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Alzheimer's Society Response To The Publication Of Revised NICE Guidance On Alzheimer's Treatments, UK
Thousands of people with Alzheimer"s will continue to be denied access to the only drug treatments for the disease following the publication of revised guidance by the National Institute for Health and Clinical Excellence (NICE). The original guidance recommended that only people in the moderate stages of Alzheimer"s disease should have access to drugs in the NHS, denying them to people in the early stages.
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Bike Paths, Other 'Healthy' Infrastructure Projects Proving Controversial
"Attempts to set billions aside for infrastructure projects like bike paths face an uphill battle on Capitol Hill," The Chicago Tribune reports, adding "GOP legislators see no health savings in parks and similar projects," while advocates say preventive efforts will bring down costs. "A draft Senate bill would provide up to $10 billion annually for a "prevention and public health investment fund" -- a portion of which could be used for projects such as bike paths, sidewalks, farmers markets and other community interventions meant to curb chronic and costly conditions like obesity."
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Spike In Severe Weather And Looming Alzheimer's Disease Epidemic - A Formula For Disaster
As the 2009 hurricane season begins, the MIT AgeLab and the Advance 50 Team of gerontologists at The Hartford Financial Services Group, Inc., offer new research and life-saving tips to help caregivers, family and friends of those with Alzheimer"s disease who live at home prepare for a natural disaster and get their lives back on track in the aftermath.
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Yale Team Identifies Key To Potential New Treatment For Allergy-Induced Asthma

In research that could lead to new asthma drugs, scientists at Yale School of Medicine, Hydra Biosciences of Cambridge, Massachusetts, and the University of California, San Francisco have discovered that a protein may be a trigger of allergy-induced asthma in mice. They also demonstrated how a drug known to reduce inflammatory and neuropathic pain may also inhibit asthma symptoms in mice. Their paper is published in the May 18-22 online Early Edition of the Proceedings of the National Academy of Sciences. There has been a dramatic increase in the number of asthma cases reported in recent decades. Scientists know that asthma involves an immune response to inhaled allergens that results in inflammation, mucus secretion and bronchial constriction. But limitations of existing treatments aimed at the immune system suggest that additional physiological mechanisms may be involved in asthmatic inflammation. The new study tracks the role of the ion channel protein TRPA1. While the exact function of TRPA1 in the airway inflammation of asthma is not completely understood, scientists do know from previous research that this ion channel protein is a sensor for chemical irritants such as cigarette smoke and certain chemicals that also trigger asthma. TRPA1 is found in airway nerves that mediate pain and irritation and trigger coughing and sneezing. The researchers found that mice with no TRPA1 showed fewer signs of asthma. According to the paper"s lead author, Sven-Eric Jordt, Ph.D., assistant professor of pharmacology at Yale School of Medicine, "When compared to normal mice, those lacking the gene for TRPA1 had greatly diminished inflammation, airway mucus and bronchoconstriction." Furthermore, when the Yale-Hydra team administered a pharmacological agent, HC-030031, that is known to inhibit pain related to TRPA1, to mice with asthma, their symptoms were diminished. "Blocking TRPA1 may prevent the infiltration of the lung by the inflammatory cells responsible for asthma symptoms such as wheezing and mucus overproduction," Jordt explained. The pharmacological agent observed in this study to diminish asthmatic symptoms in mice was identified by Hydra Biosciences. Yale"s Sven-Eric Jordt serves on Hydra"s scientific advisory board and receives consulting fees from Hydra. Several other members on the research team are employees of Hydra Biosciences and have a financial interest in the potential development of HC-030031 as a pharmacological treatment. In addition to Jordt, the team included Ana I. Caceres, Marian Brackmann, Maxwell D. Elia, Bret F. Bessac, Robert J. Homer and Lauren Cohn of Yale; Donato del Camino, Marc D"Amours, JoAnn S. Witek, Christopher M. Fanger, Jayhong A. Chong, Neil J. Hayward and Magdalene M. Moran (corresponding author) of Hydra Biosciences; and Xiaozhu Huang of University of California, San Francisco. This research was funded by grants from the American Asthma Foundation and the National Institute of Environmental Health Sciences. Yale School of Medicine


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