Dual-Drug Conjugated Glyco-Nanoassemblies for Tumor-Triggered Targeting and Synergistic Cancer Therapy

Tugba Gencoglu Katmerlikaya; Aydan Dag; Pınar Sinem Omurtag Ozgen; Busra Cetin Ersen

doi:10.1021/acsabm.2c00749

Dual-Drug Conjugated Glyco-Nanoassemblies for Tumor-Triggered Targeting and Synergistic Cancer Therapy

ACS Appl Bio Mater. 2022 Nov 21;5(11):5356-5364. doi: 10.1021/acsabm.2c00749. Epub 2022 Nov 8.

Authors

Tugba Gencoglu Katmerlikaya¹, Aydan Dag^{2

3}, Pınar Sinem Omurtag Ozgen^{4

5}, Busra Cetin Ersen⁶

Affiliations

¹ Department of Biotechnology, Institute of Health Sciences, Bezmialem Vakif University, 34093Istanbul, Turkey.
² Department of Pharmaceutical Chemistry, Faculty of Pharmacy, Bezmialem Vakif University, 34093Istanbul, Turkey.
³ Pharmaceutical Application and Research Center, Bezmialem Vakif University, 34093Istanbul, Turkey.
⁴ Department of Analytical Chemistry, School of Pharmacy, Istanbul Medipol University, 34810Istanbul, Turkey.
⁵ Department of Basic Pharmacy Sciences, Faculty of Pharmacy, Marmara University, 34854Istanbul, Turkey.
⁶ Department of Chemistry, Institute of Graduate Studies, Ankara Haci Bayram Veli University, 06900Ankara, Turkey.

PMID: 36346990
DOI: 10.1021/acsabm.2c00749

Abstract

Drug-conjugated nanoassemblies potentiate the efficiency of anticancer drugs through the advantages of high drug-loading capacity and passive/active targeting ability in cancer therapy. This study describes the synthesis of gemcitabine (Gem) and cisplatin (cisPt) dual-drug-functionalized glyco-nanoassemblies (GNs) for anticancer drug delivery systems. It also investigates the pH-triggered drug delivery of the conventional anticancer drug cisPt. A Gem-functionalized well-defined glycoblock copolymer backbone (P(iprFruMA-b-MAc)-Gem), which consists of fructose and methacrylic acid segments, was synthesized via a reversible addition-fragmentation chain transfer (RAFT) polymerization method. Following the hydrolysis of the protecting groups on the backbone copolymer, cisPt functionalization of P(FruMA-b-MAc)-Gem in aqueous media was carried out during the transformation of glycoblock polymers into self-assembled spherical glyco-nanoassemblies (GN3). Monodrug-functionalized glyco-nanoassemblies were also prepared either with Gem (GN1) or cisPt (GN2) to compare the synergetic effect of dual-drug conjugated glyco-nanoassemblies (GN3). The sizes of glyco-nanoassemblies GN1, GN2, and GN3 were found as 5.76 ± 0.64, 59.80 ± 0.13, and 53.80 ± 3.90 nm and dispersity (Đ) values as 0.476, 0.292, and 0.311 by dynamic light scattering (DLS) measurement, respectively. The in vitro studies revealed that the drug-free glyco-nanoassemblies are biocompatible at concentrations higher than 296 μg/mL. The drug-conjugated glyco-nanoassemblies (GN1 and GN2) exhibited in vitro cytotoxicity against human breast cancer cell lines of MDA-MB-231 comparable to free Gem and cisPt, illustrating an efficient drug release into the tumor environment. Additionally, GNs exhibited higher selectivity and preferential cellular internalization in MDA-MB-231 when compared to healthy cell lines of CCD-1079Sk. These dual-drug conjugated GNs can effectively enhance the killing of cancer cells and increase synergistic chemotherapy.

Keywords: cellular uptake; cisPt; gemcitabine; glyco-nanoassemblies; synergistic chemotherapy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Cisplatin / pharmacology
Drug Delivery Systems
Humans
Neoplasms*
Pharmaceutical Preparations
Polymers
Precipitating Factors

Substances

Pharmaceutical Preparations
Cisplatin
Polymers