| Literature DB >> 27519652 |
Julie Soblet1, Jaakko Kangas2, Marjut Nätynki2, Antonella Mendola1, Raphaël Helaers1, Melanie Uebelhoer1, Mika Kaakinen2, Maria Cordisco3, Anne Dompmartin4, Odile Enjolras5, Simon Holden6, Alan D Irvine7, Loshan Kangesu8, Christine Léauté-Labrèze9, Agustina Lanoel3, Zerina Lokmic10, Saskia Maas11, Maeve A McAleer7, Anthony Penington10, Paul Rieu12, Samira Syed13, Carine van der Vleuten14, Rosemarie Watson7, Steven J Fishman15, John B Mulliken15, Lauri Eklund2, Nisha Limaye1, Laurence M Boon16, Miikka Vikkula17.
Abstract
Blue rubber bleb nevus syndrome (Bean syndrome) is a rare, severe disorder of unknown cause, characterized by numerous cutaneous and internal venous malformations; gastrointestinal lesions are pathognomonic. We discovered somatic mutations in TEK, the gene encoding TIE2, in 15 of 17 individuals with blue rubber bleb nevus syndrome. Somatic mutations were also identified in five of six individuals with sporadically occurring multifocal venous malformations. In contrast to common unifocal venous malformation, which is most often caused by the somatic L914F TIE2 mutation, multifocal forms are predominantly caused by double (cis) mutations, that is, two somatic mutations on the same allele of the gene. Mutations are identical in all lesions from a given individual. T1105N-T1106P is recurrent in blue rubber bleb nevus, whereas Y897C-R915C is recurrent in sporadically occurring multifocal venous malformation: both cause ligand-independent activation of TIE2, and increase survival, invasion, and colony formation when expressed in human umbilical vein endothelial cells.Entities:
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Year: 2016 PMID: 27519652 DOI: 10.1016/j.jid.2016.07.034
Source DB: PubMed Journal: J Invest Dermatol ISSN: 0022-202X Impact factor: 8.551