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Phase Change Dimethyldioctadecylammonium-Shelled Microdroplets as a Promising Drug Delivery System: Results on 3D Spheroids of Mammalian Tumor Cells
* These authors contributed equally
In This Article
Summary
Decafluoropentane microdroplets developed with a shell of dimethyldioctadecylammonium bromide exhibited an exceptional colloidal stability and an actractive biointerface. DDAB-MDs proved to be efficient drug reservoirs characterized by a high affinity to plasma membranes together with enhanced uptake and antitumor activity of Doxorubicin against human triple-negative breast cancer (MDA-MB-231) 3D model.
Abstract
Significant improvement of phase-change perfluorocarbon microdroplets (MDs) in the vast theranostic scenario passes through the optimization of the MDs composition with respect to synthesis efficiency, stability, and drug delivery capability. To this aim, decafluoropentane (DFP) MDs stabilized by a shell of dimethyldioctadecylammonium bromide (DDAB) cationic surfactant were designed. A high concentration of DDAB-MDs was readily obtained within a few seconds by pulsed high-power insonation, resulting in low polydisperse 1 µm size droplets. Highly positive ζ-potential, together with a long, saturated hydrocarbon chains of the DDAB shell, are key factors to stabilize the droplet and the drug cargo therein. The high affinity of the DDAB shell with cell plasma membrane allows for localized chemotherapeutics delivery by increasing the drug concentration at the tumor cell interface and boosting the uptake. This would turn DDAB-MDs into a relevant drug delivery tool exhibiting high antitumor activity at very low drug doses.
In this work, the efficacy of such an approach is shown to dramatically improve the effect of doxorubicin against 3D spheroids of mammalian tumor cells, MDA-MB-231. The use of three-dimensional (3D) cell cultures developed in the form of multicellular tumor spheroids (i.e., densely packed cells in a spherical shape) has numerous advantages compared to 2D cell cultures: in addition to have the potential to bridge the gap between conventional in vitro studies and animal testing, it will improve the ability to perform more predictive in vitro screening assays for preclinical drug development or evaluate the potential of off-label drugs and new co-targeting strategies.
Introduction
Drug-delivery vectors capable of ensuring high antitumor efficacy and reducing side effects are primary goals while remaining a severe chemical-pharmaceutical challenge1,2. To date, their progress is limited at first by the contrast of an insufficient in situ drug release and a critical level of nonspecific toxicity3,4,5. In recent years, several drug delivery systems have been implemented to improve the administration of anticancer agents, including liposomes, polymeric micelles, polymersomes
Protocol
NOTE: All the reagents and instruments are listed in the Table of Materials.
1. Fabricating and characterizing microdroplets
- Preparing Dox-loaded DDAB-MDs
- Dissolve the DDAB powder in ethanol to obtain a final concentration of 10 mM and a final volume of 1 mL. Prepare 1 mL of Dox stock solution dissolving 2 mg Dox powder in ethanol.
CAUTION: Dox is known to have acute oral toxicity, category 4 and carcinogenicity, category 1B. Us.......
- Dissolve the DDAB powder in ethanol to obtain a final concentration of 10 mM and a final volume of 1 mL. Prepare 1 mL of Dox stock solution dissolving 2 mg Dox powder in ethanol.
Representative Results
Dox@DDAB-MDs were developed according to protocol (Section 1) as schematically described in Figure 1. The obtained MDs are made of a monolayer of DDAB encapsulating the DFP core (Figure 1A). The cationic charge of DDAB and the sonication procedure avoid the formation of DDAB multilamellar layers stacked at the DFP and water interface23.
The CLSM micrograph (Figure 1B
Discussion
To improve the efficacy of anthracyclines as antitumor drugs, this work presents the formation of DDAB shelled PFC droplets encapsulating the chemotherapeutic drug doxorubicin (Dox) and the effect of such formulation interacting with the high aggressive triple-negative breast cancer cells, MDA-MB-231.
Building up of DOX@DDAB-MDs
Dox loaded MDs have been formulated by the insonation method with an extremely fast, well reproducible, user-friendly, and efficient protocol. T.......
Acknowledgements
This work has received funding from the European Union Horizon 2020 research and innovation program under grant agreement AMPHORA (766456).
....Materials
| Name | Company | Catalog Number | Comments |
| µ-Petri dish | Ibidi | 81156 | 35mm high, IbiTreat |
| 1,1,1,2,3,4,4,5,5,5-Decafluoropentane | Sigma-Aldrich | 138495-42-8 | b.p. 55°C |
| 12-well culture plate | Corning | ||
| 15 ml centrifuge tube | Falcon | 89039-664 | |
| 3D-Petri dishes 12:256 | Microtissues (Sigma-Aldrich) | Z764000-6EA | Small |
| 3D-Petri dishes 12:81 | Microtissues (Sigma-Aldrich) | Z764019-6EA | Large |
| 5%CO2 culture incubator, 37°C | Thermo Scienific | HERAcell 150i | |
| 50 ml centrifuge tube | Falcon | 352070 | |
| Biological safety cabinet, II level | |||
| Calcein | Sigma-Aldrich | ||
| Calcein-AM | Sigma-Aldrich | 148504-34-1 | 4mM stock solution in DMSO |
| cam sCMOS Andor Zyla 4.2 | Andor Instruments | ||
| Centrifuge Hettich Universal 320R | Hettich Lab. Technology | ||
| DAPI | SIgma-Aldrich | ||
| Dimethyldioctadecylammonium bromide powder | Sigma-Aldrich | 3700-67-2 | |
| DMEM (Dulbecco's Modified Eagle Medium) | Corning | 15-013-CV | |
| Doxorubicin hydrochloride | Sigma-Aldrich | 25316-40-9 | |
| DPBS (Dulbecco's Modified PBS) | Corning | 21-030-CV | pH 7,4 |
| Ethanol 70% | Sigma-Aldrich | ||
| EZ-C1 digital ecliplse | Nikon Instruments | Silver version 3.91 | |
| Fetal Bovine Serum (FBS) | Corning | 35-079-CV | |
| Goniometer BI-200SM | Brookhaven Instruments Corporations | ||
| Laser Ar+ | Spectra Physics | ||
| Laser He-Ne | Melles-Griot | ||
| L-Glutammine | Corning | 25-005-CI | |
| Mcroscope Nikon Eclipse Ti | Nikon Instruments | ||
| MDA-MB 231 cell line | ATCC | ||
| Microsoft Excel | Microsoft | ||
| Microplates reader Spark | Tecan group | ||
| NanoZetaSizer ZS | Malvern Instruments LTD | ||
| Neubauer improved chamber | 718605 | ||
| NIS Elements software | Nikon Instruments | AR 4.30 | |
| Pen/Strepto | Corning | 30-002-CI | |
| Photocorrelator BI-9000 AT | Brookhaven Instruments Corporations | 62927-1 | |
| Photometer HC120 | Brookhaven Instruments Corporations | N° 1275 | |
| Pipettors and tips, various size | Gilson | ||
| Propidium Iodide | SIgma-Aldrich | ||
| Serological pipets, various size | Corning | ||
| Solid-state laser | Suwtech Laser | N° 22368 | |
| T25 Flasks | Sarstedt | 83.3910.002 | |
| T75 Flasks | Sarstedt | 83.3911.002 | |
| Trypsin/EDTA 0.05% | EuroClone | ECB3052D | |
| Vibra-Cell VCX-400 | Sonics & Materials, inc | ||
| Water bath | 37°C |
References
- Aryal, S., Park, H., Leary, J. F., Key, J. Top-down fabrication-based nano/microparticles for molecular imaging and drug delivery. International Journal of Nanomedicine. 14, 6631-6644 (2019).
- Peng, Y., et al.
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