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Philadelphia Area Increases Inpatient Hospice Care
A new market emerges for special end-of-life care that is inpatient and offers quiet rooms, home-like settings and high-tech alternatives. The Philadelphia Inquirer reports: "For most people, hospice is a collection of services -- and an attitude -- that helps the terminally ill die comfortably at home. But as the number of patients entering hospice grows and as the drugs and technology used to ease pain become more sophisticated, some hospice providers say they"re seeing more patients who need more care than their families can provide at home. That need, combined with the availability of some empty hospital buildings, has led to the creation, since November, of three new inpatient hospice units in this area."
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Hyperferritinemia Is Another Surrogate Marker Of Advanced Liver Disease
High serum ferritin, being a hallmark of hereditary hemochromatosis , is frequently found in chronic hepatitis C, alcoholic or non-alcoholic steatohepatitis and non-alcoholic fatty liver disease patients . A study in Italy has investigated the link between ferritin and steatosis in a non-obese cohort of non-alcoholic patients. In southern European populations, high ferritin levels, after exclusion of diagnosis of HH, represent a risk factor for steatosis and clinical relevance, being associated with low platelet count.
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Sports Injuries Cause 1 In 5 Emergency Department Visits For Kids
Sports-related injuries such as bruises, scrapes and broken bones accounted for 22 percent of hospital emergency department visits for children ages 5 to 17 in 2006, according to the latest News and Numbers from the Agency for Healthcare Research and Quality.
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Hearing Improved In First Successful Medical Treatment For Tumor-Inducing Genetic Disorder

Treatment with the angiogenesis inhibitor bevacizumab improved hearing and alleviated other symptoms in patients with neurofibromatosis type 2 (NF2). In a paper to appear in the July 23 New England Journal of Medicine, which is receiving early online release, researchers from Massachusetts General Hospital (MGH) report that bevacizumab treatment successfully shrank characteristic tumors in a small group of NF2 patients, the first reported successful NF2 treatment not involving surgery or radiation. "This kind of treatment response is unprecedented," says Scott Plotkin, MD, PhD, of the Pappas Center for Neuro-Oncology in the MGH Cancer Center, lead author of the NEJM paper. "Our study is the first to provide evidence that a drug can shrink vestibular schwannomas - benign tumors on the balance and hearing nerves - and the first to show that patients" hearing can be improved." NF2 is an inherited genetic disorder in which benign tumors develop throughout the nervous system. Vestibular schwannomas are the most common NF2-associated tumors, and although they grow slowly, they usually cause patients to lose all or most of their hearing by young adulthood or middle age. The tumors can be removed surgically or treated with radiation, but in patients with vestibular schwannomas on both sides, which is typical in NF2, such treatment usually leads to complete hearing loss. Growing vestibular schwannomas can also press on the brainstem, leading to headaches, difficulty swallowing and other serious neurologic symptoms. Since vestibular schwannomas are benign tumors, it was believed that they did not stimulate formation of new blood vessels as malignant tumors do. However, when the researchers studied tissue samples from NF2-related schwannomas, sporadic tumors not caused by NF2 and normal spinal nerves, they found evidence of excess blood vessel development and increased expression of angiogenesis-related molecules in both NF2-associated and sporadic vestibular schwannomas. With this suggestion that angiogenesis was involved in these tumors, members of the research team offered treatment with bevacizumab (Avastin), which is FDA-approved for treatment of several forms of cancer, to NF2 patients in danger of complete hearing loss or other significant neurological damage. Among the first ten NF2 patients to receive bevacizumab, treatment led to tumor shrinkage in nine, and six had 20 percent or greater reduction in tumor size. In those six patients, tumor shrinkage lasted from 11 to 16 months, longer than the four months typically seen in bevacizumab treatment of malignant brain tumors. Of seven patients who had started to lose their hearing before treatment, four experienced some hearing restoration - two returning to work or school as a result - improvement that has also lasted for up to 16 months. In one patient without significant tumor shrinkage or hearing improvement (he had lost all hearing prior to treatment), treatment alleviated headaches and nausea caused by brainstem compression, allowing him also to return to school. "This study has opened a new approach to research and understanding of these tumors," says Emmanuelle di Tomaso, PhD, the study"s senior author, formerly with the Steele Laboratory of Tumor Biology in the MGH Department of Radiation Oncology. "There had been a dogma that these tumors do not produce edema and are not angiogenic, concepts that now need to be reevaluated." She adds that the study also suggests that VEGF - the angiogenesis factor blocked by bevacizumab - may have a role in nerve physiology beyond the stimulation of blood vessel growth. Plotkin notes, "Based on the results of this study, we have just opened the first formal clinical trial of a drug treatment for NF2. We are testing an exciting new, oral VEGF inhibitor that will be easier for patients to take - bevacizumab is administered intravenously - and may have fewer side effects." Notes: Plotkin is an assistant professor of Neurology at Harvard Medical School (HMS). Formerly an assistant professor of Radiation Oncology at HMS, di Tomaso recently joined the Novartis Institutes for BioMedical Research. Additional co-authors of the NEJM report are Anat Stemmer-Rachamimov, MD, MGH Pathology; Fred Barker, MD, MGH Neurosurgery; Timothy Padera, PhD, Alex Tyrrell, PhD, and Rakesh Jain, PhD, MGH Radiation Oncology; Gregory Sorensen, MD, MGH Radiology, and Chris Halpin, PhD, Massachusetts Eye and Ear Infirmary. The study was supported by the HMS Center for Neurofibromatosis and Allied Disorders, Neurofibromatosis Inc. New England, Children"s Tumor Foundation, the Department of Defense, the National Institutes of Health, and the MGH Executive Committee on Research. No support was provided by Genentech, which produces and markets bevacizumab under the brand name Avastin. Katie Marquedant Massachusetts General Hospital


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