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Study Examines PEPFAR Efforts In Zambia
A report from researchers at the Sexuality Information and Education Council of the United States examines how $577 million in PEPFAR funding between 2004 and 2008 was used in Zambia, PlusNews/IRIN reports. According to the findings, the authors write, "we observed and documented some impressive prevention programming funded through PEPFAR ò€¦ Nonetheless, when stepping back and observing the whole picture, it becomes apparent that the overall approach of PEPFAR dollars to HIV prevention is far from comprehensive. Instead, it is overly restrictive, adhering to a narrow vision of a moralistic ideal, rather than responding to the reality of the epidemic and the needs of the entire population."

New Guidelines To Standardise Access Criteria For IVF Treatment
The National Infertility Awareness Campaign (NIAC) welcomed the document "Standardising Access Criteria to NHS Fertility Treatment"1 produced by Infertility Network UK (I N UK) and funded by the Department of Health.
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Media Looks At Surgeon General Nominee's Potential Influence On HIV/AIDS, Other Health Issues
The AP/Lexington Herald-Leader on Tuesday examined the nomination of Alabama physician Regina Benjamin for U.S. Surgeon General by President Obama, the history of the position and how former Surgeon Generals have addressed health issues such as HIV/AIDS (Stobbe, 7/14). According to Advocate.com, "During her speech accepting the nomination, Benjamin acknowledged her familiarity with HIV complications and issues, as her brother died at the age of 44 of an HIV-related illness. Having such a personal experience, especially a loss, due to HIV/AIDS could have a strong impact on her policy and public health campaigns, [Phil Curtis, director of government affairs at AIDS Project Los Angeles], told Advocate.com on Tuesday." The article states, "Curtis said that Benjamin has the ability to reach out to communities that have been largely underserved by efforts to reduce the rate of infection," and she "will also be able to contribute to Congress"s current debate on health care policy, including strategies for early HIV prevention, and accessibility to prescription drugs" (Garcia, 7/14).
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Traumatic Brain Injury Treated By Alzheimer's Disease Drug

The destructive cellular pathways activated in Alzheimer"s disease are also triggered following traumatic brain injury, say researchers from Georgetown University Medical Center (GUMC). They say this finding suggests that novel therapy might successfully target both conditions. In an oral presentation at the Alzheimer"s Association 2009 International Conference on Alzheimer"s Disease, the scientists showed that deactivating these pathways in part by using a gamma secretase inhibitor - a class of Alzheimer"s disease drugs currently being tested - reduced loss of neurons in animal models of traumatic brain injury and protected the animals against motor and cognitive deficits. "The goal for both diseases is to prevent neuronal cell death, and this study suggests that one therapy could possibly work for both," says the study"s lead author, neuroscientist Mark Burns, PhD, an assistant professor at GUMC. Both disorders are associated with build-up of beta amyloid, a toxic brain peptide. This substance is commonly found in the brains of elderly patients who died from Alzheimer"s disease, but has also been found in a third of traumatic brain injury victims, some of whom are children, Burns says. It is also known that people who experience such a brain injury have a 400 percent increased risk of developing Alzheimer"s disease. Burns says that buildup of beta amyloid occurs in a second wave of damage that follows immediate "necrotic" death of nerve cells after traumatic brain injury. This secondary injury can last months, if not years, resulting in large holes within brain tissue. Amyloid peptides are produced when a long brain protein known as the amyloid precursor protein (APP) is cut in two by the enzyme beta secretase, and then cut once again by a second enzyme known as gamma secretase. Agents that inhibit the activity of gamma secretase are now being studied as treatment for Alzheimer"s disease. In this study, researchers used mice that were either treated with DAPT, an experimental gamma secretase inhibitor, or mice which were "BACE knock-outs" - so called because they were genetically altered in such a way that they could not produce beta secretase. In unaltered and untreated "normal" mice, brain injury resulted in a rapid accumulation of beta amyloid, along with cognitive and motor deficits. But DAPT and BACE knock-out mice had brain lesions that were as much as 70 percent smaller than control animals and they experienced minimal impairment. The findings further cement the connection between Alzheimer"s disease and traumatic brain injury, Burns says, and show that "modulation of beta and gamma secretase may provide novel therapeutic targets for the treatment of traumatic brain injury." The study was funded by grants from the National Institutes of Health and by the Klingel Family Foundation. The scientists report no potential financial conflicts in this research. Georgetown University has filed a patent application for the technology involved in this research. Karen Mallet Georgetown University Medical Center


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