Three <i>GLI2</i> mutations combined potentially underlie non‐syndromic cleft lip with or without cleft palate in a Chinese pedigree

Meng, Peiqi; Zhao, Huaxiang; Huang, Wenbin; Zhang, Yunfan; Zhong, Wenjie; Zhang, Mengqi; Jia, Peizeng; Zhou, Zhibo; Maimaitili, Gulibaha; Chen, Feng; Zhang, Jieni; Jun, Lin

doi:10.1002/mgg3.714

Cited by 9 publications

(12 citation statements)

References 54 publications

(60 reference statements)

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“…The findings supported the role of CLPTM1(3), NECTIN1 (19), OFC1 (22), SPRY2 (23), THADA (24), SHTN1 (54), NOGGIN (27), TPM1 (30), GREM1 (31), PAX7 (34), SHH (36), SIX3 (37), BRIP1(BACH1) (38), BRCA1 (40), MAFB (26), FOXE1 (42), AXIN2 (43), SNAI1 (46), BRCA2 (40), GLI2 (48), GRHL3 (49), COL21A1 (50), WNT5A (51), TOX3 (52), and SOX9 (52) in the development of a CL ± P malformative phenotype. The findings also revealed that GAD1 (28), ARHGAP29 (39), and DVL2 (43) were regulatory proteins essential for proper development of the face.…”

Section: Genes Associated With Orofacial Closure Defectssupporting

confidence: 59%

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Orofacial Closure Defects: Forty-Five Genes Associated Cleft Lip and Palate

Ashouri¹,

Hamidreza

Ebadifar

2021

Precis Med Clin OMICS

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Context: Cleft lip and palate (CLP) is the most common congenital malformations in the face and neck. Given that the inheritance of this disease is multifactorial and both genetic and environmental factors play crucial roles in its creation, studying these factors may be a step toward reducing the prevalence of the disease in future generations. Method: For this study, we looked through several national and international databases, consisting of Scientific Information Database, IranDoc, ScienceDirect, Google Scholar, PubMed, and Scopus. Based on our search method, we found 800 published articles, of which 750 were obtained from the international databases, and the remaining 50 were extracted from the national databases. After data refining, 600 articles with eligible criteria remained for data extraction, and data related to embryological origin, classification and etiology, genes and environmental factors, and complications caused by CLP were collected. Results: The CLP etiology was multifactorial and involved both genetic and environmental risk factors. The primary purpose of this review was to give the reader an overview of studies on multifactorial causes of this congenital disability. The functions of genes are very different, indicating a high level of vulnerability in the cranial and facial growth pathways. Conclusions: These findings have advanced our understanding of genes associated with CLP and genetic polymorphisms involved in orofacial closure defects. The findings can create new clinical and molecular research opportunities.

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Section: Genes Associated With Orofacial Closure Defectssupporting

confidence: 59%

“…A study conducted on Gli2 in 2019 among Chinese people found the mutation c. 2684C > T_p. Ala895Val plays a role in the pathogenesis of NSCL/P (48).…”

Section: Genes Associated With Orofacial Closure Defectsmentioning

confidence: 99%

Orofacial Closure Defects: Forty-Five Genes Associated Cleft Lip and Palate

Ashouri¹,

Hamidreza

Ebadifar

2021

Precis Med Clin OMICS

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“…In our previous work involving identification of the genetic mutations underlying CL/P, 10 , 17 , 18 many variants were left after the traditional screening process, and a manual literature search was required to identify the candidate(s). In this study, we employed a web crawler strategy for the first time to narrow down the list of variants.…”

Section: Discussionmentioning

confidence: 99%

Identification of rare PTCH1 nonsense variant causing orofacial cleft in a Chinese family and an up-to-date genotype-phenotype analysis

et al. 2021

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The Patched 1 ( PTCH1 ) gene encodes a membrane receptor involved in the Hedgehog (Hh) signaling pathway, an abnormal state of which may result in congenital defects or human tumors. In this study, we conducted whole-exome sequencing on a three-generation Chinese family characterized with variable penetrance of orofacial clefts. A rare heterozygous variant in the PTCH1 gene (c.2833C > T p.R945X) was identified as a disease-associated mutation. Structural modeling revealed a truncation starting from the middle of the second extracellular domain of PTCH1 protein. This may damage its ligand recognition and sterol transportation abilities, thereby affecting the Hh signaling pathway. Biochemical assays indicated that the R945X protein had reduced stability compared to the wild-type in vitro . In addition, we reviewed the locations and mutation types of PTCH1 variants in individuals with clefting phenotypes, and analyzed the associations between clefts and locations or types of variants within PTCH1 . Our findings provide further evidence that PTCH1 variants result in orofacial clefts, and contributed to genetic counseling and clinical surveillance in this family.

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“…We reviewed the literature for comprehensive phenotypic descriptions of individuals with confirmed pathogenic (a) intragenic GLI2 variants and (b) chromosome 2q14.2 deletions encompassing only GLI2 . We re‐evaluated the pathogenicity of previously published GLI2 missense variants (Table 2) (Arnhold et al, 2015; Babu et al, 2019; Bear et al, 2014; Bertolacini et al, 2012; Brauner et al, 2020; Flemming et al, 2013; França et al, 2013; Gregory et al, 2015; Juanes et al, 2016; Meng et al, 2019; Rahimov et al, 2006; Vaaralahti et al, 2012; Vishnopolska et al, 2021). This re‐evaluation was primarily based on population variant frequency in the gnomAD database (Karczewski et al, 2020).…”

Section: Clinical Reportmentioning

confidence: 99%

Truncating and zinc‐finger variants in GLI2 are associated with hypopituitarism

Corder

Berland

Førsvoll

et al. 2021

American J of Med Genetics Pt A

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Variants in transcription factor GLI2 have been associated with hypopituitarism and structural brain abnormalities, occasionally including holoprosencephaly (HPE). Substantial phenotypic variability and nonpenetrance have been described, posing difficulties in the counseling of affected families. We present three individuals with novel likely pathogenic GLI2 variants, two with truncating and one with a de novo missense variant p.(Ser548Leu), and review the literature for comprehensive phenotypic descriptions of individuals with confirmed pathogenic (a) intragenic GLI2 variants and (b) chromosome 2q14.2 deletions encompassing only GLI2. We show that most of the 31 missense variants previously reported as pathogenic are likely benign or, at most, low‐risk variants. Four Zn‐finger variants: p.(Arg479Gly), p.(Arg516Pro), p.(Gly518Lys), and p.(Tyr575His) were classified as likely pathogenic, and three other variants as possibly pathogenic: p.(Pro253Ser), p.(Ala593Val), and p.(Pro1243Leu). We analyze the phenotypic descriptions of 60 individuals with pathogenic GLI2 variants and evidence a morbidity spectrum that includes hypopituitarism (58%), HPE (6%) or other brain structure abnormalities (15%), orofacial clefting (17%) and dysmorphic facial features (35%). We establish that truncating and Zn‐finger variants in GLI2 are associated with a high risk of hypopituitarism, and that a solitary median maxillary central incisor is part of the GLI2‐related phenotypic variability. The most prevalent phenotypic feature is post‐axial polydactyly (65%) which is also the mildest phenotypic expression of the condition, reported in many parents of individuals with systemic findings. Our approach clarifies clinical risks and the important messages to discuss in counseling for a pathogenic GLI2 variant.

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Three GLI2 mutations combined potentially underlie non‐syndromic cleft lip with or without cleft palate in a Chinese pedigree

Cited by 9 publications

References 54 publications

Orofacial Closure Defects: Forty-Five Genes Associated Cleft Lip and Palate

Orofacial Closure Defects: Forty-Five Genes Associated Cleft Lip and Palate

Identification of rare PTCH1 nonsense variant causing orofacial cleft in a Chinese family and an up-to-date genotype-phenotype analysis

Truncating and zinc‐finger variants in GLI2 are associated with hypopituitarism

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