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American Hospital Association Announces 2009-2010 Class Of Patient Safety Leadership Fellows
The American Hospital Association announces the 2009-2010 class of Patient Safety Leadership Fellows. Thirteen individuals have been selected to participate in this year"s fellowship class.
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New England Cord Blood Bank Installs Automated Cord Blood Processing Line
New England Cord Blood Bank, Inc. (NECBB), a global cord blood processing and storage facility, announced today that it will be implementing an automated blood processing system at the company"s Newton facility. The AutoXpress™ System (AXP), developed by ThermoGenesis Corp. and distributed by GE Healthcare, is a state-of-the-art, fully closed and sterile system that will provide automated cell separation and processing for cord blood samples, ensuring quality and consistency in cord blood processing while maximizing the yield of valuable stem cells from the cord blood.
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Washington Post Examines Northern Virginia Clinic That Serves People Living With HIV/AIDS
The Washington Post examines one of INOVA Juniper Program"s six clinics serving those with HIV/AIDS located "[t]wo blocks down the road" from the old Whitman-Walker clinic, which "served the Northern Virginia HIV/AIDS community for more than a decade, [and] closed this year because of financial constraints." As of late last month the new Arlington, Va., clinic served 198 people, but Karen Berube, director of the program, said she expects to have 250 clients there by the end of the year. By comparison, the Whitman-Walker center treated 678 people at its Arlington clinic, according to the Post. Services are provided on a sliding-fee scale based on income, "but the majority of patients do not pay anything. Instead, they are funded by Medicaid, Medicare or private insurance, or they receive charity care through government and private donor grants," the article states (Caputo, 7/9).
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Gliomas Exploit Immune Cells Of The Brain For Rapid Expansion

Gliomas are among the most common and most malignant brain tumors. These tumors infiltrate normal brain tissue and grow very rapidly. As a result, surgery can never completely remove the tumor. Now, the neurosurgeons Dr. Darko S. Markovic (Helios Klinikum Berlin-Buch) and Dr. Michael Synowitz (Charité) as well as Dr. Rainer Glass and Professor Helmut Kettenmann (both Max DelbrÃøck Center for Molecular Medicine, MDC, Berlin-Buch), have been able to show that glioma cells exploit microglia, the immune cells of the brain, for their expansion (PNAS Early Edition)*. Microglial cells are the immune cells of the brain/central nervous system. They constantly screen the brain environment. On their surface they use sensors to detect changes in their environment due to brain damage or infections. An important family of these sensors are Toll-like receptors (TLR). However, microglia do not attack glioma cells. On the contrary: they support the growth of the tumor and, thus, make the disease worse. Together with researchers in Warsaw, Poland, Amsterdam, The Netherlands, and Bethesda, USA, the researchers in Berlin have been able to show how the immune cells promote the tumor growth. Microglial cells are attracted toward the glioma cells and gather in and around the tumor in large numbers. Interestingly, gliomas consist of up to 30 per cent of microglia, especially at the tumor edge. Gliomas release certain enzymes, metalloproteases, which digest the extracellular matrix, and also dissolve the ties between cells. However, the metalloproteases are produced and released as inactive precursor protein which need to be cleaved to be activated. This cleavage is accomplished by another enzyme, which is produced by the microglial cells. This enzyme is anchored in the membrane and was therefore named membrane type 1 metalloprotease (MT1-MMP). MT1-MMP activates the metalloproteases which clear the way for the glioma cells and allows them to infiltrate normal brain tissue and expand very rapidly. Normally, microglial cells do not produce MT1-MMP. However, the glioma cells manipulate the microglial cells by stimulating microglial TLR which trigger the expression of MT1-MMP. The researchers could confirm their data from petri dish in mice. "Those mice, in which we had knocked out the MT1-MMP gene or a crucial gene for TLR signalling, did attract fewer microglial cells and the tumor grew much more slowly", explains Professor Kettenmann. They could also demonstrate that MT1-MMP was present in tissue from glioma patients. Remarkably, the gliomas with high level of microglial MT1-MMP were also more aggressive. Moreover microglial cells were more abundant in tissue sample from the tumor edge as compared to the center of the tumor. Glioma cells themselves do not produce MT1-MMP. However, when the researchers experimentally over expressed MT1-MMP in glioma cells, they died. The researchers hope, that interfering with TLR receptors or their intracellular pathways might reduce the rapid expansion of glioma cells. Professor Kettenmann: "Microglia are a new target for glioma researchers." * Gliomas induce and exploit microglial MT1-MMP expression for tumor expansion D. S. Markovica,b, K. Vinnakotaa, S. Chirasania, M. Synowitza,c, H. Ragueta, K. Stocka, M. Sliwad, S. Lehmanne, R. Ka¨ linf,N. van Rooijeng, K. Holmbeckh, F. L. Heppnerf, J. Kiwitb, V. Matyasha, S. Lehnardte, B. Kaminskad, R. Glassa,1,2, and H. Kettenmanna,1 aCellular Neuroscience, Max DelbrÃøck Center for Molecular Medicine, 13125 Berlin, Germany; bDepartment of Neurosurgery, Helios Clinics, 13125 Berlin, Germany; cDepartments of Neurosurgery and fNeuropathology and eCecilie Vogt Clinic for Neurology, Charité - Universitätsmedizin Berlin, 13353 Berlin, Germany; dLaboratory of Transcription Regulation, Nencki Institute of Experimental Biology, 02-093 Warsaw, Poland; gDepartment of Molecular Cell Biology, Faculty of Medicine, Vrije Universiteit, VU University Medical Center, 1081 BT Amsterdam, The Netherlands; and hCraniofacial Skeletal Diseases Branch, Matrix Metalloproteinase Unit, National Institute of Dental and Craniofacial Research, National Institutes of Health, Bethesda, MD 20892 Barbara Bachtler Helmholtz Association of German Research Centres


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