A novel drug delivery system developed uses a synthetic-biological hybrid nanocapsule to fight against various diseases at the genetic level by targeting specific cells, reveals a new study. The hybrid offers a way to correct diseased //cells at the genetic level while at the same time leaving healthy cells alone to increase the effectiveness of treatments and reduce unwanted side effects.
‘The new drug delivery system is programmable and can combat the diseased cells at the genetic level without affecting the healthy cells.’"There's no one-size-fits-all delivery system," says Jessica Rouge, assistant professor of chemistry at UConn, and author of a new paper on the technology in Bioconjugate Chemistry. "The beauty of this system is that it is programmable, modular, and has the ability to rapidly integrate diverse peptide sequences. It can be tailored to combat new disease challenges as they emerge."
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The delivery platform, featured in the paper by Rouge and her research team, combines synthetic peptides, surfactants, and nucleic acids to form a nanocapsule that allows time-appropriate, enzyme-specific co-release of a given pharmaceutical and an oligonucleotide (DNA or RNA).
These findings build on Rouge's work to understand how enzymes and nucleic acids can be used in new ways to engineer highly specific and targeted responses in chemical and biological systems.
As part of this aim, Rouge has developed a unique linker technology to connect a synthetic drug delivery vehicle referred to as a nucleic acid nanocapsule (NAN) with a new peptide cross-linker approach.
The NAN enables both a small molecule drug and a nucleic acid - RNA or DNA - to be delivered to a cell. This combination generates a nanocapsule capable of shepherding genetic or pharmaceutical molecules to a target on or within a cell.
In Rouge's method, this release doesn't occur unless the peptide cross-linker is triggered by specific enzymes that cause the nanocapsule to deteriorate and eventually biodegrade.
For the current study, Rouge and her team conducted in vitro testing with two trigger enzymes often present in elevated concentrations in malignant cells - cathepsin B (an intracellular protease), and MMP9 (an extracellular protease).
Once synthesized using Rouge's system, the cathepsin B and MMP9 targeted nanocapsules, also called pep-NANs, successfully released their cargo when treated with their intended enzyme targets and under biologically relevant conditions. They showed no signs of biodegradation when treated with non-target enzymes, a key to proving that only the right enzymatic "key" can unlock the drug they carry.
Rouge and her team also tested whether or not drug release would be triggered when the pep-NANs came into contact with similar enzymes at various pH levels. They found that the pep-NANs remained intact unless pH levels specific to the target enzymes were present, indicating that the pH of the cellular environment can regulate the enzyme-specific cargo release.
Nanocapsules synthesized using Rouge's method were not unintentionally set off by enzymes similar to their target - a critical difference between the system Rouge developed and conventional pH-sensitive drug delivery approaches.
With standard therapies, delivery is rapid and total, and it is often insensitive to enzyme expression levels. It also increases the risk of over-medication, requires frequent dosing, and doesn't guarantee that the medication will reach affected cells.
With this systemic means of delivery often come widespread adverse effects that can sometimes be worse than the illness being treated - a fact that is particularly true in the case of chemotherapy, which is designed to kill cells but cannot distinguish between those that are healthy and those that are diseased.
Along with cancer applications, Rouge says she is focused on tailoring her lab's materials for other challenging diseases and disorders that don't currently have effective treatment options but which could benefit from her approach.
She is currently collaborating with researchers at UConn Health in Farmington and UConn's main campus in Storrs on several interdisciplinary projects that seek a better balance between short-term and long-term therapies, including treatment of optical neuropathies and asthma.
In one project, Rouge is collaborating with assistant professor of pathobiology and veterinary science Steven Szczepanek. Szczepanek's research focuses on disease pathology and vaccine development.
The pair will begin testing the in vivo efficacy of Rouge's drug delivery system for genetically silencing a key pro-inflammatory response in asthmatic mice later this month. The technology is patent pending and is being marketed to potential industry licensees.
"There is no question that joining forces with industry partners to leverage our unique resources and expertise helps transform discoveries from an invention to an innovation that benefits society," says Radenka Maric, UConn's vice president for research.
"We're committed to continuing to foster an entrepreneurial and industry-aware culture at the University to ensure UConn research has a positive impact on the health of Connecticut's citizens, as well as our economy."