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Building the lymphatic drainage system
Normal valve-containing lymph vessels (left) fail to form in mice that lack Foxc2 and NFATc1 (right). The study by Norrmen et al. suggests that these two transcription factors direct the building of mature lymph-collecting vessels by coming together to regulate target gene loci.
Credit: Norrmen, C., et al. 2009. J. Cell Biol. doi:10.1083/jcb.200901104. The engineers are the transcription factors, Foxc2 and NFATc1. Foxc2 had been implicated in lymph vessel development already, but Norrmn and his colleagues have now observed that the factor specifically regulates a late stage of lymph development when large, valve-containing vessels arise from more primitive capillaries. The study will be published online April 27 (www.jcb.org) and will appear in the May 4 print issue of the Journal of Cell Biology Foxc2 built the lymph vessel valves with the help of NFATc1, which was a known heart valve engineer. Norrmn and his colleagues also showed that Foxc2 and NFATc1 physically interact and that a number of DNA binding sites for the two transcription factors are closely linked. This latter finding generated a long list of target genes that might be controlled by the two factors. The team now plans to investigate these targets as well as to work out the upstream molecular pathways controlling Foxc2 and NFATc1. Whatever the mechanisms, if the team can show that Foxc2 and NFATc1 also prompt lymph vessel regeneration in adults, boosting these factors could help patients with lymph drainage problems including those that have suffered extensive tissue injuries, or have had lymph nodes removed as part of cancer therapy. Posted by: Emily Source |
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