| Autor: |
Zajac, Allison, Baek, SeungHak, Salhab, Imad, Radecki, Melissa A., Kim, Sukwha, Hakonarson, Hakon, Nah, HyunDuck |
| Zdroj: |
American Journal of Medical Genetics. Part A; March 2010, Vol. 152 Issue: 3 p770-776, 7p |
| Abstrakt: |
Craniometaphyseal dysplasia is caused by mutations in ANKHankylosis, progressive homolog mouse in the majority of cases, and all of the reported mutations are single amino acid changes. Genomic DNA from an affected patient, his biological parents, and a sibling was amplified and ANKHwas sequenced. The affected patient had a complex heterozygous mutation in exon 7 c.936T > C, c.938C > G, c.942953delTGGTTGACGGAA, predicting p.Try290Gln and p.Trp292Glu295del. We studied the effect of the predicted mutation on the subcellular distribution of ANKH protein. Immunofluorescent labeling of COS7 cells transduced with normal or mutant Ank murine progressive ankylosis, showed that normal Ank localized to both the plasma membrane and cytoplasm, whereas mutant Ank was detected only in the cytoplasmic compartment. We propose that this craniometaphyseal dysplasia mutation causes a loss of ANKH protein expression and activity in the plasma membrane as a result of aberrant intracellular protein trafficking. © 2010 WileyLiss, Inc. |
| Databáze: |
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