UCLA Researchers Discover Genes Linked To Lymphoma, Opening Way For New Targeted Drugs
Lymphoma is a blood cancer   that affects more than 60,000 Americans each year. Researchers at The  University of California Los Angeles have identified genes that when  inactivated help cause B-cell non-Hodgkin's lymphoma (NHL). These genetic  defects may also be involved in promoting the formation of other cancers  since they can inactivate normal tumor-suppressing gene activities in a  range of cell types.
     The team led by Michael Teitell, M.D., Ph.D., and funded by The  Leukemia & Lymphoma Society, used genetically engineered mice to accurately  mimic human B-cell cancers. They had previously published research in which  they identified frequent genetic abnormalities in cancer cells from NHL  patients -- namely defects in the TCL1 gene -- and showed that TCL1  abnormalities can cause NHL in mice when accompanied by additional genetic  defects. Now, they have found some of these cancer collaborators.
        Teitell's team used a powerful genetic technique called "restriction  landmark genomic scanning" (RLGS) to find genes that work with abnormal  TCL1 to promote lymphoma formation. These genes are inactivated in  lymphomas by defects known as DNA hypermethylation. The breakthrough  research, published in the January 29, 2007, issue of the journal Oncogene,  is likely to help in the development of new targeted drugs for NHL   patients.
        The researchers are working to determine which hypermethylation gene  defects also occur in human lymphomas, at which point they will be ready to  help develop new targeted therapies for NHL patients. Drugs that target DNA  hypermethylation are already known to have anti-cancer activity. The drug  Decitabine (Dacogen(R); SuperGen/MGI Pharma) has recently been approved by  the U.S. Food and Drug Administration to treat patients with   myelodysplastic syndrome, and is being tested in other cancers. Teitell's  findings suggest that such drugs should be tested for anti-lymphoma  activity.
        Dr. Teitell is the recipient of a Society Scholar Award -- a program  that provides funding to highly qualified investigators conducting original  research on leukemia, lymphoma or myeloma.
        "The goal of the Scholar program is to help advance promising original  research with the potential to have the highest impact on blood cancers,"  said Deborah Banker, Ph.D., the Society's vice president for research  communications. "Dr. Teitell's research shows great promise in leading to   more effective treatments for NHL patients."
        Dr. Teitell said that the Society's support was fundamental in moving  his research forward. "I am truly grateful to The Leukemia & Lymphoma  Society for having confidence in our work and providing our group with this  funding," he said. "I am optimistic that our efforts will improve outcomes   for NHL patients."
        About The Leukemia & Lymphoma Society
      The Leukemia & Lymphoma Society(R), headquartered in White Plains, NY,  with 66 chapters in the United States and Canada, is the world's largest  voluntary health organization dedicated to funding blood cancer research  and providing education and patient services. The Society's mission: Cure  leukemia, lymphoma, Hodgkin's disease and myeloma, and improve the quality  of life of patients and their families. Since its founding in 1949, the  Society has invested more than $483 million in research specifically  targeting leukemia, lymphoma and myeloma. Last year alone, the Society made  4.2 million contacts with patients, caregivers and healthcare  professionals.
        For more information about blood cancer, visit http://www.LLS.org/ or  call the Society's Information Resource Center (IRC), a call center staffed  by master's level social workers, nurses and health educators who provide  information, support and resources to patients and their families and  caregivers.
   The Leukemia & Lymphoma Society
 http://www.LLS.org/

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