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A cluster of translocation breakpoints in 2q37 is associated with overexpression of NPPC in patients with a similar overgrowth phenotype

✍ Scribed by Anne Moncla; Chantal Missirian; Pierre Cacciagli; Eve Balzamo; Laurence Legeai-Mallet; Jean-Luc Jouve; Brigitte Chabrol; Martine Le Merrer; Ghislaine Plessis; Laurent Villard; Nicole Philip


Book ID
102261284
Publisher
John Wiley and Sons
Year
2007
Tongue
English
Weight
297 KB
Volume
28
Category
Article
ISSN
1059-7794

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✦ Synopsis


Communicated by Garry R. Cutting

Overexpression of the C-type natriuretic peptide, encoded by the NPPC gene in 2q37.1, was recently reported in a patient presenting an overgrowth phenotype and a balanced t(2;7)(q37.1;q21.3) translocation. We present clinical, cytogenetic, and molecular data from two additional patients carrying balanced translocations involving the same 2q37.1 chromosome band and chromosomes 8 and 13, respectively. The clinical phenotype of these patients is very similar to the first patient described. In addition to the overgrowth syndrome, there is evidence of generalized cartilage dysplasia. In these two new cases, we found overexpression of NPPC, confirming that this unusual overgrowth phenotype in humans is due to the overexpression of this gene. The involvement of three different chromosomes and a cluster of breakpoints around the NPPC gene suggests that the overexpression of this gene in translocation patients could be due to its separation from a negative regulatory element located on chromosome 2, which would constitute a previously undescribed mutational mechanism.


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