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AVMA Response To PETA Protest At The Association's Annual Convention
The American Veterinary Medical Association (AVMA) respects and values PETA"s right to express an opinion and hold a peaceful demonstration at our 146th Annual Convention in Seattle. On the other hand, we disagree with their position on our use of fish during an educational and motivational presentation by the fishmongers of Pike Place Fish Market.
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Some Governors Oppose Medicaid Expansion Proposals
"Some governors are pushing to scale back or kill proposals to expand Medicaid to provide health-care coverage to the uninsured, raising a new challenge to President Barack Obama"s effort to overhaul the system," The Wall Street Journal reports. Health care proposals in the House and Senate "would expand the program to cover at least a third of the nation"s 46 million uninsured, but states are worried they would get stuck with a big part of the tab." Medicaid is "expected to be a primary topic" when a group of governors -- "including Democratic Gov. Christine Gregoire of Washington and Republican Gov. Haley Barbour of Mississippi" -- head to Washington, D.C., this week "to discuss health care with White House and congressional officials."
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QuantRx Announces FluoroPharma To Present Phase I Study Results Of Novel Positron Emission Tomography (PET) Myocardial Perfusion Imaging (MPI) Tracer
QuantRx® Biomedical Corporation (OTCBB:QTXB), a broad-based diagnostic company focused on the development and commercialization of innovative diagnostic products, announced that its affiliate, FluoroPharma Inc., a company developing breakthrough PET molecular imaging agents, will present Phase I data relating to the safety, dosimetry, and pharmacokinetics in human subjects of BFPET, its novel 18-F labeled (PET) tracer for myocardial perfusion imaging, at the Society of Nuclear Medicine 2009 Annual Meeting in Toronto.
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Prostate Cancer Diagnosis, Treatment Could Be Improved By Protein That Suppresses Androgen Receptors

A protein that helps regulate expression of androgen receptors could prove a new focal point for staging and treating testosterone-fueled prostate cancer, Medical College of Georgia researchers say. Levels of the protein, í²arrestin2, are lower in some prostate cancer cells than in normal prostate cells while expression of testosterone-fed androgen receptors is higher, they report in Proceedings of the National Academy of Sciences Online Early Edition this week. "An increase in the number of androgen receptors is believed responsible for prostate cancer progression in men with advanced disease," says the study"s corresponding author, Dr. Yehia Daaka, Distinguished Chair in Oncologic Pathology in the MCG School of Medicine. With increased numbers of androgen receptors, prostate cancer can make use of the limited testosterone available after a diseased prostate gland is removed or after testosterone production is blocked by drug therapy. In fact, the increased number of androgen receptors may mutate so they can start feeding off other steroids or even growth factors, Dr. Daaka says. These wily skills help explain why cancer returns despite initially promising treatment results. "It is clear that signaling by the androgen receptor is paramount for not only the initiation but also the progression of the disease, including escape to a hormone-refractory disease," he says. Moves androgen receptors make to support cancer growth make it "unbeatable at this point," for some patients. However increased levels of í²arrestin2 appear to halt the potentially deadly increase in androgen receptor expression, the MCG research team has found. Androgen receptors have co-factors that can activate or repress their activity. "You could make the leap and say perhaps prostate cancer initiation and progression may be regulated by expression or non-expression of these co-factors," says Dr. Daaka, a Georgia Cancer Coalition Distinguished Cancer Scholar. Their studies in human tissue - both in culture and transplanted into mice - show this appears the case for í²arrestin2. First the team identified í²arrestin2 as cofactor for androgen receptors. Next they found a reciprocal relationship: androgen receptor expression is low when í²arrestin2 expression increases. That"s the scenario in healthy prostate cells while the exact opposite is true in some prostate cancer. When they forced increased expression of í²arrestin2, androgen receptor expression and activity went down. í²arrestin2 locks up an androgen receptor by binding to it, then the pair bind to yet another protein, ubiquitin ligase, which tags the receptor as waste and the trio make their way to the cell"s garbage dump. "The neat thing about it is í²arrestin2 inhibits or blunts the androgen receptor by promoting its degradation. So it disappears," Dr. Daaka says. His future studies include determining what happens when í²arrestin2 expression is further decreased in the face of prostate cancer. These studies will also help determine how big a player í²arrestin2 is in prostate cancer progression, says Dr. Daaka, noting that numerous other corepressors and activators of androgen receptors are known. Since all the happenings occur inside prostate cells, the findings don"t point toward a new blood or urine test for prostate cancer but could lead to new ways to stage prostate cancer from the first biopsy. In fact, Dr. Daaka and his team already are collecting samples from patients whose cancer has been staged to see if specific levels of í²arrestin2 expression correlate with different stages of disease. Another goal is to develop a small molecule that can get inside a patient"s cell and mimic í²arrestin2"s ability to suppress androgen receptor expression and so restore healthy levels found in prostate cells. Prostate cancer falls behind skin cancer as the second most common cancer in men and more than 192,000 new cases will be diagnosed this year in the United States, according to the American Cancer Society. Collaborators include Dr. Vijayabaskar Lakshmikanthan, postdoctoral fellow; Dr. Lin Zou, former postdoctoral fellow; Jae Kim, graduate student; Dr. Nidia C. Messias, assistant professor; and Dr. Zhongzhen Nie, assistant professor; from the MCG Department of Pathology; and Drs. Allison Michal and Jeffrey L. Benovic from Thomas Jefferson University. Toni Baker Medical College of Georgia


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