论文信息 - Two novel translocation breakpoints upstream of SOX9 define borders of the proximal and distal breakpoint cluster region in campomelic dysplasia - 字舞流文

Two novel translocation breakpoints upstream of SOX9 define borders of the proximal and distal breakpoint cluster region in campomelic dysplasia

The semilethal skeletal malformation syndrome campomelic dysplasia (CD) with or without XY sex reversal is caused by mutations within the SOX9 gene on 17q24.3 or by chromosomal aberrations (translocations, inversions or deletions) with breakpoints outside the SOX9 coding region. The previously published CD translocation breakpoints upstream of SOX9 fall into two clusters: a proximal cluster with breakpoints between 50–300 kb and a distal cluster with breakpoints between 899–932 kb. Here, we present clinical, cytogenetic and molecular data from two novel CD translocation cases. Case 1 with karyotype 46,XY,t(1;17)(q42.1;q24.3) has characteristic symptoms of CD, including mild tibial bowing, cryptorchidism and hypospadias. By standard fluorescence in situ hybridization (FISH) and by high‐resolution fiber FISH, the 17q breakpoint was mapped 375 kb from SOX9, defining the centromeric border of the proximal breakpoint cluster region. Case 2 with karyotype 46,X,t(Y;17)(q11.2;q24.3) has the acampomelic form of CD and complete XY sex reversal. By FISH and somatic cell hybrid analysis, the 17q breakpoint was mapped 789 kb from SOX9, defining the telomeric border of the distal breakpoint cluster region. We discuss the structure of the 1 Mb cis‐control region upstream of SOX9 and the correlation between the position of the 14 mapped translocation breakpoints with respect to disease severity and XY sex reversal.

P. Stankiewicz | M. Smyk | G. Scherer | S. Yatsenko | A. Shanske | M. Theurl | M. Leipoldt | P Stankiewicz | G Scherer | M Leipoldt | M Erdel | G A Bien-Willner | M Smyk | M Theurl | S A Yatsenko | J R Lupski | A H Lane | A L Shanske | J. Lupski | G. Bien-Willner | M. Erdel | SA Yatsenko | AH Lane | S. Yatsenko

[1] B. Oostra,et al. A long-range Shh enhancer regulates expression in the developing limb and fin and is associated with preaxial polydactyly. , 2003, Human molecular genetics.

[2] P N Goodfellow,et al. Deletion of long-range regulatory elements upstream of SOX9 causes campomelic dysplasia. , 1998, Proceedings of the National Academy of Sciences of the United States of America.

[3] Jobst Meyer,et al. Translocation breakpoints in three patients with campomelic dysplasia and autosomal sex reversal map more than 130 kb from SOX9 , 1996, Human Genetics.

[4] N. Svenningsen,et al. Camptomelic dwarfism. A genetically determined mesenchymal disorder combined with sex reversal. , 2009, Hereditas.

[5] O. Haas,et al. Mutational analysis of the SOX9 gene in campomelic dysplasia and autosomal sex reversal: lack of genotype/phenotype correlations. , 1997, Human molecular genetics.

[6] Colin E Bishop,et al. Long-range activation of Sox9 in Odd Sex (Ods) mice. , 2004, Human molecular genetics.

[7] J. Opitz,et al. The campomelic syndrome: review, report of 17 cases, and follow-up on the currently 17-year-old boy first reported by Maroteaux et al in 1971. , 1983, American journal of medical genetics.

[8] B. Kerr,et al. Domain disruption and mutation of the bZIP transcription factor, MAF, associated with cataract, ocular anterior segment dysgenesis and coloboma. , 2002, Human molecular genetics.

[9] P. Stankiewicz,et al. Position effects due to chromosome breakpoints that map approximately 900 Kb upstream and approximately 1.3 Mb downstream of SOX9 in two patients with campomelic dysplasia. , 2005, American journal of human genetics.

[10] Paul A. Overbeek,et al. A transgenic insertion upstream of Sox9 is associated with dominant XX sex reversal in the mouse , 2000, Nature Genetics.

[11] Y. Nakamura,et al. Isolation of a testis-specific cDNA on chromosome 17q from a region adjacent to the breakpoint of t(12;17) observed in a patient with acampomelic campomelic dysplasia and sex reversal. , 1996, Human molecular genetics.

[12] C. Ferraz,et al. Comparative genomics of the SOX9 region in human and Fugu rubripes: conservation of short regulatory sequence elements within large intergenic regions. , 2001, Genomics.

[13] M. Nóbrega,et al. Scanning Human Gene Deserts for Long-Range Enhancers , 2003, Science.

[14] A. Sturtevant. The Effects of Unequal Crossing over at the Bar Locus in Drosophila. , 1925, Genetics.

[15] J. W. Foster,et al. Mutations in SOX9, the gene responsible for Campomelic dysplasia and autosomal sex reversal. , 1995, American journal of human genetics.

[16] A. Offiah,et al. The phenotype of survivors of campomelic dysplasia , 2002, Journal of medical genetics.

[17] Katherine L Hill-Harfe,et al. Fine mapping of chromosome 17 translocation breakpoints > or = 900 Kb upstream of SOX9 in acampomelic campomelic dysplasia and a mild, familial skeletal dysplasia. , 2005, American journal of human genetics.

[18] U. Dohrmann,et al. Long-range upstream and downstream enhancers control distinct subsets of the complex spatiotemporal Sox9 expression pattern. , 2006, Developmental biology.

[19] P. Stankiewicz,et al. Position effects due to chromosome breakpoints that map ∼900 Kb upstream and ∼1.3 Mb downstream of SOX9 in two patients with campomelic dysplasia , 2005 .

[20] N. Tommerup,et al. Autosomal sex reversal and campomelic dysplasia are caused by mutations in and around the SRY-related gene SOX9 , 1994, Cell.

[21] B. Birren,et al. Campomelic dysplasia translocation breakpoints are scattered over 1 Mb proximal to SOX9: evidence for an extended control region. , 1999, American journal of human genetics.

[22] G. Utermann,et al. Counting the repetitive kringle-IV repeats in the gene encoding human apolipoprotein(a) by fibre-FISH , 1999, Nature Genetics.

[23] L. Bolund,et al. Assignment of an autosomal sex reversa– locus (SRA1) and campomelic dysplasia (CMPD1) to 17q24.3–q25.1 , 1993, Nature Genetics.

[24] T. Dobzhansky. POSITION EFFECTS ON GENES , 1936 .

[25] K. Lindenberg,et al. Screening of the 1 Mb SOX9 5′ control region by array CGH identifies a large deletion in a case of campomelic dysplasia with XY sex reversal , 2004, Journal of Medical Genetics.

[26] Sahar Mansour,et al. Campomelic dysplasia and autosomal sex reversal caused by mutations in an SRY-related gene , 1994, Nature.

[27] C. Cremers,et al. Identification of a hot spot for microdeletions in patients with X-linked deafness type 3 (DFN3) 900 kb proximal to the DFN3 gene POU3F4. , 1996, Human molecular genetics.

[28] M. Pembrey,et al. A clinical and genetic study of campomelic dysplasia. , 1995, Journal of medical genetics.

[29] E. Maltby,et al. Campomelic dysplasia associated with a de novo 2q;17q reciprocal translocation. , 1992, Journal of medical genetics.