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  • Alterations in CDH15 and KIRREL3 in patients with mild to severe intellectual disability.

Alterations in CDH15 and KIRREL3 in patients with mild to severe intellectual disability.

American journal of human genetics (2008-11-18)
Kavita Bhalla, Yue Luo, Tim Buchan, Michael A Beachem, Gregory F Guzauskas, Sydney Ladd, Shelly J Bratcher, Richard J Schroer, Janne Balsamo, Barbara R DuPont, Jack Lilien, Anand K Srivastava
摘要

Cell-adhesion molecules play critical roles in brain development, as well as maintaining synaptic structure, function, and plasticity. Here we have found the disruption of two genes encoding putative cell-adhesion molecules, CDH15 (cadherin superfamily) and KIRREL3 (immunoglobulin superfamily), by a chromosomal translocation t(11;16) in a female patient with intellectual disability (ID). We screened coding regions of these two genes in a cohort of patients with ID and controls and identified four nonsynonymous CDH15 variants and three nonsynonymous KIRREL3 variants that appear rare and unique to ID. These variations altered highly conserved residues and were absent in more than 600 unrelated patients with ID and 800 control individuals. Furthermore, in vivo expression studies showed that three of the CDH15 variations adversely altered its ability to mediate cell-cell adhesion. We also show that in neuronal cells, human KIRREL3 colocalizes and interacts with the synaptic scaffolding protein, CASK, recently implicated in X-linked brain malformation and ID. Taken together, our data suggest that alterations in CDH15 and KIRREL3, either alone or in combination with other factors, could play a role in phenotypic expression of ID in some patients.

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Sigma-Aldrich
多聚甲醛, prilled, 95%
Sigma-Aldrich
多聚甲醛, powder, 95%
Sigma-Aldrich
多聚甲醛, reagent grade, crystalline
Sigma-Aldrich
Taq DNA聚合酶 来源于水生栖热菌, with 10× PCR reaction buffer containing MgCl2
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Taq DNA聚合酶 来源于水生栖热菌, with 10× PCR reaction buffer without MgCl2
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多聚甲醛, meets analytical specification of DAC, 95.0-100.5%