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Researchers Learn Why Immune System’s Watch Dogs Howl

A class of proteins known as toll-like receptors are the guard dogs of the immune system, sniffing out bacteria or viruses then rousing the rest of the immune system for attack. Because of their ability to activate the body’s defenses, toll-like receptors are a darling of drug developers. New research led by Brown University immunologist Wen-Ming Chu, M.D., identifies what protein alerts toll-like receptor 9, one of the most powerful guard dogs in the pack.

PROVIDENCE, R.I. [Brown University] — Toll-like receptors are the guard dogs of the immune system, sniffing out bacteria and viruses then activating the body’s immune system for an attack on these invaders.

Because of their ability to quickly activate the body’s defenses, toll-like receptors have recently become a darling of drug makers. One of the proteins in this class, toll-like receptor 9 or TLR9, can pick up a very specific scent – a snippet of DNA common in bacteria and viruses.

The idea for drug makers is to create DNA-based drugs containing these snippets, called CpG DNA. The drugs would get the guard dogs howling, which, in turn, would trip a fast immune response, causing the body to attack cancerous tumors or, if used as an ingredient in vaccines, bolster the assault on infectious diseases such as hepatitis B and C. CpG DNA could even be used to treat immune system disorders such as asthma and allergies.

To make these pills or vaccines, however, it would be helpful to know what gets the guard dogs howling. New research led by Brown University immunologist Wen-Ming Chu, M.D., has uncovered one of these molecular mechanisms – high-mobility group box 1 protein, or HMGB1, a protein released when infection occurs, when cells are damaged or when tissue is injured.

Chu and his team found a direct interaction between HMGB1 and TLR9. When the invader’s DNA is present, researchers found that TLR9 meets up with HMGB1. The combination occurs inside tiny cellular cargo boxes, with a long name: endoplasmic reticulum-Golgi intermediate compartments or ERGIC. In these boxes, researchers found, the proteins bind to form a complex. Formation of this complex sets off a biochemical cascade that triggers the body’s immune response.

When HMGB1 is absent from cells, researchers found, the body’s immune response is significantly delayed.

“We found out that HMGB1 acts an accelerator, quickly activating the body’s defenses,” Chu said. “What’s exciting is that drug makers might be able to use this knowledge to treat disease. CpG DNA and HMGB1 could be used together in a vaccine.”

Results of the research were published in the June issue of the journal Blood then highlighted in the July issue of Nature Reviews Immunology.

Chu is an assistant professor of medical science in Brown’s Department of Molecular Microbiology and Immunology. Other members of the research team from Brown include Stanimir Ivanov, Ana-Maria Dragoi, Xin Wang, Jennifer Louten, George Yap and Christine Biron, all from the Department of Molecular Microbiology and Immunology.

Corrado Dallacosta, Giovanna Musco, Giovanni Sitia and and Marco Bianchi from the San Raffaele Scientific Institute at San Raffaele University contributed, as did Yinsheng Wan of Providence College and Haichao Wang from North Shore-Long Island Jewish Health System.

The National Institute of Allergy and Infectious Diseases, the Department of Defense, and the Leukemia and Lymphoma Society funded the work.

Editors: Brown University has a fiber link television studio available for domestic and international live and taped interviews and maintains an ISDN line for radio interviews. For more information, call the Office of Media Relations at (401) 863-2476.

 
 
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