Open AccessLoss-of-Function Mutations in HPSE2 Cause the Autosomal Recessive Urofacial Syndrome
Author(s) -
Junfeng Pang,
Shu Zhang,
Ping Yang,
Bobbilynn HawkinsLee,
Jixin Zhong,
Yushan Zhang,
Bernardo Ochoa,
José A. G. Agúndez,
MarieAntoinette Voelckel,
Weikuan Gu,
Wen-Cheng Xiong,
Lin Mei,
Jin-Xiong She,
CongYi Wang
Publication year - 2010
Publication title -
the american journal of human genetics
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 6.661
H-Index - 302
eISSN - 1537-6605
pISSN - 0002-9297
DOI - 10.1016/j.ajhg.2010.04.016
Subject(s) - gene , heparanase , loss function , genetics , biology , locus (genetics) , homology (biology) , heparan sulfate , phenotype , cell
Previously, we localized the defective gene for the urofacial syndrome (UFS) to a region on chromosome 10q24 by homozygosity mapping. We now report evidence that Heparanse 2 (HPSE2) is the culprit gene for the syndrome. Mutations with a loss of function in the Heparanase 2 (HPSE2) gene were identified in all UFS patients originating from Colombia, the United States, and France. HPSE2 encodes a 592 aa protein that contains a domain showing sequence homology to the glycosyl hydrolase motif in the heparanase (HPSE) gene, but its exact biological function has not yet been characterized. Complete loss of HPSE2 function in UFS patients suggests that HPSE2 may be important for the synergic action of muscles implicated in facial expression and urine voiding.
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