polyurethane Microstructures for 2′-Deoxycytidinic Acid Delivery: Preparation and Preliminary Characterization

Author:

Jeleriu Roxana Maria1,Cavaloiu Bogdana12,Onofrei Lidia Manuela1,Borcan Florin3ORCID,Albulescu Ramona Carmen4,Puiu Maria56

Affiliation:

1. PhD School, Faculty of Medicine, Department of Microscopic Morphology, Genetics Discipline, Center of Genomic Medicine, “Victor Babes” University of Medicine and Pharmacy Timisoara, 2 E. Murgu, Sq., 300041 Timisoara, Romania

2. Department of Radiology, “Victor Gomoiu” Children’s Clinical Hospital, 21 Basarabia Blvd., 022102 Bucharest, Romania

3. Department I, Advanced Instrumental Screening Center, Faculty of Pharmacy, “Victor Babes” University of Medicine and Pharmacy, 2 E. Murgu Sq., 300041 Timisoara, Romania

4. Department XI (Pediatrics II), Faculty of Medicine, “Victor Babes” University of Medicine and Pharmacy Timisoara, 2 E. Murgu, Sq., 300041 Timisoara, Romania

5. Department II (Microscopic Morphology), Genetics Discipline, Center of Genomic Medicine, Faculty of Medicine, “Victor Babes” University of Medicine and Pharmacy Timisoara, 2 E. Murgu, Sq., 300041 Timisoara, Romania

6. Clinical Emergency Hospital for Children “Louis Turcanu”, Regional Center of Medical Genetics, 2 Dr. I. Nemoianu, 300011 Timisoara, Romania

Abstract

Background and Objectives: Nucleotide delivery has emerged as a noteworthy research trend in recent years because of its potential utility in addressing a range of genetic defects resulting in the presence of incorrect nucleotides. The primary goals of this research were to create and to characterize polyurethane microstructures, with the aim of utilizing them for nucleotide transport. Materials and Methods: Two samples were prepared using an aliphatic diisocyanate in reaction with a mixture of polyethylene glycol and polycaprolactone diol, where 2′-deoxycytidinic acid was used as the active agent and glycerol 1,2-diacetate was used as an enhancer of the aqueous solubility. The solubility, pH, size distribution, and surface charge of the samples were measured, and encapsulation efficacy and release, cell proliferation, and irritation tests on mouse skin were conducted. Results: The results showed almost neutral acidic–basic structures with a high heterogeneity, and a medium tendency to form clusters with non-cytotoxic and non-irritative potentials. Conclusions: Future research could explore the efficacy of this carrier in delivering other nucleotides, as well as investigating the long-term effects and safety of these microstructures in vivo.

Funder

University of Medicine and Pharmacy Timisoara, Romania

Publisher

MDPI AG

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