Clinical and molecular characterization of a Brazilian cohort of campomelic dysplasia patients, and identification of seven new SOX9 mutations

Mattos, Eduardo Preusser de; Sanseverino, Maria Teresa Vieira; Magalhães, José Antônio A.; Leite, Júlio César Loguercio; Félix, Têmis Maria; Todeschini, Luiz Alberto; Cavalcanti, Denise Pontes; Schüler‐Faccini, Lavínia

doi:10.1590/s1415-475738120140147

Cited by 8 publications

(5 citation statements)

References 38 publications

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“…In addition to these phenotypes in the developing bones and gonads, patients with CMPD may also show defects within other tissues in which SOX9 is expressed, such as brain (e.g., the absence of olfactory bulbs), heart, kidney and lung abnormalities [ 132 ]. Loss-of-function mutations within the coding sequence of SOX9 occur, for example, in the DNA-binding domain HMG-box, the nuclear localisation signals (NLS), or in the transactivating domain ( Figure 6 ) [ 82 , 101 , 128 , 131 , 134 , 135 , 136 , 137 , 138 , 139 , 140 , 141 , 142 , 143 , 144 , 145 , 146 , 147 , 148 , 149 , 150 , 151 , 152 , 153 , 154 , 155 , 156 ]. In some CMPD patients with associated sex reversal, the SOX9 coding sequence is not affected, but translocation breakpoints have been identified in the SOX9 regulatory region up to several hundred kb upstream of SOX9 .…”

Section: Disorders Arising From Sox9 Mutations In Humansmentioning

confidence: 99%

Diverse Regulation but Conserved Function: SOX9 in Vertebrate Sex Determination

Vining

Ming

Bagheri‐Fam

et al. 2021

Genes

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Sex determination occurs early during embryogenesis among vertebrates. It involves the differentiation of the bipotential gonad to ovaries or testes by a fascinating diversity of molecular switches. In most mammals, the switch is SRY (sex determining region Y); in other vertebrates it could be one of a variety of genes including Dmrt1 or dmy. Downstream of the switch gene, SOX9 upregulation is a central event in testes development, controlled by gonad-specific enhancers across the 2 Mb SOX9 locus. SOX9 is a ‘hub’ gene of gonadal development, regulated positively in males and negatively in females. Despite this diversity, SOX9 protein sequence and function among vertebrates remains highly conserved. This article explores the cellular, morphological, and genetic mechanisms initiated by SOX9 for male gonad differentiation.

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Section: Disorders Arising From Sox9 Mutations In Humansmentioning

confidence: 99%

Diverse Regulation but Conserved Function: SOX9 in Vertebrate Sex Determination

Vining

Ming

Bagheri‐Fam

et al. 2021

Genes

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“…In prehypertrophic chondrocytes, instead, Sox9 is responsible for the activation of Col10a1 , thereby initiating the onset of hypertrophy ( 82 ). Mutations of SOX9 have been associated with campomelic dysplasia, a severe skeletal dysplasia characterized by congenital bowing and angulation of long bones and other skeletal and extraskeletal defects ( 115 ).…”

Section: Shox-related Pathwaysmentioning

confidence: 99%

A Track Record on SHOX: From Basic Research to Complex Models and Therapy

2016

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SHOX deficiency is the most frequent genetic growth disorder associated with isolated and syndromic forms of short stature. Caused by mutations in the homeobox gene SHOX, its varied clinical manifestations include isolated short stature, Léri-Weill dyschondrosteosis, and Langer mesomelic dysplasia. In addition, SHOX deficiency contributes to the skeletal features in Turner syndrome. Causative SHOX mutations have allowed downstream pathology to be linked to defined molecular lesions. Expression levels of SHOX are tightly regulated, and almost half of the pathogenic mutations have affected enhancers. Clinical severity of SHOX deficiency varies between genders and ranges from normal stature to profound mesomelic skeletal dysplasia. Treatment options for children with SHOX deficiency are available. Two decades of research support the concept of SHOX as a transcription factor that integrates diverse aspects of bone development, growth plate biology, and apoptosis. Due to its absence in mouse, the animal models of choice have become chicken and zebrafish. These models, therefore, together with micromass cultures and primary cell lines, have been used to address SHOX function. Pathway and network analyses have identified interactors, target genes, and regulators. Here, we summarize recent data and give insight into the critical molecular and cellular functions of SHOX in the etiopathogenesis of short stature and limb development.

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“…The range of functions that Sox proteins serve is broad, including maintaining stem cell features, restricting lineage, and directing terminal differentiation. Germline SOX9 heterozygous inactivating missense and nonsense mutations result in campomelic dysplasia, a syndrome resulting in skeletal malformations, central nervous system dysfunction, as well as abnormalities in other organs [1–2]. …”

Section: Introductionmentioning

confidence: 99%

Recurrent, truncating SOX9 mutations are associated with SOX9 overexpression, KRAS mutation, and TP53 wild type status in colorectal carcinoma

et al. 2016

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PurposeThe extent to which the developmental transcription factor SOX9 functions as an oncogene or tumor suppressor in colorectal carcinoma (CRC) is debatable. We aimed to clarify the effect of SOX9 mutations on SOX9 protein expression and their association with known molecular subtypes and clinical characteristics in advanced CRC.Experimental DesignNext generation sequencing data (MSK-IMPACT) from CRC patients was used to interrogate SOX9, KRAS, NRAS, BRAF, TP53, APC, and PIK3CA. Mutant and wild type (WT) SOX9 cases underwent immunohistochemical (IHC) staining to assess protein expression. SOX9 allele-specific copy number was assessed by Affymetrix Oncoscan array.ResultsSOX9 was mutated in 38 of 353 (10.7%) CRC, of which 82% were frameshift or nonsense. Compared to SOX9 WT, SOX9 mutation was strongly associated with coexistent mutant KRAS (p=0.0001) and WT TP53 (p=0.0004). SOX9 was overexpressed in both SOX9 mutant and WT CRC. Among SOX9 mutants, the highest expression was noted for truncating exon 3 mutants (mean H scores 239±105 versus 147±119, p value=0.02). Further, SOX9 truncating mutants with loss of the WT allele demonstrated protein overexpression indicating the WT protein was not required for protein stabilization.ConclusionsSOX9 is overexpressed in CRC, including those with recurrent distal truncating mutations. The latter has structural similarity to the oncogenic isoform MiniSOX9, which is distally truncated due to aberrant splicing. This information suggests that truncated SOX9 has oncogenic features. SOX9 mutations are highly enriched in KRAS mutant and TP53 wild type CRC; and may provide a therapeutic target in approximately 11% of CRC.

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Clinical and molecular characterization of a Brazilian cohort of campomelic dysplasia patients, and identification of seven new SOX9 mutations

Cited by 8 publications

References 38 publications

Diverse Regulation but Conserved Function: SOX9 in Vertebrate Sex Determination

Diverse Regulation but Conserved Function: SOX9 in Vertebrate Sex Determination

A Track Record on SHOX: From Basic Research to Complex Models and Therapy

Recurrent, truncating SOX9 mutations are associated with SOX9 overexpression, KRAS mutation, and TP53 wild type status in colorectal carcinoma

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