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Artificial Cells Devised that Boost the Immune Response to Cancer

By Biotechdaily staff writers
Posted on 27 Mar 2008
Using artificial cell-like particles, biomedical engineers have created a rapid and efficient way to produce a 45-fold enhancement of T cell activation and expansion, an immune response crucial for a patient's ability to fight cancer and infectious diseases.

The artificial cells, developed by Dr. More...
Tarek Fahmy, assistant professor of biomedical engineering at Yale University (New Haven, CT, USA) and his graduate student Dr. Erin Steenblock, are made of a material typically used for biodegradable sutures. The investigators reported that the new method is the first "off-the-shelf” antigen-presenting artificial cell that can be tuned to target a specific disease or infection. "This procedure is likely to make it to the clinic rapidly,” said senior author Dr. Fahmy. "All of the materials we use are natural, biodegradable, [and] already have FDA [U.S. Food and Drug Administration] approval.”

The report was published in the advance online February 26, 2008, issue of the journal Molecular Therapy. Cancer, viral infections, and autoimmune diseases have responded to immunotherapy that boosts a patient's own antigen-specific T cells. In those earlier procedures, a patient's immune cells were harvested and then exposed to cells that stimulate the activation and proliferation of antigen-specific T-cells. The "boosted” immune cells were then infused back into the patient to attack the disease.

Limitations of these procedures include expensive and time-consuming custom isolation of cells for individual patients and the risk of adverse reaction to foreign cells, according to the Yale researchers. They also pointed to difficulty in obtaining and maintaining sufficient numbers of activated T-cells for effective therapeutic response.

In the new system, the outer surface of each particle is covered in universal adaptor molecules that serve as attachment points for antigens--molecules that activate the patient's T-cells to recognize and fight off the targeted diseases--and for stimulatory molecules. Inside of each particle, there are slowly released cytokines that further stimulate the activated T-cells to proliferate to as much as 45 times their original number.

"Our process introduces several important improvements,” said lead author Dr. Steenblock. "First, the universal surface adaptors allow us to add a span of targeting antigen and co-stimulatory molecules. We can also create a sustained release of encapsulated cytokines. These enhancements mimic the natural binding and signaling events that lead to T-cell proliferation in the body. It also causes a fast and effective stimulation of the patient's T-cells, particularly T-cells of the cytotoxic type important for eradicating cancer.”

"Safe and efficient T-cell stimulation and proliferation in response to specific antigens is a goal of immunotherapy against infectious disease and cancer,” said Dr. Fahmy. "Our ability to manipulate this response so rapidly and naturally with an ‘off the shelf' reproducible biomaterial is a big step forward.”

Dr. Fahmy was recently awarded a five-year U.S. National Science Foundation (NSF; Arlington, VA, USA) Career Award for work on this process and methods of engineering biomaterials to manipulate immune responses to fight cancer and other diseases. His application incorporates signals important for T-cell stimulation in biocompatible polymer particulates, and integrates all the signals needed for efficient T-cell stimulation.

According to the NSF, devices as such these offer ease and flexibility in targeting different types of T-cells, and are expected to lead to state-of-the-art improvements in the preparation of a new generation of therapeutic systems.


Related Links:
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