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PinPointe™ FootLaser™ Submits Its Breakthrough Laser Treatment For Toenail Fungus To Health Canada For Approval
PinPointe FootLaser announced it has submitted its innovative new laser treatment for toenail fungus (Onychomycosis) to Health Canada for approval. As the Federal department responsible for helping Canadians maintain and improve their health, Health Canada reviews medical devices to assess their safety, effectiveness and quality before being authorized for sale in Canada. PinPointe FootLaser has been awarded the CE Mark certifying it has met European Union consumer health and safety standards, has been cleared for use in the treatment of toenail fungus in the EU, and can be offered by healthcare providers throughout Europe. Additionally, the treatment is FDA cleared for applications in dermatology, plastic surgery, and podiatry in the United States.
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New Jersey Department Of Health Confirms Fifth Novel H1N1-Related Death, USA
The New Jersey Department of Health and Senior Services recently announced a fifth death of a New Jersey resident with novel H1N1 influenza.
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House Rejects Amendment To HHS Bill To Limit Funding To Planned Parenthood Clinics
The House on Friday voted 264-153 to approve its fiscal year 2010 Labor-HHS-Education spending bill (HB 3293) after voting on five amendments addressing price and policy issues, CQ Today reports. The bill would appropriate $730.5 billion. The Senate Appropriations Committee is scheduled to begin markup of its version of the bill on July 28.The House voted 183-247 to reject an amendment offered by Rep. Mike Pence (R-Ind.) that would have prohibited family planning funding through the Title X program to Planned Parenthood clinics. The House also voted 211-218 to reject an amendment by Rep. Mark Souder (R-Ind.) that would have stripped language to lift the ban on federal funding for needle-exchange programs. Lawmakers did approve an amendment offered by Rep. Darrell Issa (R-Calif.) to strip $5 million in funding for three NIH grants to study the HIV/AIDS risks associated with alcohol and substance use among sex workers in Asia and alcoholics in Russia (Wolfe, CQ Today, 7/24).
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Viral RNA And Human Immune Response Linked

In its fight against an intruding virus, an enzyme in our immune system may sense certain types of viral RNA pairs, according to scientists. The key lies in a virus" RNA -- a long molecular chain often used to make proteins -- and how it regulates an enzyme called protein kinase R (PKR), according to researchers from Penn State, the University of Connecticut and the University of Beijing. "PKR plays an important role in the human immune system," said Laurie Heinicke, graduate student of chemistry and first author for the paper. "It is activated by long stretches of double-stranded RNA. As a part of our built-in immune response, PKR can recognize viral double-stranded RNAs and inhibit their production." Viral RNA enters human cells when attacking viruses inject their genetic material into the cells and force them to manufacture future generations of viruses. By latching on to specific sites on viral RNA, PKR can interrupt this process. Or, according to Heinicke, "once activated by certain RNAs, PKR stops protein synthesis in the infected cell and ultimately causes cell death." One way for this to happen is for the viral RNA to first form linked pairs called dimers. These RNA dimers then allow separate sets of PKR to bind with themselves, also forming dimers, a state where the paired PKR is most effective against a viral onslaught. "We showed that a small region of the HIV-1 genome termed TAR can regulate PKR," Heinicke continued. "The caveat, however, is that this RNA must form a dimer in order to be an activator." The extra length that dimer RNA provides is critical in encouraging PKR to pair up and function properly. "The length needed for one PKR to bind to RNA is fifteen base pairs," said Philip Bevilacqua, professor of chemistry, Penn State, one of the lead scientists on the project along with James Cole, associate professor, University of Connecticut. "To get two PKRs to bind and dimerize, you need an RNA strand that is twice as long." Cole"s laboratory provided evidence of dimerization of RNA and PKR. In their experiments at Penn State, the scientists found the dimer RNA activated PKR from 9 to 118 times more than the single strand RNA, depending on the RNA type. TAR RNA dimerization activated the most PKR when the TAR did not exhibit structural defects. The researchers report their findings in a recent issue of the Journal of Molecular Biology. "Adding these defects decreases the number of places where PKR can bind to the RNA," Heinicke explained. RNAs that showed the greatest degree of symmetry are more potent PKR activators than ones with defects. "It appears as though length is a necessary, but not sufficient condition for activation," said Bevilacqua. The scientists constructed RNAs to remove TAR defects. Dimers of these RNAs increased PKR activity, compared to more asymmetric "wild-type" TAR dimers. Single strands of these RNAs did not activate PKR. This is in contrast to previous work, which reported that the single strand wild-type TAR showed a 50-fold increase of activation over more symmetric variants. "This helps us find what the actual molecular structure is that activates PKR," said Bevilacqua. "It is still basic research for now, but finding the cause for this may ultimately lead to understanding disease." Notes: Heinicke, Bevilacqua and Cole worked with Subba Rao Nallagatla, chemistry research associate, Penn State, University Park; Amy Diegelman-Parente, assistant professor of biochemistry, Penn State Altoona; Jason Wong, molecular and cell biology postdoctoral fellow and Jeffrey Lary, analytical ultracentrifugation biotechnology facility scientist, University of Connecticut, and Xiaofeng Zheng, professor of biochemistry and molecular biology, University of Beijing. The NIH funded this project. A"ndrea Messer Penn State


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