Issue 21, 2021
From the journal:

Nanoscale Advances

Fabrication of self-assembled nanostructures for intracellular drug delivery from diphenylalanine analogues with rigid or flexible chemical linkers

Amutha Arul, ORCID logo a   Priya Rana,a   Kiran Das,b   Ieshita Pan,c   Debasish Mandal,d   Adele Stewart,e   Biswanath Maity,*b   Soumyajit Ghosh ORCID logo *a  and  Priyadip Das ORCID logo *a  

* Corresponding authors

a Department of Chemistry, SRM Institute of Science and Technology, SRM Nagar, Potheri, Kattankulathur, Tamil Nadu-603203, India
E-mail: priyadipcsmcri@gmail.com, priyadip@srmist.edu.in, soumyajitghosh89@gmail.com

b Centre of Biomedical Research, Sanjay Gandhi Post-Graduate Institute of Medical Sciences (SGPGI) Campus, Raebareli Road, Lucknow, Uttar Pradesh 226014, India
E-mail: bmaity28@gmail.com

c Department of Biotechnology, Saveetha School of Engineering, Saveetha Institute of Medical and Technical Sciences, Saveetha University, Tamil Nadu 602105, India

d School of Chemistry and Biochemistry, Thapar Institute of Engineering and Technology, Bhadson Rd, Adarsh Nagar, Prem Nagar, Patiala, Punjab 147004, India

e Department of Biomedical Science, Charles E. Schmidt College of Medicine, Florida Atlantic University, Jupiter, FL 33458, USA

Abstract

Self-assembly of molecular building blocks is a simple and useful approach to generate supramolecular structures with varied morphologies and functions. By studying the chemical properties of the building blocks and tuning the parameters of their self-assembly process, the resultant supramolecular assemblies can be optimized for the required downstream applications. To this end, in the present study we have designed and synthesized three different molecular building blocks composed of two diphenylalanine (FF) units connected to each other through three different linkers: ethylenediamine, succinic acid, or terephthalaldehyde. Under identical conditions, all the three building blocks self-assemble into supramolecular architectures with distinct morphologies. However, by varying the polarity of the self-assembly medium, the nature of the non-covalent interactions changes in such a way as to generate additional self-assembled structures unique to each building block. Utilizing microscopic and spectroscopic techniques, we characterized the morphological variety generated by each building block/linker combination. These data represent the first report analysing the diversity of nanostructures that can be generated from identical dipeptide-based molecular backbones simply by varying the chemical linker. We also demonstrate that the spherical assemblies and nanorod structures fabricated from these dipeptide/linker pairs can act as drug delivery systems. More specifically, the spherical assembly generated by two FF dipeptides linked via ethylenediamine and nanorods fabricated from terephthalaldehyde linked FF dipeptides were able to encapsulate the cancer chemotherapeutic agent doxorubicin (DOX) and chaperone the drug into cells. Thus, these supramolecular assemblies represent a new platform for the development of efficient and effective intracellular drug delivery systems.

Graphical abstract: Fabrication of self-assembled nanostructures for intracellular drug delivery from diphenylalanine analogues with rigid or flexible chemical linkers

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Article information

DOI
https://doi.org/10.1039/D1NA00510C
Article type
Paper
Submitted
29 Jun 2021
Accepted
30 Aug 2021
First published
30 Aug 2021
This article is Open Access
Creative Commons BY-NC license

Nanoscale Adv., 2021,3, 6176-6190

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Fabrication of self-assembled nanostructures for intracellular drug delivery from diphenylalanine analogues with rigid or flexible chemical linkers

A. Arul, P. Rana, K. Das, I. Pan, D. Mandal, A. Stewart, B. Maity, S. Ghosh and P. Das, Nanoscale Adv., 2021, 3, 6176 DOI: 10.1039/D1NA00510C

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