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Abstract

Background:

Frontonasal dysplasia (FND) is a rare developmental disorder characterized by mild to severe changes in skull and brain structures. It is a phenotypically variable and heterogeneous disorder. This study was designed to provide a clinical and genetic analysis of FND in a consanguineous family of Pakistani origin.

Methodology and Results:

Affected individuals in the family showed characteristic features of frontonasal dysplasia type-2 (FND2), such as nasal bone hypoplasia, hypertelorism, and alopecia. Skull and brain imaging of affected members revealed ossification defects and various types of brain structural anomalies that created a split-brain. Sanger sequencing of the ALX4 gene revealed a homozygous missense variant [NM_021926.4: c.652C>T; p.(Arg218Trp)] in three affected members who demonstrated severe craniofacial anomalies. Heterozygous carriers in the family showed mild FND2 phenotypes.

Conclusion:

Clinical and genetic analysis of a family, exhibiting FND2 phenotypes, revealed several previously unreported clinical features and a novel missense variant in the ALX4 gene. These results will facilitate diagnosis and genetic counseling of the FND patients in the Pakistani population.

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References

Adzhubei

, Schmidt

, Peshkin

, et al. (2010) A method and server for predicting damaging missense mutations. Nat Methods, 7:248.

Altunoglu

, Satkın

, Uyguner

, et al. (2014) Mild nasal clefting may be predictive for ALX4 heterozygotes. Am J Med Genet A, 164:2054-2058.

Attanasio

, Nord

, Zhu

, et al. (2013) Fine tuning of craniofacial morphology by distant-acting enhancers. Science, 342:1241006.

Bertola

, Rodrigues

, Quaio

, et al. (2013) Vertical transmission of a frontonasal phenotype caused by a novel ALX4 mutation. Am J Med Genet A, 161:600-604.

Brunskill

, Potter

, Distasio

, et al. (2014) A gene expression atlas of early craniofacial development. Dev Biol, 391:133-146.

El-Ruby

, El-Din Fayez

, El-Dessouky

, et al. (2018) Identification of a novel homozygous ALX4 mutation in two unrelated patients with frontonasal dysplasia type-2. Am J Med Genet Part A, 176:1190-1194.

Joshi

, Chang

, Hamel

. (2006) Loss of Alx4, a stromally-restricted homeodomain protein, impairs mammary epithelial morphogenesis. Dev Biol, 297:284-294.

Kariminejad

, Bozorgmehr

, Alizadeh

, et al. (2014) Skull defects, alopecia, hypertelorism, and notched alae nasi caused by homozygous ALX4 gene mutation. Am J Med Genet A, 164:1322-1327.

Kayserili

, Altunoglu

, Ozgur

, et al. (2012) Mild nasal malformations and parietal foramina caused by homozygous ALX4 mutations. Am J Med Genet A, 158:236-244.

10.

Kosugi

, Hasebe

, Matsumura

, et al. (2009) Six classes of nuclear localization signals specific to different binding grooves of importin α. J Biol Chem, 284:478-485

11.

Pettersen

, Goddard

, Huang

, et al. 2004) UCSF Chimera—a visualization system for exploratory research and analysis. J Comput Chem, 25:1605-1612.

12.

, Niswender

, Ji

, et al. (1997) Polydactyly and ectopic ZPA formation in Alx-4 mutant mice. Development, 124:3999-4008.

13.

Ribeiro

, Quiezi

, Nascimento

, et al. (2010) Holoprosencephaly and holoprosencephaly-like phenotype and GAS1 DNA sequence changes: report of four Brazilian patients. Am J Med Genet Part A, 152:1688-1694.

14.

Rice

, Rice

, Olsen

, et al. (2003) Progression of calvarial bone development requires Foxc1 regulation of Msx2 and Alx4. Dev Biol, 262:75-87.

15.

Rodrigues

, Myung

, Pires

, et al. (2019) mCSM-PPI2: predicting the effects of mutations on protein-protein interactions. Nucleic Acids Res, 47:W338-W344.

16.

Roy

, Kucukural

, Zhang

. (2010) I-TASSER: a unified platform for automated protein structure and function prediction. Nat Protoc, 5:725-738.

17.

Schwarz

, Cooper

, Schuelke

, et al. (2014) MutationTaster2: mutation prediction for the deep-sequencing age. Nat Methods, 11:361.

18.

Sim

, Kumar

, Hu

, et al. (2012) SIFT web server: predicting effects of amino acid substitutions on proteins. Nucleic Acids Res, 40:W452-W457.

19.

Takahashi

, Tamura

, Buscher

, et al. (1998) The role of Alx-4 in the establishment of anteroposterior polarity during vertebrate limb development. Development, 125:4417-4425.

20.

Tucker

, Wisdom

. (1999) Site-specific heterodimerization by paired class homeodomain proteins mediates selective transcriptional responses. J Biol Chem, 274:32325-32332.

21.

Twigg

, Versnel

, Nürnberg

, et al. (2009) Frontorhiny, a distinctive presentation of frontonasal dysplasia caused by recessive mutations in the ALX3 homeobox gene. Am J Hum Genet, 84:698-705.

22.

Ullah

, Kalsoom

, Umair

, et al. (2017) Exome sequencing revealed a novel splice site variant in the ALX1 gene underlying frontonasal dysplasia. Clin Genet, 91:494-498.

23.

, Alanay

, Aktas

, et al. (2010) Disruption of ALX1 causes extreme microphthalmia and severe facial clefting: expanding the spectrum of autosomal-recessive ALX-related frontonasal dysplasia. Am J Hum Genet, 86:789-796.

24.

Waterhouse

, Bertoni

, Bienert

, et al. (2018) SWISS-MODEL: homology modelling of protein structures and complexes. Nucleic Acids Res, 46:W296-W303.

25.

Yan

, Zhang

, Zhou

, et al. (2017) HDOCK: a web server for protein-protein and protein-DNA/RNA docking based on a hybrid strategy. Nucleic Acids Res, 45:W365-W373.

26.

Yasuhara

, Shibazaki

, Tanaka

, et al. (2007) Triggering neural differentiation of ES cells by subtype switching of importin-α. Nat Cell Biol, 9:72.

27.

, Lin

, Tartakoff

, et al. (2011) Karyopherins in nuclear transport of homeodomain proteins during development. Biochim Biophys Acta, 1813:1654-1662.

28.

Zucchelli

, Ferrari

, Blasi

, et al. (2017) New insights into cooperative binding of homeodomain transcription factors PREP1 and PBX1 to DNA. Sci Rep, 7:40665.

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A Novel Missense Variant in the ALX4 Gene Underlies Mild to Severe Frontonasal Dysplasia in a Consanguineous Family