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Quality Data Made Accessible To Clinical Teams
NHS clinical teams will have access to data showing their performance against a set of more than 200 indicators of high quality care in the NHS in one place. It is the next phase in the drive to help NHS professionals improve the quality of care they deliver to patients, and will also support providers and commissioners of NHS services. Buy arimidex to treat cancer.

CEL-SCI Developing Immune-Based Treatment Against Swine And Other H1N1 Flu Viruses Using Proprietary L.E.A.P.S. Technology
CEL-SCI Corporation (NYSE AMEX: CVM) announced that it is developing an immune-based treatment for the "swine flu and related H1N1" flu viruses, utilizing its proprietary L.E.A.P.S.(TM) (Ligand Epitope Antigen Presentation System) vaccine technology. The Company plans to utilize the expertise and knowledge it has gained from developing protective and therapeutic vaccines utilizing L.E.A.P.S. to develop a therapeutic treatment based upon the technology for people infected with the swine and H1N1 flu viruses. CEL-SCI has already commenced pre-clinical testing.

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News of the day
McGill University Receives Almost $63 Million Under CFI Program To Support Five Research Projects
Dr. Denis Therien, Vice-Principal (Research and International Relations) of McGill University has welcomed the Canada Foundation for Innovation"s (CFI) investment of $32,649,184 supporting five projects led by Dr. David Plant, Dr. Paul Lasko, Dr. David Thomas, Dr. Vincent Giguç¨re and Dr. Chao-Jin (C.J.) Li. The Quebec government also confirmed it would match that funding.
Endocrinology

Halting Advanced Metastatic Breast Cancer By Targeting MMPs

An upcoming G&D paper reveals how two specific matrix metalloproteinase (MMP) proteins contribute to bone metastasis in advanced breast cancer - lending important new insight into the design of clinically useful small molecule inhibitors. The study was led by Dr. Yibin Kang in Princeton University in close collaboration with Dr. Joan Massaguç© at MSKCC and Dr. Michael Reiss at the Cancer Institute of New Jersey. It will be published online ahead of print athttp:// www.genesdev.org/cgi/doi/10.1101/gad.1824809. "More than 70% of late stage breast cancer patients have skeletal complications," explains Dr. Yibin Kang. "It is important to uncover molecular mechanism of bone metastasis in order to come up with better treatments to reduce the pain and suffering from bone metastasis." MMPs are a large class of related enzymatic proteins that degrade the extracellular matrix. Normal MMP activity is tightly regulated, and is necessary for a number of physiological processes, like tissue remodeling, angiogenesis, ovulation and wound healing. However, MMP dysregulation facilitates tumor metastasis. MMP1 and ADAMTS1 are two different MMP family members that were previously identified in a genomic screen for breast cancer bone metastasis genes. Dr. Kang and colleagues now show how alterations in MMP1 and ADAMTS1 expression promote bone metastasis. MMP1 and ADAMTS1 are upregulated in breast cancer cell lines with an enhanced ability to metastasize to bone. Dr. Kang and colleagues demonstrated that MMP1 and ADAMTS1 enzymatically cleave and release EGF-like growth factors from tumor cells to stimulate EGFR signaling in the bone-building osteoblasts. The researchers went on to show that such signaling reduces the production of OPG, a suppressor of the bone-resorbing osteoclasts, eventually leading to hyperactivity of osteoclasts, bone destruction and subsequent expansion of bone metastasis. Thus, this paper supports a rationale for the therapeutic targeting of MMP1 and ADAMTS1, and suggests that inhibition of EGFR signaling in bone stromal cells to block osteoclast activity may represent a viable method of mitigating bone complications in advanced metastatic breast cancers. Reference: ADAMTS1 and MMP1 proteolytically engage EGF-like ligands in an osteolytic signaling cascade for bone metastasis Xin Lu, Qiongqing Wang, Guohong Hu, Catherine Van Poznak, Martin Fleisher, Michael Reiss, Joan Massague, and Yibin Kang Heather Cosel-Pieper Cold Spring Harbor Laboratory


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