Bi-allelic TMEM94 Truncating Variants Are Associated with Neurodevelopmental Delay, Congenital Heart Defects, and Distinct Facial Dysmorphism

Stephen, Joshi; Maddirevula, Sateesh; Nampoothiri, Sheela; Burke, John D.; Herzog, Matthew; Shukla, Anju; Steindl, Katharina; Eskin, Ascia; Patil, Siddaramappa J.; Joset, Pascal; Lee, Hane; Garrett, Lisa; Yokoyama, Tadafumi; Balanda, Nicholas; Bodine, Steven P.; Tolman, Nathanial J.; Zerfas, Patricia M.; Zheng, Allison; Ramantani, Georgia; Girisha, Katta M.; Rivas, Cecilia; Suresh, Pujar Venkatesh; Elkahloun, Abdel G.; Alsaif, Hessa S.; Wakil, Salma M.; Mahmoud, Laila; Ali, Rehab; Procházková, Michaela; Kulkarni, Ashok B.; Ben‐Omran, Tawfeg; Çolak, Dilek; Morris, H Douglas; Rauch, Anita; Martínez‐Agosto, Julian A.; Nelson, Stanley F.; Alkuraya, Fowzan S.; Gahl, William A.; Malicdan, May Christine V.

doi:10.1016/j.ajhg.2018.11.001

Cited by 18 publications

(21 citation statements)

References 63 publications

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“…The well-established environmental factors underlying CHD include maternal conditions (such as innutrition, viral infection and endocrine disorder) and exposures to toxic chemicals, therapeutic drugs, or ionizing radiation during pregnancy (Patel and Burns, 2013). However, increasing studies underscore the genetic defects underpinning CHD, and variations in over 70 genes, encompassing those encoding transcription factors, signaling molecules, and sarcomeric proteins, have been involved in CHD (Bashamboo et al, 2018;Cantù et al, 2018;Jaouadi et al, 2018;Li et al, 2018a,c;Lombardo et al, 2018;Manheimer et al, 2018;Pierpont et al, 2018;Razmara and Garshasbi, 2018;Stephen et al, 2018;Xu et al, 2018;Yu Z et al, 2018;Alankarage et al, 2019;Gao et al, 2019;Kalayinia et al, 2019Kalayinia et al, , 2020Ma et al, 2019;Wang J et al, 2019, Wang Z et al, 2019Watkins et al, 2019;Zhu et al, 2019;Faucherre et al, 2020;Shabana et al, 2020;Zhao et al, 2020). Among the recognized CHD-causative genes, the majority code for cardiac transcription factors, encompassing TBX5, GATA4, and NKX2-5 (Li and Yang, 2017).…”

Section: Introductionmentioning

confidence: 99%

A novel TBX5 mutation predisposes to familial cardiac septal defects and atrial fibrillation as well as bicuspid aortic valve

Jiang

Zhao

et al. 2020

Genet. Mol. Biol.

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Section: Introductionmentioning

confidence: 99%

A novel TBX5 mutation predisposes to familial cardiac septal defects and atrial fibrillation as well as bicuspid aortic valve

Jiang

Zhao

et al. 2020

Genet. Mol. Biol.

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“…It is well known that gene defects in many members of the transmembrane protein family, such as TMEM138 [ 9 ], TMEM165 [ 10 ], TMEM231 [ 11 ], TMEM237 [ 12 ], TMEM67 [ 13 ], and TMEM5 [ 14 ] are associated with fetal anomalies. TMEM94 defects have been reported with a prenatal history of omphalocele, atrioventricular septal defect (AVSD), and intestinal malrotation, which was surgically corrected after birth in a Turkish patient aged 24 years of age [ 1 ]. The previous report also included three families with Arabian ancestry (from Oman, Qatar, and Egypt).…”

Section: Resultsmentioning

confidence: 99%

“…In both families, cardiac abnormality was the obvious structural irregularity identified by antenatal ultrasound. The loss of function variants detected in these two fetuses are correlated to the cardiac abnormality phenotype observed in the mouse model [ 1 ]. The identification of these two novel mutations increases the spectrum of pathogenic variants in TMEM94 that associated with IDDCDF.…”

Section: Resultsmentioning

confidence: 99%

“…Neurodevelopmental disorders are genetically and phenotypically heterogeneous conditions and can be accompanied by congenital heart defects and dysmorphic features. Intellectual developmental disorder with cardiac defects and dysmorphic facies (IDDCDF, MIM 618316) is a recently described neurodevelopmental disorder, which is characterized by global developmental delay, intellectual disability and speech delay, congenital cardiac malformations, and dysmorphic facial features [ 1 ]. It was initially reported in ten patients from six unrelated families with an autosomal recessive pattern of inheritance.…”

Section: Introductionmentioning

confidence: 99%

“…TMEM94 was mapped to chromosome 17q25.1 [ 2 ] and consisted of 31 coding exons (RefSeq NM_014738), which encoded for an uncharacterized transmembrane nuclear protein. In a murine model, homozygous loss of TMEM94 was embryonically lethal and led to craniofacial defects, cardiac abnormalities, and abnormal neuronal migration in the central nervous system that mimicked human phenotype [ 1 ]. To date, all of the seven mutations in TMEM94 were predicted to result in truncated proteins lacking the highly conserved C-terminal domain and showed significantly decreased TMEM94 expression [ 1 ].…”

Section: Introductionmentioning

confidence: 99%

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Fetal Anomalies Associated with Novel Pathogenic Variants in TMEM94

Al‐Hamed

Alsahan

Tulbah

et al. 2020

Genes

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Background: Intellectual developmental disorder with cardiac defects and dysmorphic facies (IDDCDF, MIM 618316) is a newly described disorder. It is characterized by global developmental delay, intellectual disability and speech delay, congenital cardiac malformations, and dysmorphic facial features. Biallelic pathogenic variants of TMEM94 are associated with IDDCDF. Methods and Results: In a prenatal setting, where fetal abnormalities were detected using antenatal sonography, we used trio-exome sequencing (trio-ES) in conjunction with chromosomal microarray analysis (CMA) to identify two novel homozygous loss of function variants in the TMEM94 gene (c.606dupG and c.2729-2A>G) in two unrelated Saudi Arabian families. Conclusions: This study provides confirmation that TMEM94 variants may cause IDDCDF. For the first time we describe the pathogenicity of TMEM94 defects detected during the prenatal period.

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An investigation of the etiology and follow‐up findings in 35 children with overgrowth syndromes, including biallelic SUZ12 variant

Ülker

Alkaya

Çağlayan

et al. 2023

American J of Med Genetics Pt A

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Overgrowth-intellectual disability (OGID) syndromes are clinically and genetically heterogeneous group of disorders. The aim of this study was to examine the molecular etiology and long-term follow-up findings of Turkish OGID cohort. Thirty-five children with OGID were included in the study. Single gene sequencing, clinical exome analysis, chromosomal microarray analysis and whole exome sequencing were performed. Five pathogenic copy number variants were detected in the patients; three of them located on chromosome 5q35.2 (encompassing NSD1), others on 9q22.3 and 22q13.31. In 19 of 35 patients; we identified pathogenic variants in OGID genes associated with epigenetic regulation, NSD1 (n = 15), HIST1H1E (n = 1), SETD1B(n = 1), and SUZ12 (n = 2). The pathogenic variants in PIK3CA (n = 2), ABCC9 (n = 1), GPC4 (n = 2), FIBP (n = 1), and TMEM94 (n = 1) which had a role in other growth pathways were detected in seven patients. The diagnostic yield was 31/35(88%).Twelve pathogenic variants were novel. The common facial feature of the patients was prominent forehead. The patients with Sotos syndrome were observed to have milder intellectual disability than patients with other OGID syndromes. In conclusion, this study showed, for the first time, that biallelic variants of SUZ12 caused Imagawa-Matsumoto syndrome, monoallelic variants in SETDIB resulted in OGID. Besides expanded the phenotypes of very rare OGID syndromes caused by FIBP and TMEM94.

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Bi-allelic TMEM94 Truncating Variants Are Associated with Neurodevelopmental Delay, Congenital Heart Defects, and Distinct Facial Dysmorphism

Cited by 18 publications

References 63 publications

A novel TBX5 mutation predisposes to familial cardiac septal defects and atrial fibrillation as well as bicuspid aortic valve

A novel TBX5 mutation predisposes to familial cardiac septal defects and atrial fibrillation as well as bicuspid aortic valve

Fetal Anomalies Associated with Novel Pathogenic Variants in TMEM94

An investigation of the etiology and follow‐up findings in 35 children with overgrowth syndromes, including biallelic SUZ12 variant

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