Rare variants found in multiplex families with orofacial clefts: Does expanding the phenotype make a difference?

Exome sequencing (ES) is now a relatively straightforward process to identify causal variants in Mendelian disorders. However, the same is not true for ES in families where the inheritance patterns are less clear, and a complex etiology is suspected. Orofacial clefts (OFCs) are highly heritable birt...

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Bibliographic Details
Published in:American journal of medical genetics. Part A 2023-10, Vol.191 (10), p.2558-2570
Main Authors: Diaz Perez, Kimberly K, Chung, Sydney, Head, S Taylor, Epstein, Michael P, Hecht, Jacqueline T, Wehby, George L, Weinberg, Seth M, Murray, Jeffrey C, Marazita, Mary L, Leslie, Elizabeth J
Format: Article
Language:English
Subjects:
Cleft Lip - genetics
Cleft Palate - genetics
Congenital defects
Etiology
Exome Sequencing
Genetic diversity
Genotype & phenotype
Heredity
Humans
Interferon Regulatory Factors - genetics
Orofacial clefts
Phenotype
Phenotypes
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Summary:Exome sequencing (ES) is now a relatively straightforward process to identify causal variants in Mendelian disorders. However, the same is not true for ES in families where the inheritance patterns are less clear, and a complex etiology is suspected. Orofacial clefts (OFCs) are highly heritable birth defects with both Mendelian and complex etiologies. The phenotypic spectrum of OFCs may include overt clefts and several subclinical phenotypes, such as discontinuities in the orbicularis oris muscle (OOM) in the upper lip, velopharyngeal insufficiency (VPI), microform clefts or bifid uvulas. We hypothesize that expanding the OFC phenotype to include these phenotypes can clarify inheritance patterns in multiplex families, making them appear more Mendelian. We performed exome sequencing to find rare, likely causal genetic variants in 31 multiplex OFC families, which included families with multiple individuals with OFCs and individuals with subclinical phenotypes. We identified likely causal variants in COL11A2, IRF6, SHROOM3, SMC3, TBX3, and TP63 in six families. Although we did not find clear evidence supporting the subclinical phenotype hypothesis, our findings support a role for rare variants in the etiology of OFCs.
ISSN:1552-4825
1552-4833
1552-4833
DOI:10.1002/ajmg.a.63336