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FDA Recommends Gardasil Recipients Sit, Lie Down After Receiving Vaccination
In a posting aimed at health care professionals, FDA on its Web site on Wednesday said that recipients of Merck"s human papillomavirus vaccine, Gardasil, should be closely observed afterward for 15 minutes while they remain seated or lying down to avoid the possibility of fainting, the Wall Street Journal reports. FDA said that since October 2007, Gardasil"s labeling for both health care providers and patients has included a discussion about fainting. The agency said the strengthened recommendation comes in response to reports of "traumatic injuries" among some recipients who experienced fainting (Corbett Dooren, Wall Street Journal, 6/10). Gardasil protects against the strains of HPV that cause most cases of cervical cancer and genital warts. The Centers for Disease Control and Prevention recommends that girls ages 11 and 12 receive the three-dose vaccine before they are sexually active. Girls and women ages 13 to 26 who have not been vaccinated or completed the vaccine series also should receive the vaccine (CDC fact sheet, June 2008). On Wednesday, FDA also approved changes to Gardasil materials that place warnings about fainting in a more prominent place on drug labels and handouts. The agency said that the new recommendations are intended to "prevent falls and injuries" (Wall Street Journal, 6/10).

Health Care Overhaul Could Include Changes To Doctor Payments
The Wall Street Journal reports that "Democratic centrists said they won a tentative commitment from the White House to back a proposal to curb the growth of Medicare costs. ... One proposal pushed both by President Barack Obama and some centrists is to give the executive branch the authority to implement cuts to Medicare spending that would be recommended by independent experts. Congress could stop the cuts, but only if it acted swiftly. Fiscal conservatives say that under the current system, which gives Congress more power, lawmakers shy away from politically tough votes to restrain Medicare costs."
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Nutrition

Enzyme Doesn't Act Alone In Atrial Fibrillation

An overactive enzyme is behind a leaky calcium channel that plays a role in the development of atrial fibrillation, which is the most common cardiac arrhythmia that is responsible for a third of all strokes. However, it doesn"t act alone, say researchers at Baylor College of Medicine. The findings can be found online in the current edition of the Journal of Clinical Investigation. "When the heart pumps properly, the muscle contractions are regulated by waves of calcium. When the heart relaxes, the calcium is stored; when the heart contracts, it is released," said Dr Xander Wehrens, assistant professor of molecular physiology and biophysics, and cardiology at BCM. "In atrial fibrillation, the calcium is released too early. As it leaks out, the heart beats too fast and irregularly." Researchers knew that an enzyme called calmodulin kinase II is overactive in several heart diseases and believed it played a role in the leaky channels - a tiny pore that controls release of calciu through the cell"s membrane. In the current study, Wehrens and colleagues were able to show in mouse models that if this enzyme is inhibited, calcium channels normalize and atrial fibrillation is prevented. To determine if the calcium leak alone was enough to set off atrial fibrillation, researchers bred a mouse with a specific genetic mutation in the calcium channel, making it prone to leaks. "The mice were fine. They did not develop atrial fibrillation despite the leak," Wehrens said. "There had to be another factor that contributed to arrhythmias." Wehrens said they discovered that a sudden increase in heart rate is a very specific activator of calmodulin kinase II. The research team found that mice with the mutation were more prone to atrial fibrillation after their heart rate was sped up, activating the enzyme. Mice that lacked the mutation did not suffer from arrhythmias despite having the enzyme activated. From that they surmised that the enzyme alone did not lead to atrial fibrillation. When they used a drug to block activity calmodulin kinase II, and the mices" heart rates were raised, the mice with the calcium channel mutation had no signs of arrhythmia. Again the results further supported the conclusion that the enzyme does play a role in the disorder but does not act alone. "It"s a synergy. The models had to have a preexisting problem on top of overactive calmodulin kinase II," Wehrens said. "If you don"t have the mutation and the enzyme, but only one or the other, then you don"t develop the arrhythmia." Since calmodulin kinase II is important to many other functions in the heart, blocking it all together is not a realistic treatment. Instead, they were able to make a change to one amino acid in the genetic code and stop the specific calcium channel from being affected by the enzyme. Further studies with similar models showed this as an effective treatment. "More trials are needed, but this is a promising way to target one regulatory event that contributes to atrial fibrillation," Wehrens said. "These findings could lead to new drug therapies for arrhythmias and better patient care." Notes: Others who took part in the study include Drs. Mihail Chelu, Satyam Sarma, Subeena Sood, Ralph van Oort, Darlene Skapura, Na Li, and Marco Santonastasi, all of the department of molecular physiology and biophysics at BCM; Sufen Wang and Miquel Valderrábano, both of the department of cardiology at The Methodist Hospital; Frank-Ulrich MÃøller and Wilhelm Schmitz, both of the Institute of Pharmacology and Toxicology, Universitätsklinikum MÃønster, MÃønster, Germany; Ulrich Schotten, department of physiology Maastricht University, Maastricht, The Netherlands; Mark E. Anderson, department of internal medicine, division of cardiovascular medicine, University of Iowa Carver College of Medicine; and Dobromir Dobrev, department of pharmacology and toxicology, Dresden University of Technology, Dresden, Germany. Funding for the study came from the American Heart Association, the National Institutes of Health National Heart Lung and Blood Institute, the March of Dimes, the Heart Rhythm Society, the Houston Texans, and the Foundation Leducq Award to the Alliance of Calmodulin Kinase Signaling in Heart Disease. Graciela Gutierrez Baylor College of Medicine


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