A novel locus for parietal foramina maps to chromosome 4q21-q23 |
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| Authors: | Gang?Chen,Desan?Zhang,Guoying?Feng,Wanqing?Liu,Lin?He author-information" > author-information__contact u-icon-before" > mailto:helin@sjtu.edu.cn" title=" helin@sjtu.edu.cn" itemprop=" email" data-track=" click" data-track-action=" Email author" data-track-label=" " >Email author |
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| Affiliation: | (1) Shanghai Research Center of Life Sciences, Chinese Academy of Sciences, Shanghai, China;(2) Epidemic Prevention Station of Gansu Province, Lanzhou, China;(3) Bio-X Life Science Research Center, Shanghai Jiao Tong University, Hao Ran Building, 1954 Hua Shan Road, PO Box 501, 200030 Shanghai, China |
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| Abstract: | Parietal foramina [PFM], inherited usually in an autosomal dominant mode, is an extremely rare developmental defect characterized by a symmetrical, oval hole in the parietal bone. It can be present as either an isolated or a syndromic feature. PFM types 1 and 2 (PFM1 and PFM2) have been found to be caused by mutations in the MSX2 and ALX4 genes, located to chromosomes 5 and 11, respectively. After exclusion of both the above loci in a large Chinese pedigree with autosomal dominant PFM, a genome-wide search revealed a linkage of the PFM to markers at the 4q21-q23 region. The maximum LOD score from two-point linkage analysis is 3.87 for marker D4S2961. Analysis of co-segregated haplotype localized the region to a 20-cM interval that flanks D4S392 and D4S2945. Therefore, we concluded that the PFM in the family is a new PFM locus. Although three genes, BMPR1B, PP1 and IBSP, are located to 4q21-q25 and their functions are related to bone morphogenesis, no mutations were identified by sequencing analysis of their exons. |
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| Keywords: | Parietal bone Chromosome 4 Genetics Linkage Mapping |
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