Whole-Exome Sequencing of Discordant Monozygotic Twin Families for Identification of Candidate Genes for Microtia-Atresia

Background: Microtia is a congenital malformation of the outer ears caused by improper embryonic development. The origin of microtia and causes of its variations remain unknown. Because of the lack of clarity regarding the role of genetic variables in microtia, we conducted a systematic review to qualitatively identify the genes most important in the development of microtia to provide an up-to-date review. Methods: Using six search engines, we searched all published studies related to the genetic factors of isolated microtia and syndromic microtia. The identified publications were screened and selected based on inclusion and exclusion criteria by the authors and assessed for methodological quality using the Joanna Briggs Institute (JBI) critical appraisal tools. We found 40 studies, including 22 studies on syndromic microtia and 18 studies on isolated microtia. Data extraction of each study was arranged in tabulation for syndromic and isolated microtia. The extracted data were: first author’s surname, year of publication, country of origin, study design, sample characteristic and gene assessed. Results: After the data were extracted, analyzed, and reviewed, the most common gene suspected to be involved in isolated microtia was Homeobox A2 (HOXA2, 12.1%). Conversely, in syndromic microtia, the two most common genes supposed to play a role were Fibroblast Growth Factor 3 (FGF3, 47.2%) and Treacher–Collins–Franceschetti syndrome 1 (TCOF1, 30.2%). From the studies, the three most prevalent genes associated with microtia were HOXA2 (10%), FGF3 (8.4%), and TCOF1 (5.4%). In syndromic microtia, the most common mutation types were deletion in TCOF1 (46.9%) and missense and deletion in FGF3 (both 38%), and in isolated microtia, the most common mutation type was silent in HOXA2 (54.2%). Conclusions: In summary, genetic factors are involved in microtia; thus, molecular analysis is strongly advised. PROSPERO registration: CRD42021287294 (25/10/21).

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“…Characteristics of the studies of isolated microtia.1,9,17,22,41,46,[48][49][50][65][66][67][68][69][70][71][72]132,133 …”

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confidence: 99%

The role of genetic factors in microtia: A systematic review

Putri

Stephanie²,

Pramanasari³

et al. 2022

F1000Res

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“…These findings may be, at least partially, related to the limitations of genome wide SNP array [25] which may not detect very small deletions/duplications, balanced rearrangements or small/single nucleotide variants. Recent studies using whole exome sequencing (WES) in cases of isolated microtia yielded promising results [24,26]. During WES, the entire exome is analyzed to investigate for variants in the coding part of the human genome (the exomes) that could explain the development of CAA/microtia.…”

Section: Discussionmentioning

confidence: 99%

“…During WES, the entire exome is analyzed to investigate for variants in the coding part of the human genome (the exomes) that could explain the development of CAA/microtia. Data obtained by WES in discordant monozygotic twins with a consistent clinical phenotype (unilateral type 3 microtia and CAA) revealed HOXA4 as a likely pathogenetic variant for microtia-atresia [26]. Soon, we aim to perform WES in a large group of microtia/CAA patients with a similar phenotype.…”

Section: Discussionmentioning

confidence: 99%

Search for a genetic cause in children with unilateral isolated microtia and congenital aural atresia

Mortier

Ende

Declau

et al. 2022

Eur Arch Otorhinolaryngol

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PurposeMicrotia describes a spectrum of auricular malformations ranging from mild dysplasia to anotia. A vast majority of microtia patients demonstrate congenital aural atresia (CAA). Isolated microtia has a right ear predominance (58 -61%) and is more common in the male sex. Isolated microtia is a multifactorial condition involving genetic and environmental causes. The aim of this study is to perform describe the HIGHLIGHTS  Type III microtia (peanut-shell type) of the auricle and type 2b CAA were the most common occurring phenotype of unilateral isolated microtia. Crosstabulation of the Weerda and HEAR classification suggests an association between the classification of the visible auricular deformities (Weerda) and the anatomical status (HEAR). Genome wide microarray analysis did not reveal any pathological copy number variant (CNV) that could explain the phenotype.

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“…Except for mosaicism in other than blood cells, one may suspect the presence of additional modifiers of the phenotype, including epigenetic factors [ 18 – 20 ]. To check whether the variable severity of CFNS in both twin females resulted from skewed X chromosome inactivation, we performed XCI testing.…”

Section: Discussionmentioning

confidence: 99%

Clinical and molecular characterization of craniofrontonasal syndrome: new symptoms and novel pathogenic variants in the EFNB1 gene

Bukowska‐Olech

Gawliński²,

Jakubiuk‐Tomaszuk

et al. 2021

Orphanet J Rare Dis

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Background Craniofrontonasal syndrome (CFNS) is a rare X-linked disorder that results from pathogenic variants in the EFNB1 gene. The syndrome paradoxically presents with greater severity of the symptoms in heterozygous females than hemizygous males. Results We have recruited and screened a female cohort affected with CFNS. Our primary finding was the description of monozygotic twins, i.e., patients 5 and 6, discordant for the CFNS phenotype. Intriguingly, patient 5 presented classical CFNS gestalt, whereas patient 6 manifested only very subtle craniofacial features, not resembling CFNS. Besides, we have expanded the mutational spectrum of the EFNB1 gene through reporting four novel pathogenic variants—p.(Trp12*), p.(Cys64Phe), p.(Tyr73Metfs*86), p.(Glu210*). All those alterations were found applying either targeted NGS of a custom gene panel or PCR followed by Sanger sequencing and evaluated using in silico predictors. Lastly, we have also expanded the CFNS phenotypic spectrum by describing in patient 3 several novel features of the syndrome, such as bifid hallux, bicornuate uterus, and abnormal right ovary segmented into six parts. Conclusions We have described the unreported so far differences of the clinical phenotype in the monozygotic twin patients 5 and 6 harboring an identical p.(Glu210*) variant located in the EFNB1 gene. With our finding, we have pointed to an unusual phenomenon of mildly affected females with CFNS, who may not manifest features suggestive of the syndrome. Consequently, this study may be valuable for geneticists consulting patients with craniofacial disorders.

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Whole-Exome Sequencing of Discordant Monozygotic Twin Families for Identification of Candidate Genes for Microtia-Atresia

Cited by 11 publications

References 38 publications

The role of genetic factors in microtia: A systematic review

The role of genetic factors in microtia: A systematic review

Search for a genetic cause in children with unilateral isolated microtia and congenital aural atresia

Clinical and molecular characterization of craniofrontonasal syndrome: new symptoms and novel pathogenic variants in the EFNB1 gene

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