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Hpv Cervical Cancer Vaccine

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While preparing a lecture in biochemistry and virology for his graduate students at the University of Alberta in the early 1980s, Dr. Lorne Tyrrell ran across a study just published in the medical journal, Cell. The research by William Mason and Jesse Summers, entitled “Replication of Hepatitis B,” discussed their study of the hepatitis B virus in infected duck liver.

After studying their duck model theory, Tyrrell speculated if the hepatitis B virus (HBV) might be susceptible to antiviral agents, and consulted with a colleague, who specialized in nucleoside chemistry. Both medical professors became excited about the possibility of inhibiting the HBV virus with nucleoside analogues. Thus began the infectious disease specialist's first leg of a journey, which led to the use of lamivudine as a therapy for chronic HBV infections.

More than 350 million people across the world, especially in Asia, now had new hope, some for their lifelong infections contracted vertically at birth from their mothers. In 2003, the Center for Disease Control estimated 73,000 Americans were infected with HBV, and about 5,000 die each year from sickness caused by HBV. It is reportedly 100 times more contagious than the AIDS virus. Many in North America, who had been infected with the virus from sexual transmission or intravenous drug use, were offered a potentially life-saving therapy.

Licensed in 1998, lamivudine is now used in 120 countries as a standard therapy for chronic HBV carriers. The compound is also used in combination with other drugs, such as protease inhibitors, for HIV therapy. Development rights were licensed to Glaxo Wellcome in 1990, which is now sold under the brand name Epivir®. For his pioneering efforts in developing the antiviral agent, Dr. Tyrrell was awarded the gold medal by the Canadian Liver Foundation and the Canadian Association for the Study of Liver in 2000. In 2005, he won the prestigious EnCana Principal Award for his development of the first effective oral medication for Hepatitis B.

HIS UNANSWERED QUESTIONS LAUNCHED A NEW HBV INVESTIGATION

Despite the awards and recognition, questions remained for Dr. Tyrrell about the shortcomings of lamivudine. He was troubled that some viruses would develop resistance to the compound. “I was disappointed the sustained viral response was not complete,” Tyrrell told us. In April 2003, the Journal of Antimicrobial Chemotherapy published a study in Japan showing, “long-term (lamivudine) therapy is associated with increased emergence of lamivudine-resistant strains of HBV.” Researchers concluded in this study, “The therapeutic challenge to effectively treat chronic HBV infection continues.”

Having screened lamivudine for use in Hepatitis B at Glaxo's research lab at the University of Alberta, Dr. Tyrrell was able to observe the immune response of various HBV patients. “What really got me interested in doing more work in this area was that we noticed patients, who have an immune response to the virus and take lamivudine, will have a better sustained response rate,” Tyrrell explained. “A patient with elevated liver transaminases taking lamivudine had a higher probability of a sustained viral response,” Tyrrell said with excitement in his voice. “In a patient with normal liver enzymes, who gets lamivudine, the virus will go down, but as soon as you stop the therapy, the virus comes right back up.” He told us the sustained viral response is only about two to three percent. Only about 30 percent remain free of the virus, about one year after patients have stopped taking lamivudine.

“How do you break tolerance?” Tyrrell asked himself, hoping to develop a way to stimulate an immune response. All of the patients, he had observed, seemed to be tolerant of the hepatitis B virus. He pondered the dilemma, “Was there some way to break tolerance to hepatitis B by stimulating the immune response?” Tyrrell studied what others were attempting and wasn't satisfied with the approaches others were taking to stimulate immune response. His ViRexx Medical research team brainstormed about different ways to target the antigen into the dendritic cells.

“That's where we came in with the Chimigen™ technology,” Tyrrell said. “The dendritic cells have receptors on their surface that will bind the Fc portion of an antibody.” He pointed out a key feature of the Chimigen™ platform, “We used the Fc portion of a murine (mouse) antibody to hook onto our hepatitis B antigens. This would direct the viral antigens into dendritic cells in vivo.” Because the dendritic cells are the sentries of the immune system, they guard what comes in. Recognizing a ‘foreign situation' in the murine antibody, it treats the whole molecule including the virus antigen as foreign.

LINK RECOGNITION MAY HOLD THE KEY

Dr. Rajan George, ViRexx Medical's vice president of research and development, told us, “The dendritic cells chop up this protein into small pieces called peptides, also known as epitopes. The dendritic cells have a system where they put the T-cell epitope on another protein, MHC Class I, and bring it to the surface of the dendritic cell. They are presented as a complex on the surface of the dendritic cell to attract the T-cells.” When the T-cells arrive to inspect the foreign entity, the cytotoxic T-cells are activated. Then, they begin attacking and killing the virus-infected cells.

Research at Tokyo's Cancer Institute Hospital, published in 1987 in Nippon Sanka Fujinka Gakkai Zasshi, suggested a feasibility of linked recognition of a virus antigen as a helper in tumor immunity with a target antigen. In the case of ViRexx Medical, Tyrrell's team has created a new molecule, called “chimigen.” The term is shorthand for a chimeric antigen, meaning it is an antigen created from two different sources, part virus and part murine monoclonal antibody.

Dr. Tyrrell's work at ViRexx Medical with Dr. George suggested the linked-recognition theory might be the key to breaking tolerance. Dr. George emphasized, “The new ‘chimigen' stimulates an immune response to the antigen as well as the viral antigen. This is very important because the virus antigen was previously being ignored.” That brings us back to why lamivudine had limited success. The immune systems of some HBV carriers failed to recognize the viral infection as a threat to the body. Tyrell's ViRexx Medical research team hopes the body's immune system sees the threat, thus stimulating the immune system, and breaking tolerance. It appears Dr. Tyrell may soon find out whether or not the questions he asked will bring the answers he hoped for.

END OF PART ONE

Hpv Cervical Cancer Vaccine

In late April, ViRexx Medical, for which Dr. Tyrrell serves as the Chief Executive, received authorization from Health Canada, the country's regulatory arm which is similar in nature to the U.S. Food and Drug Administration, to undertake a Phase I clinical trial for its lead Chimigen? platform vaccine candidate, HepaVaxx B. Dr. Tyrrell hopes it might become a potential treatment for chronic carriers of the hepatitis B virus. Tyrrell told StockInterview, "The platform is designed to try to get both a T and B cell response. Most conventional vaccines induce just a B cell response."

STIMULATING BOTH ARMS OF THE IMMUNE SYSTEM

It is the dendritic cells, which stimulate the B-Lymphocytes and produce antibodies. For example, the mumps vaccine was designed to give a B cell response, providing someone with good protection for a number of years. As Dr. Rajan George had told us, "The B-Cells produce antibodies against the virus antigen, which we have put in the Chimigen? vaccine. The antibodies are specific to the antigen and bind to the viruses because they have the antigen. The system removes the virus by binding with the antibody." The platform is also expected to remove the infected cells using cytotoxic T-lymphocytes.

The big breakthrough in treating many infectious, and other, diseases would come with the vaccine platform capable of stimulating both a T and B cell response. "It would be a major step forward," Tyrrell noted, "if we could find a way to increase the efficiency of some of these therapeutic vaccines." ViRexx Medical's infectious disease department conducted a number of ex vivo laboratory experiments to evaluate the immune responses the Chimigen? platform might produce. "We showed what we had predicted in theory has been true," Dr. George told us. "We have also done some animal experiments, where the vaccine showed similar effects, again, as predicted. For HepaVaxx B, the animal results are also showing great progress and promise." Tyrrell is more reserved in his expectations, "Let's see how the platform works when tested in humans. If this can be used to stimulate both a T and B cell response, then it would be a significant breakthrough."

There could be stumbling blocks ahead. A chronic hepatitis B carrier is exposed to a number of antigens in his or her body. Tyrrell has further concerns which may arise. Perhaps the antigen might not trigger a strong enough response. Or something may be discovered during the Phase I trials, such as "Are there regulatory T cells, or cells that are being paralyzed and not being allowed to stimulate a strong immune response in these patients? That is why one tests in humans after successful animal tests, to address those points of interest. As Dr. George reminded us, "Until then, our optimism is based on laboratory results."

Tyrrell has already begun thinking a few steps into the future, "I really believe we've found a way of directing the right immune response chimigens, but we may have to use adjuvants to get a strong immune response." Adjuvants are immunological agents designed to induce the production of antibodies. "We haven't used the platform with an adjuvant to get an even stronger response," explained Tyrrell. For example, nucleotidesis, the short nucleotide sequences which are rich in CpG, or growth factors, such as cytokines, can enhance the immune response.

DEVELOPING A CLASS OF FLEXIBLE VACCINES?

Ever the optimist, Tyrrell outlined his strategy, "Our plan is to go with one or two antigens first and see that we get the appropriate immune response. If we do, then we will be looking at other antigens, not only from viruses, but we can be looking at cancer antigens in this platform." Dr. George echoed Tyrrell's sentiment, "We should be able to use this platform for cancer therapy, depending upon the cancer antigen we use. We can plug in a specific cancer antigen into this platform, and the vaccine targeted to dendritic cells." The company has also been evaluating some bioterrorist viruses in conjunction with an arm of Canada's Defense Department. Dr. George also pointed out, "Our chimigen technology is not found anywhere outside of our laboratories. This approach has not been tried before for chronic HBV or HCV infections." Because the scientists believe the Chimigen? platform is one which may be flexible and adaptable for the treatment of both infectious viruses and cancers, a new class of vaccines may be developed over the coming decade.

While awaiting the results of the initial human clinical trials, Dr. Tyrrell did reach a very definite conclusion about the mission in his journey, "Unless you have both arms of the immune system, you may not have lifelong immunity." Tyrrell's down-to-earth thinking may have come from being born on a farm in rural Alberta, west of Edmonton, the big city where his college alma mater can be found. At one time, he had considered becoming a rural family physician or a veterinarian. His erstwhile aspiration to work with animals is ironic, because his research has involved virally infected duck models, chimps who love the taste of Tang?, and mouse antibodies. But Tyrrell's curiosity to solve complex scientific riddles has taken him beyond those once-simple goals.

His competitive drive for milestones was first evidenced by winning a gold medal in science, while an undergraduate majoring in chemistry at the University of Alberta. An then, with an award of a New York Life insurance scholarship, during his second year in medical school, for a combined MD/PhD. Only twenty-two medical students in North American won such a scholarship that year. Or perhaps he hoped where his journey might someday take him, when he won an MRC Centennial fellowship to study virology, for two years, at the Karolinska Institute in Stockholm. For those unfamiliar with this Swedish institute, it is the home of the Nobel Prize. Is this where Dr. Lorne Tyrrell's journey might one day reach its final destination? The answer to this question may come from the results of the clinical trials for his Chimigen? platform.

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Julie Ickes has sinced written about articles on various topics from Types of Cancer, Modelling. To read Part 2 of this interview, please visit James Finch contributes to StockInterview.com and other publications. Write to James Finch at jfinch@. Julie Ickes's top article generates over 1600 views. to your Favourites.

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