Extension of the mutational and clinical spectrum of <i>SOX2</i> related disorders: Description of six new cases and a novel association with suprasellar teratoma

Blackburn, Patrick R.; Chacón‐Camacho, Oscar F.; Ortiz-González, Xilma R.; Reyes, Mariana; López-Uriarte, G. A.; Zarei, Shabnam; Bhoj, Elizabeth; Pérez-Solórzano, Sofía; Vaubel, Rachael A.; Murphree, Marine I.; Nava, Jessica; Cortés‐González, Vianney; Parisi, Joseph E.; Villanueva‐Mendoza, Cristina; Tirado-Torres, Iris G.; Liu, Dong; Klee, Eric W.; Pichurin, Pavel N.; Zenteno, Juan Carlos

doi:10.1002/ajmg.a.40644

Cited by 7 publications

(9 citation statements)

References 48 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…While many of the first cases in the literature with normal eyes and SOX2 variants were identified because other family members were found to have pathogenic variants (Chassaing et al, 2007; Mihelec et al, 2009; Stark et al, 2011; Zenteno et al, 2006), several were the first in their families, presenting with overlapping syndromic features including brain anomalies, hypogonadotropic hypogonadism (HH), developmental delay/intellectual disability (ID), seizures, or genital anomalies (Blackburn et al, 2018; Dennert et al, 2017; Errichiello et al, 2018; Kelberman et al, 2006; Pilz et al, 2019; Shima et al, 2017; Takagi et al, 2013). Some of these patients, on further examination, had slight ocular anomalies, such as narrowed palpebral fissure (Zenteno et al, 2006), mild retinal anomalies (Errichiello et al, 2018; Mihelec et al, 2009; Pilz et al, 2019; Shima et al, 2017; Takagi et al, 2013), subtle anterior segment anomalies (Dennert et al, 2017, Mihelec et al, 2009), ocular motility disorders (Errichiello et al, 2018; Pilz et al, 2019), or optic nerve hypoplasia (Kelberman et al, 2008).…”

Section: Discussionmentioning

confidence: 99%

Review of 37 patients with SOX2 pathogenic variants collected by the Anophthalmia/Microphthalmia Clinical Registry and DNA research study

Amlie‐Wolf

Bardakjian

Kopinsky

et al. 2021

American J of Med Genetics Pt A

View full text Add to dashboard Cite

SOX2 variants and deletions are a common cause of anophthalmia and microphthalmia (A/M). This article presents data from a cohort of patients with SOX2 variants, some of whom have been followed for 20+ years. Medical records from patients enrolled in the A/M Research Registry and carrying SOX2 variants were reviewed. Thirty‐seven patients were identified, ranging in age from infant to 30 years old. Eye anomalies were bilateral in 30 patients (81.1%), unilateral in 5 (13.5%), and absent in 2 (5.4%). Intellectual disability was present in all with data available and ranged from mild to profound. Seizures were noted in 18 of 27 (66.6%) patients, usually with abnormal brain MRIs (10/15, 66.7%). Growth issues were reported in 14 of 21 patients (66.7%) and 14 of 19 (73.7%) had gonadotropin deficiency. Genitourinary anomalies were seen in 15 of 19 (78.9%) male patients and 5 of 15 (33.3%) female patients. Patients with SOX2 nucleotide variants, whole gene deletions or translocations are typically affected with bilateral or unilateral microphthalmia and anophthalmia. Other associated features include intellectual disability, seizures, brain anomalies, growth hormone deficiency, gonadotropin deficiency, and genitourinary anomalies. Recommendations for newly diagnosed patients with SOX2 variants include eye exams, MRI of the brain and orbits, endocrine and neurology examinations. Since the clinical spectrum associated with SOX2 alleles has expanded beyond the originally reported phenotypes, we propose a broader term, SOX2‐associated disorder, for this condition.

show abstract

Section: Discussionmentioning

confidence: 99%

Review of 37 patients with SOX2 pathogenic variants collected by the Anophthalmia/Microphthalmia Clinical Registry and DNA research study

Amlie‐Wolf

Bardakjian

Kopinsky

et al. 2021

American J of Med Genetics Pt A

View full text Add to dashboard Cite

show abstract

“…At least 24 patients with heterozygous SOX2 pathogenic variants have been described in publications or genomic databases as having normal eyes in the presence of other features of SOX2 syndrome (Amlie‐Wolf et al, 2022; Bakrania et al, 2007; Blackburn et al, 2018; Chassaing et al, 2007; Dennert et al, 2017; Errichiello et al, 2018; Firth et al, 2009; Kelberman et al, 2006; Mihelec et al, 2009; Pilz et al, 2019; Shima et al, 2017; Stark et al, 2011; Takagi et al, 2014; Wang et al, 2008; Wang et al, 2022; Zenteno et al, 2006). On closer inspection, 11 of these patients had no ocular defects reported except for refractive errors or strabismus (Blackburn et al, 2018; Chassaing et al, 2007; Dennert et al, 2017; Firth et al, 2009; Stark et al, 2011; Wang et al, 2022; Zenteno et al, 2006), and on this basis, have been described in herein as having genuinely normal eyes. These are summarized in Table 1 along with our reported two patients.…”

Section: Discussionmentioning

confidence: 99%

“…As SOX2 is a single exon gene, these variants are not expected to invoke nonsense‐mediated mRNA decay (Bakrania et al, 2007; Ragge et al, 2005). Almost all SOX2 pathogenic variants reported to date appear to represent heterozygous loss of function, and thus it is difficult to determine any obvious genotype–phenotype correlation within this sub‐category of patients with normal eyes (Blackburn et al, 2018; Stark et al, 2011; Suzuki et al, 2014). Other reports have observed that identical pathogenic SOX2 variants can lead to ocular and extraocular defects of varying severity (Blackburn et al, 2018; Wang et al, 2022).…”

Section: Discussionmentioning

confidence: 99%

SOX2 pathogenic variants with normal eyes: Expanding the phenotypic spectrum

Okoye

Capasso

Kopinsky

et al. 2023

American J of Med Genetics Pt A

View full text Add to dashboard Cite

SOX2 pathogenic variants, though rare, constitute the most commonly known genetic cause of clinical anophthalmia and microphthalmia. However, patients without major ocular malformation, but with multi-system developmental disorders, have been reported, suggesting that the range of clinical phenotypes is broader than previously appreciated. We detail two patients with bilateral structurally normal eyes along with 11 other previously published patients. Our findings suggest that there is no obvious phenotypic or genotypic pattern that may help set apart patients with normal eyes.Our patients provide further evidence for broadening the phenotypic spectrum of SOX2 mutations and re-appraising the designation of SOX2 disorder as an anophthalmia/microphthalmia syndrome. We emphasize the importance of considering SOX2 pathogenic variants in the differential diagnoses of individuals with normal eyes, who may have varying combinations of features such as developmental delay, urogenital abnormalities, gastro-intestinal anomalies, pituitary dysfunction, midline structural anomalies, and complex movement disorders, seizures or other neurological issues.

show abstract

“…Mutations in other genes involved in the regulation of the Wnt/β-catenin signaling pathway have been reported in SOD cases: SOX2 (3q26.33) (OMIM 184429), SOX3 (Xq27.1) (OMIM 313430), OTX2 (14q22.3) (OMIM 600037), TCF7L1 (2p11.2) (OMIM 604652) or TAX1BP3 (17p13.2) (OMIM 616484). SOX2 mutations are associated with severe eye abnormalities, and additional features (genital anomalies, esophageal atresia, intellectual disability, seizures) (Blackburn et al, 2018). SOX3 duplications/point mutations have been reported in cases with hypopituitarism and/or intellectual disability (Arya et al, 2019;Li et al, 2022).…”

Section: Septo-optic Dysplasia (Sod)mentioning

confidence: 99%

Genetic heterogeneity in corpus callosum agenesis

et al. 2022

View full text Add to dashboard Cite

The corpus callosum is the largest white matter structure connecting the two cerebral hemispheres. Agenesis of the corpus callosum (ACC), complete or partial, is one of the most common cerebral malformations in humans with a reported incidence ranging between 1.8 per 10,000 livebirths to 230–600 per 10,000 in children and its presence is associated with neurodevelopmental disability. ACC may occur as an isolated anomaly or as a component of a complex disorder, caused by genetic changes, teratogenic exposures or vascular factors. Genetic causes are complex and include complete or partial chromosomal anomalies, autosomal dominant, autosomal recessive or X-linked monogenic disorders, which can be either de novo or inherited. The extreme genetic heterogeneity, illustrated by the large number of syndromes associated with ACC, highlight the underlying complexity of corpus callosum development. ACC is associated with a wide spectrum of clinical manifestations ranging from asymptomatic to neonatal death. The most common features are epilepsy, motor impairment and intellectual disability. The understanding of the genetic heterogeneity of ACC may be essential for the diagnosis, developing early intervention strategies, and informed family planning. This review summarizes our current understanding of the genetic heterogeneity in ACC and discusses latest discoveries.

show abstract

Extension of the mutational and clinical spectrum of SOX2 related disorders: Description of six new cases and a novel association with suprasellar teratoma

Cited by 7 publications

References 48 publications

Review of 37 patients with SOX2 pathogenic variants collected by the Anophthalmia/Microphthalmia Clinical Registry and DNA research study

Review of 37 patients with SOX2 pathogenic variants collected by the Anophthalmia/Microphthalmia Clinical Registry and DNA research study

SOX2 pathogenic variants with normal eyes: Expanding the phenotypic spectrum

Genetic heterogeneity in corpus callosum agenesis

Contact Info

Product

Resources

About