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The European Association For The Study Of The Liver Renews Publishing Partnership With Elsevier
Elsevier, the leading publisher of scientific, technical and medical information, is pleased to announce its renewed publishing partnership with The European Association for the Study of the Liver (EASL), the leading European association in the field of liver research. The agreement calls for Elsevier to publish the society"s flagship journal, the Journal of Hepatology, for the next five years.
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UN And WHO Heads Meet Vaccine Manufacturers
World Health Organization (WHO) Director-General Dr Margaret Chan and United Nations Secretary-General Ban Ki-moon met with over 30 vaccine manufacturers from developing and developed countries at WHO headquarters today. Both the Director-General and the Secretary-General stressed the importance of assuring that any eventual vaccine for Influenza A(H1N1) was made available in a spirit of equity and fairness, and invited the manufacturers to continue to work with them to develop a strategy for this. Industry representatives affirmed their wish to cooperate in making supplies available to developing countries, and said they stood ready to produce the vaccine when requested.
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Experts Launch Think Tank For Mystery Disease
Ten leading scientists in Europe have formed a Think Tank for ME and will hold their first meeting on the 13th of June. They want to initiate an effective research effort to find the secret behind the mystery disease that cripples an increasing number of lives. Myalgic Encephalomyelitis, often referred to as Chronic Fatigue Syndrome (CFS), is a disease which affects at least one million individuals in the US, and an even greater number in Europe. Despite the large number of people affected, there is a lack of serious large-scale research initiatives focused on the disease. The number of patients is rapidly increasing but healthcare personnel lack knowledge about existing research and possible treatments.
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Pitt Team Reports In Nature That Unique Portion Of Enzyme Fights Lung Infection

An enzyme known to play a key role in the development of emphysema serves as the first line of defense against bacterial infection of the lung, according to researchers at the University of Pittsburgh School of Medicine. They also found that the antimicrobial activity comes from a small portion of the enzyme that is structurally and sequentially unique in nature. Lead author A. McGarry Houghton, M.D., assistant professor, Division of Pulmonary, Allergy and Critical Care Medicine, Pitt School of Medicine, said that prior to this discovery scientists thought that the enzyme, called macrophage elastase, matrix metalloproteinase-12 or MMP-12, which is produced in excess in smokers, didn"t do anything but degrade the lung"s elastic fibers, thereby contributing to the tissue destruction of emphysema. "But we found that mice that didn"t have the gene to make this enzyme could not clear bacteria well and were more likely to die of infection," he explained. "They couldn"t make this small protein, which kills bacteria by poking holes in cell membranes." The findings were described today in Nature. "While not the initial purpose of this study, finding novel antimicrobial mechanisms is extremely important," said senior author Steven D. Shapiro, M.D., Jack D. Myers Professor and chair of the Department of Medicine, Pitt School of Medicine, whose research teams cloned the MMP-12 gene almost 20 years ago and conducted the work that showed its role in emphysema. "Many microorganisms have adapted to circumvent our current and stagnant arsenal of antibiotics. We must find new weapons so that we don"t fall back to the public health problems we had prior to penicillin." MMP-12 is stored in macrophages, the cells that swallow up invading bacteria. When Staphylococcus aureus was injected into the tail vein of healthy and MMP-12-deficient mice, the two-week mortality rate was about the same. However, the amount of bacteria was much greater in the lungs of MMP-12-deficient mice. In models of pneumonia and peritonitis, MMP-12-deficient mice were much less likely to survive the infection. Macrophages are present in very high numbers in the lungs and the peritoneum, which is the lining of the abdomen. "Our experiments also showed that while the MMP-12-deficient macrophages were able to ingest bacteria, they couldn"t kill them," Dr. Houghton said. "The intracellular bacteria level escalated rather than diminished." The researchers then looked for what gave MMP-12 its antibacterial properties. While the portion of the enzyme that catalyzes, or speeds up, chemical reactions degrades lung tissue in emphysema, its tail is the portion that kills microbes. Protein fragments were tested to identify a chain of 20 amino acids that could kill Staph aureus in culture dishes. A computer-generated 3-dimensional model of the enzyme"s tail, including the 20-amino acid chain, revealed there were only a few exposed places permitting interaction with bacterial surfaces, and that one of those loops had a protrusion containing a sequence of four amino acids, called KDEK, that is not present in any other enzymes of the MMP class. "Humans, mice, rats and rabbits all have that special sequence and structure in MMP-12, but not in other MMPs," Dr. Houghton noted. He and his colleagues synthesized chains nearly identical to the 20-amino acid sequence but substituted other segments for KDEK, and found that both the sequence and the loop structure was necessary to kill bacteria. The team plans to study whether the same part of the enzyme is able to kill viruses and fungi, and whether there are any connections between MMP-12"s roles in emphysema and infection defense. Notes: Study co-authors include William O. Hartzell, M.D., formerly of Brigham and Women"s Hospital, Boston; F. Xavier Gomis-Ruth, Ph.D., Molecular Biology Institute of Barcelona, Spain; and Clinton S. Robbins, Ph.D., postdoctoral fellow, Division of Pulmonary, Allergy and Critical Care Medicine, University of Pittsburgh School of Medicine. The research was supported by grants from the National Institutes of Health and Spanish and European public agencies. Anita Srikameswaran University of Pittsburgh Schools of the Health Sciences


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