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New class of synthetic vaccines explored

Date:
July 25, 2012
Source:
Arizona State University
Summary:
Biodesign immunologists are developing the first vaccine complex that could be delivered safely and effectively by piggybacking onto self-assembled, three-dimensional DNA nanostructures.
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In a quest to make safer and more effective vaccines, scientists at the Biodesign InstituteÒ at Arizona State University have turned to a promising field called DNA nanotechnology to make an entirely new class of synthetic vaccines.

In a study published in the journal Nano Letters, Biodesign immunologist Yung Chang joined forces with her colleagues, including DNA nanotechnology innovator Hao Yan, to develop the first vaccine complex that could be delivered safely and effectively by piggybacking onto self-assembled, three-dimensional DNA nanostructures.

"When Hao treated DNA not as a genetic material, but as a scaffolding material, that made me think of possible applications in immunology," said Chang, an associate professor in the School of Life Sciences and a researcher in the Biodesign Institute's Center for Infectious Diseases and Vaccinology. "This provided a great opportunity to try to use these DNA scaffolds to make a synthetic vaccine."

"The major concern was: Is it safe? We wanted to mimic the assembly of molecules that can trigger a safe and powerful immune response in the body. As Hao's team has developed a variety of interesting DNA nanostructures during the past few years, we have been collaborating more and more with a goal to further explore some promising human health applications of this technology."

The core multidisciplinary research team members also included: ASU chemistry and biochemistry graduate student and paper first author Xiaowei Liu, visiting professor Yang Xu, chemistry and biochemistry assistant professor Yan Liu, School of Life Sciences undergraduate Craig Clifford and Tao Yu, visiting graduate student from Sichuan University.

Chang points out that vaccines have led to the some of the most effective public health triumphs in all of medicine. The state-of-the-art in vaccine development relies on genetic engineering to assemble immune system stimulating proteins into virus-like particles (VLPs) that mimic the structure of natural viruses -- minus the harmful genetic components that cause disease.

DNA nanotechnology, where the molecule of life can be assembled into 2-D and 3-D shapes, has an advantage of being a programmable system that can precisely organize molecules to mimic the actions of natural molecules in the body.

"We wanted to test several different sizes and shapes of DNA nanostructures and attach molecules to them to see if they could trigger an immune response," said Yan, the Milton D. Glick Distinguished Chair in the Department of Chemistry and Biochemistry and researcher in Biodesign's Center for Single Molecule Biophysics. With their biomimicry approach, the vaccine complexes they tested closely resembled natural viral particles in size and shape.

As proof of concept, they tethered onto separate pyramid-shaped and branched DNA structures a model immune stimulating protein called streptavidin (STV) and immune response boosting compound called an adjuvant (CpG oligo-deoxynucletides) to make their synthetic vaccine complexes.

First, the group had to prove that the target cells could gobble the nanostructures up. By attaching a light-emitting tracer molecule to the nanostructures, they found the nanostructures residing comfortably within the appropriate compartment of the cells and stable for several hours -- -long enough to set in motion an immune cascade.

Next, in a mouse challenge, they targeted the delivery of their vaccine cargo to cells that are first responders in initiating an effective immune response, coordinating interaction of important components, such as: antigen presenting cells, including macrophages, dendritic cells and B cells. After the cargo is internalized in the cell, they are processed and "displayed" on the cell surface to T cells, white blood cells that play a central role in triggering a protective immune response. The T cells, in turn, assist B cells with producing antibodies against a target antigen.

To properly test all variables, they injected: 1) the full vaccine complex 2) STV (antigen) alone 3) the CpG (adjuvant) mixed with STV.

Over the course of 70 days, the group found that mice immunized with the full vaccine complex developed a more robust immune response up to 9-fold higher than the CpG mixed with STV. The pyramid (tetrahedral) shaped structure generated the greatest immune response. Not only was immune response to the vaccine complex specific and effective, but also safe, as the research team showed, using two independent methods, that no immune response triggered from introducing the DNA platform alone.

"We were very pleased," said Chang. "It was so nice to see the results as we predicted. Many times in biology we don't see that."

With the ability to target specific immune cells to generate a response, the team is excited about the prospects of this new platform. They envision applications where they could develop vaccines that require multiple components, or customize their targets to tailor the immune response.

Furthermore, there is the potential to develop targeted therapeutics in a similar manner as some of the new generation of cancer drugs.

Overall, though the field of DNA is still young, the research is advancing at a breakneck pace toward translational science that is making an impact on health care, electronics, and other applications.

While Chang and Yan agree that there is still much room to explore the manipulation and optimization of the nanotechnology, it also holds great promise. "With this proof of concept, the range of antigens that we could use for synthetic vaccine develop is really unlimited," said Chang.

The work was supported by funding from the Department of Defense and National Institutes of Health (National Cancer Institute, National Institute of Drug Abuse).


Story Source:

Materials provided by Arizona State University. Note: Content may be edited for style and length.


Journal Reference:

  1. Xiaowei Liu, Yang Xu, Tao Yu, Craig Clifford, Yan Liu, Hao Yan, Yung Chang. A DNA Nanostructure Platform for Directed Assembly of Synthetic Vaccines. Nano Letters, 2012; 120706095939006 DOI: 10.1021/nl301877k

Cite This Page:

Arizona State University. "New class of synthetic vaccines explored." ScienceDaily. ScienceDaily, 25 July 2012. <www.sciencedaily.com/releases/2012/07/120725100056.htm>.
Arizona State University. (2012, July 25). New class of synthetic vaccines explored. ScienceDaily. Retrieved December 23, 2024 from www.sciencedaily.com/releases/2012/07/120725100056.htm
Arizona State University. "New class of synthetic vaccines explored." ScienceDaily. www.sciencedaily.com/releases/2012/07/120725100056.htm (accessed December 23, 2024).

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