Dimerization of SOX9 is required for chondrogenesis, but not for sex determination

Bernard, Pascal; Tang, Paisu; Liu, Siyuan; Dewing, Phoebe; Harley, Vincent R.; Vilain, Éric

doi:10.1093/hmg/ddg182

Cited by 149 publications

(137 citation statements)

References 39 publications

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“…Colored boxes in the lower panel indicate dimerization (codon 60–101) (Bernard et al. 2003), high‐mobility group ( HMG : codon 101–184), proline/glutamine/alanine ( PQA : codon 339–379), and proline/glutamine/serine‐rich ( PQS ‐rich: codon 386–509) domains (McDowall et al. 1999).…”

Section: Resultsmentioning

confidence: 99%

“…Patients with SOX9 mutations manifest campomelia, hypoplastic scapulae, pelvic anomalies, micrognathia, and cleft palate, collectively referred to as campomelic dysplasia (CD), although a certain percentage of mutation‐positive patients show a mild variant of CD that lacks campomelia (acampomelic CD: ACD) (Bernard et al. 2003; Michel‐Calemard et al. 2004; Staffler et al.…”

Section: Introductionmentioning

confidence: 99%

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Testicular dysgenesis/regression without campomelic dysplasia in patients carrying missense mutations and upstream deletion of SOX9

Katoh‐Fukui

Igarashi

Nagasaki

et al. 2015

Molec Gen & Gen Med

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SOX9 haploinsufficiency underlies campomelic dysplasia (CD) with or without testicular dysgenesis. Current understanding of the phenotypic variability and mutation spectrum of SOX9 abnormalities remains fragmentary. Here, we report three patients with hitherto unreported SOX9 abnormalities. These patients were identified through molecular analysis of 33 patients with 46,XY disorders of sex development (DSD). Patients 1–3 manifested testicular dysgenesis or regression without CD. Patients 1 and 2 carried probable damaging mutations p.Arg394Gly and p.Arg437Cys, respectively, in the SOX9 C‐terminal domain but not in other known 46,XY DSD causative genes. These substitutions were absent from ~120,000 alleles in the exome database. These mutations retained normal transactivating activity for the Col2a1 enhancer, but showed impaired activity for the Amh promoter. Patient 3 harbored a maternally inherited ~491 kb SOX9 upstream deletion that encompassed the known 32.5 kb XY sex reversal region. Breakpoints of the deletion resided within nonrepeat sequences and were accompanied by a short‐nucleotide insertion. The results imply that testicular dysgenesis and regression without skeletal dysplasia may be rare manifestations of SOX9 abnormalities. Furthermore, our data broaden pathogenic SOX9 abnormalities to include C‐terminal missense substitutions which lead to target‐gene‐specific protein dysfunction, and enhancer‐containing upstream microdeletions mediated by nonhomologous end‐joining.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Testicular dysgenesis/regression without campomelic dysplasia in patients carrying missense mutations and upstream deletion of SOX9

Katoh‐Fukui

Igarashi

Nagasaki

et al. 2015

Molec Gen & Gen Med

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“…However, the expression of collagen IIA was detected at relatively basal levels, suggesting other cofactors and optimal differentiation culture conditions may be needed to activate the gene sufficiently. In fact, SOX9 interacts with other cofactors, such as L-Sox5 and Sox6 for dimerization and subsequently activates cartilage-specific marker genes more effectively (Bernard et al, 2003;Ikeda et al, 2004). mES cells exhibit the very unique distribution of cell cycle: 15% in G1, 75% in S, and 10% in G2/M, respectively, supporting their infinite proliferation potentials in vitro without differentiation under LIF signals (Savatier et al, 2002).…”

Section: Discussionmentioning

confidence: 96%

“…SOX9 is the member of the SOX (Sry-type HMG box) family and predominantly expressed during mesenchymal condensation and cartilage formation in mouse embryos (Wright et al, 1995). In addition, SOX9 is known to be a key regulator for the expression of collagen II, IX, XI, and aggrecan, the major matrix proteins specific for chondrocytes through binding to the enhancer region (Bell et al, 1997;Lefebvre et al, 1997;Bridgewater et al, 1998;Sekiya et al, 2000;Bernard et al, 2003). SOX9 has been also reported to be required for chondrogenesis by the generation of SOX9-mutant ES cells and chimeric mice (Bi et al, 1999).…”

Section: Discussionmentioning

confidence: 99%

Overexpression of SOX9 in mouse embryonic stem cells directs the immediate chondrogenic commitment

Kim

Do²,

Yang³

et al. 2005

Exp Mol Med

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“…Traditional discovery of TF-TF cooperative interactions has typically involved detailed experimental dissection of one or a small number of promoter sequences [15][16][17]. Selected cases are further studied by crystallography, which has resulted in a steady but slow growth of TF complexes in the Protein Data Bank (PDB; approx.…”

Section: Introductionmentioning

confidence: 99%

Structure-aided prediction of mammalian transcription factor complexes in conserved non-coding elements

Guturu

Doxey

Wenger

et al. 2013

Phil. Trans. R. Soc. B

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Mapping the DNA-binding preferences of transcription factor (TF) complexes is critical for deciphering the functions of cis -regulatory elements. Here, we developed a computational method that compares co-occurring motif spacings in conserved versus unconserved regions of the human genome to detect evolutionarily constrained binding sites of rigid TF complexes. Structural data were used to estimate TF complex physical plausibility, explore overlapping motif arrangements seldom tackled by non-structure-aware methods, and generate and analyse three-dimensional models of the predicted complexes bound to DNA. Using this approach, we predicted 422 physically realistic TF complex motifs at 18% false discovery rate, the majority of which (326, 77%) contain some sequence overlap between binding sites. The set of mostly novel complexes is enriched in known composite motifs, predictive of binding site configurations in TF–TF–DNA crystal structures, and supported by ChIP-seq datasets. Structural modelling revealed three cooperativity mechanisms: direct protein–protein interactions, potentially indirect interactions and ‘through-DNA’ interactions. Indeed, 38% of the predicted complexes were found to contain four or more bases in which TF pairs appear to synergize through overlapping binding to the same DNA base pairs in opposite grooves or strands. Our TF complex and associated binding site predictions are available as a web resource at http://bejerano.stanford.edu/complex .

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Dimerization of SOX9 is required for chondrogenesis, but not for sex determination

Cited by 149 publications

References 39 publications

Testicular dysgenesis/regression without campomelic dysplasia in patients carrying missense mutations and upstream deletion of SOX9

Testicular dysgenesis/regression without campomelic dysplasia in patients carrying missense mutations and upstream deletion of SOX9

Overexpression of SOX9 in mouse embryonic stem cells directs the immediate chondrogenic commitment

Structure-aided prediction of mammalian transcription factor complexes in conserved non-coding elements

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