INTRODUCTION
Micro- and nano-sized magnetic support is a recently developed revolutionary technology
for bioseparation, especially for ligand fishing, protein, enzyme, DNA, RNA and cell
isolation or purification. Magnetic nanoparticles (MPs) are referred to by various
synonyms, such as magnetic beads (MB) or micro- and nano-sized magnetic beads. They
are also called ferrofluids or magnetic fluids, meaning colloidal suspensions of magnetic
particles in a liquid carrier. Generally, these particles are part of nanotechnology,
which can be defined as engineering of functional systems on a molecular scale. It
has the potential to create many new materials and devices with a wide range of applications
across the biomedical, chemical, electronic and mechanical fields.
Their superparamagnetic properties have opened promising new perspectives for their
application in several areas. The pioneering “medical” application in the treatment
of lymphatic nodes and metastases based on injecting “metallic particles” preheated
in a magnetic field was first published by Gilchrist et al. in 1957 (1). Since then,
magnetic particles have been modified by coating with antibodies, enzymes, proteins
or specific ligands that enable them to bind to other biologically active compounds
or receptors on the cell surface. In the last decade, magnetic particles have been
increasingly used as a promising technique for a wide spectrum of biomedical applications.
The number of publications presenting original studies on using magnetic beads is
increasing year by year (Fig. 1). The growing interest in the magnetic carrier is
focused on biochemistry, molecular biology and medical specialties. Because of the
superparamagnetic properties and micro- and nano-dimensions, magnetic nanoparticles
can be used to isolate any target and linked to various manual and automated applications
(2–4). Innovative research has produced a new application for magnetic nanoparticles
that carries an exciting biomedical and bioengineering potential, for instance, cell
molecule and nucleic acid separation, immunoassays, pathogen detection, protein purification,
gen mutation analysis and magnetic-force-based tissue engineering (5,6). Also, the
interest in the potential application of the magnetic technique in pharmacy is significantly
growing. It is currently being recognised that this magnetic nanotechnology could
play an important role in this area.
Fig. 1
The number of publications on the subject “Magnetic Beads” and “Biochemistry and Molecular
Biology, Medicine or Pharmacology, Toxicology and Pharmaceutics” identified by Scopus
(http://www.scopus.com/home.url).
DRUG DISCOVERY
The process of drug discovery in the modern scientific aspect is very complex. It
integrates many disciplines, including biotechnology, medicine and pharmacology. For
years, drug discovery has also focused on identification of unknown biomolecular interactions
with known targets. A number of established methods are used in evaluating the binding
of ligands/drugs to receptors and proteins, such as equilibrium dialysis, ultrafiltration,
ultracentrifugation, bioaffinity chromatography and other spectroscopic methods. Also,
the BIAcore system and surface plasmon resonance (SPR) are the two most popular recently
technologies for real-time biomolecule interaction analysis. Because of the different
modifications of multifunctional surface of the magnetic particles, these approaches
are practically useful in this area.
The objective of the recent study was to adapt immobilized human serum albumin (HSA)
onto the surface of magnetic beads for the purpose of “ligand fishing” (3). These
beads correctly isolated a known binder from a mixture of known compounds, and the
whole experiment was carried out manually using a magnet and automatically using the
Magtration System. Furthermore, the magnetic separation technique was extended to
the protein-ligand and protein–protein interaction using magnetic beads with immobilized
heat-shock protein 90α (Hsp90α) (2). The advantage of this system is that the Hsp90α-coated
magnetic beads can isolate interacting partners (ligand and proteins) from complex
mixtures and cellular extracts (e.g. from KU-812 cells) in less than 15 min, unlike
co-immunoprecipitation methods, which take several hours to recover the protein of
interest. Presently, the extension of the magnetic beads method to multiple complex
cellular extracts and complex plant extracts is being investigated. The most recent
study demonstrates that ligand fishing based on biological functionalised MB is an
effective and convenient way to identify and isolate bioactive small molecules from
botanical extracts (Camptotheca acuminata and Dioscorea nipponica), and the process
has a significant structure specifity (7,8).
Using a similar concept, protein-coated magnetic beads were used as a tool for a rapid
drug-protein binding study (4). Knowledge of serum protein binding behaviour as a
significant component of blood is very important for the rational use of drugs. An
extensive understanding of the ligand/drug-protein interaction may be of special importance
for the modelling of pharmacokinetics, including possible drug–drug interaction. In
this context, magnetic beads with immobilized HSA have been successfully used to determine
the affinity of known drugs for the protein (4). Moreover, the preliminary competition
experiments suggest that protein-coated magnetic beads can be employed in drug–drug
interaction studies. However, the validation of the proposed method is being investigated.
DRUG DELIVERY
Advances in many fields are converging to make the commercialisation of advanced drug
delivery concepts possible (6). Innovative drug delivery devices should protect labile
active ingredients, precisely control drug release kinetics, and minimise the release
of the drug to non-target sites.
The major advantage of ferromagnetic materials (Fe3O4) and maghemite (γ-Fe2O3) over
other materials with a high magnetic moment is the possibility for in vivo applications
(6). Other materials, such as cobalt and nickel, can cause oxidative stress or long-term
changes in enzyme kinetics. Hence, their use should be limited in biomedical applications.
The use of magnetic nanoparticles as drug carriers in targeted therapy provides huge
opportunities in cancer treatment, as the use of such carriers considerably reduces
the side effects of conventional chemotherapy. For drug targeting, they are able to
cumulate in desired locations within the body with the help of a magnet. In 1978,
magnetic particles were first applied as a new class of drug target. The tool was
based on albumin microspheres with entrapped Fe3O4 and doxorubicin. A novel carrier
system allowed for the accumulation of local chemotherapeutic agent which was comparable
to that achieved by the administration of a 100-fold higher dose of the drug. Other
results indicate that the new targeting system of specific drug delivery based on
the “magnetic granules” might be useful for local chemotherapy of oesophageal cancer
in rabbits administered via the oral route. Another interesting application has utilised
iron oxide nanoparticles covered by starch polymers which makes the ferrofluids tolerable
to healthy tissues and cells. The time-dependent distribution of the ferrofluids as
a carrier for mitoxantrone within the body was already investigated by labelling the
nanoparticles with radioactive isotope 59Fe (9). Also, electron microscope investigations
have shown that the ferrofluids do not only concentrate in the cancer tissue but also
penetrate into the tumour cells.
The use of magnetic beads can significantly improve hyperthermia cancer treatment.
This therapy involves raising the temperature of the target tissue to 43–46°C, which
increases its sensitivity to chemo- and radiotherapy and may additionally stimulate
activities of the host immune system (10). Magnetic hyperthermia relies on the introduction
of ferro- or superparamagnetic particles into the tumor tissue. Under an applied magnetic
field, magnetic energy is converted to thermal energy, which destroys cancer tissues.
Cancer-specific binding agents could include antibodies, hormones, and other exo-
and endogenous substances. Attaching these agents, such as estrogen, testosterone,
and thyroid hormones, to magnetic nanoparticles has promising implications for magnetic
fluid hyperthermia treatment (MFH) of breast, prostate, and thyroid cancer, respectively.
Recently, monoclonal antibodies to cancer cell surface antigens and modified viruses
that are able to bind with receptors on certain types of cancer cells are being considered
as novel potentially binding agents coupled with magnetic particles. This tool could
be successfully used to locate cancer cells and deliver chemotherapeutics directly
to “cancer” location at elevated temperatures.
A recent study published in Nature Nanotechnology reports for the first time target
aerosol delivery to the lung achieved with aerosol droplets comprising superparamagnetic
iron oxide nanoparticles in combination with a target-directed magnetic gradient field
(11). Standard therapy with cytotoxic drugs relies on the attainment of high drug
concentrations at the affected site, which is particularly difficult in lung cancer
(12). Thus, the novel and promising method could be used to accumulate effective drug
doses in the affected lung areas and reduce undesirable effects. As the in vitro study
has illustrated the enhanced deposition of high aspect ratio aerosols in the small
airways using magnetic field alignment, in a recent study, computational fluid dynamics
(CFD) simulations of magnetic aerosol transport and deposition were conducted and
compared with the experimental findings (13). The demonstrated excellent predictive
power of the CFD model suggests that inhalation delivery systems for in vivo selective
respiratory drug delivery can potentially be designed based on observable magnetic
and aerosol properties. The magnetic targeted carriers (MTCs) have also been proposed
and developed to submicron-sized ferromagnetic particle preparation containing relaxant
drugs for local anesthesia and improve targeting efficiency of pharmaceutical agents
in the treatment of carcinoma in rabbits (14).
Furthermore, recent clinical research shows that exposure to iron nanoparticles increases
endothelial cell permeability caused by oxidative stress resulting from reactive oxygen
material (15). This phenomenon offers fascinating opportunities for magnetic beads
in personalised cancer therapies.
CELL AND GENE THERAPY
Cell therapies are based on biological agents involving stem cells or immune cells
to be administered to patients for the treatment of several diseases. The development
of noninvasive imaging techniques to monitor cell migration to target tissues is of
particular importance for cell-based therapies. Monitoring magnetically labeled cells
with magnetic resonance imaging (MRI) has increased our understanding of cellular
migration and the pathophysiology of diseases in experimental models and in vivo (16).
Recently, the potential clinical application of anionic magnetic nanoparticles (AMNPs),
ultrasmall paramagnetic iron oxides (USPIOs) and superparamagnetic iron oxide nanoparticles
(SPIONs) has been demonstrated to visualise cell migration during MRI monitoring of
cellular therapies (17,18). These agents cause a strong source of contrast resulting
from the increased differences in signal intensities that each tissue produces in
response to the applied radio frequency pulses. Recent reports describe utilising
small contrast agents to track the migration of stem cells, immune cells and other
cells in numerous animal models of malignancy, angiogenesis, ischaemia, organ failure,
autoimmune diseases and transplantation rejection (17). Tracking labelled cells using
magnetic particles with MRI has clearly demonstrated its usefulness in evaluating
promising cell-based therapies in preclinical models. However, their translation to
the clinical practice is being considered in the near future (17).
The successful magnetic microsphere delivery approach has been used in gene therapy
to reduce the incidence of adverse events, particularly in the case of viral and retroviral
vectors. Gene therapy is a potential therapeutic tool that requires effective gene
delivery. However, the most common methods for delivering genes into cell is associated
with two potential dangers: oncogenesis and inflammation. This therapeutic strategy,
based on magnetic technology, is an alternative method of viral gene delivery. Moreover,
magnetic reporter genes inserted into cells result in expression of iron storage proteins
that can be detected by MRI. The novel approach for improving viral DNA delivery system
has been studied using modified cationic chitosan-coated iron oxide nanoparticles
(Nac-6-IOPs) (19). The advantage of this system is the reduction of viral doses, time
of infection and viral side effects. In another study, the enhancement of non-viral
gene transfer was achieved by Lipofectamine™ 2000 or cationic lipid 67 (GL67)/plasmid
DNA (pDNA) liposome complexes coupled with superparamagnetic particles (20). A novel
non-viral delivery system based on a polyethylenimine coated on the surface of bacterial
magnetic nanoparticles (BMPs) has been developed with high transfection efficiency
and low toxicity, which presents an attractive strategy for gene therapy and DNA vaccination
(21).
The nanoparticle technology is highly novel and offers many possibilities for future
development. Although the particles possess useful properties for biomedical applications,
they also carry potential health risks. Generally, the nanomaterials pose many new
questions on risk assessment that are not yet completely answered. Thus, a reliable
risk assessment related to human health and environment and safety evaluation of these
materials should be performed for all in vivo studies. In 2007, the Food and Drug
Administration issued a report to consider developing guidance for regulation of products
that contain nanoscale materials (22).