Synthesis and transport potential study of A2B type double chain amphiphilic architectures

Author:

Aarti 1,Krishna 12,Syeda Saima3,Chandel Rishima3,Sharma Antara4,Shrivastava Anju3,Sharma Sunil K.1ORCID

Affiliation:

1. Department of Chemistry University of Delhi Delhi India

2. City University of New York New York New York USA

3. Department of Zoology University of Delhi Delhi India

4. University of Massachusetts Lowell Lowell Massachusetts USA

Abstract

AbstractThe inefficient delivery of drugs having low efficacy to their target sites is significantly hampering the treatment of many diseases and putting enormous pressure on the healthcare system. In this endeavor, the non‐ionic amphiphilic nanotransporters are drawing increasing attention over the past decades. Herein, we report the synthesis of a newer A2B type non‐ionic double chain amphiphilic nanotransporters by using dimethyl 5‐hydroxy isophthalate based central core prepared by propargylation followed by ester hydrolysis. The core was subsequently decorated with hydrophobic alkyl (C8/C20/perfluoro alkylated Cf8) chains via esterification. Monomethoxy polyethylene glycol (mPEG) moiety (Mn: 750/1000) was then incorporated by click chemistry approach to confer hydrophilicity. The aggregation behavior of synthesized non‐ionic amphiphiles in aqueous medium was evaluated by using dynamic light scattering (DLS) and fluorescence spectroscopy. The nanotransport potential of the synthesized amphiphiles was studied by using model hydrophobic guests, that is, the dye Nile red and the drugs nimodipine and curcumin by using ultraviolet–visible (UV/Vis) and fluorescence spectroscopic techniques. Evaluation of the viability of amphiphiles synthesized against HeLa cells showed them to be well tolerated up to the concentration studied. Stimuli responsive release of encapsulated Nile red from the inner core of amphiphile was successfully carried out in the presence of an immobilized enzyme Candida antarctica lipase (Novozym 435). In nutshell, the results obtained from this study may be instrumental in the design and development of promising nanotransporters for biomedical applications.

Publisher

Wiley

Subject

Polymers and Plastics

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