2019
DOI: 10.1002/mgg3.959
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Rare single‐nucleotide variants in oculo‐auriculo‐vertebral spectrum (OAVS)

Abstract: BackgroundOculo‐auriculo‐vertebral spectrum (OAVS) is a craniofacial developmental disorder that affects structures derived from the first and second pharyngeal arches. The clinically heterogeneous phenotype involves mandibular, oral, and ear development anomalies. Etiology is complex and poorly understood. Genetic factors have been associated, evidenced by chromosomal abnormalities affecting different genomic regions and genes. However, known pathogenic single‐nucleotide variants (SNVs) have only been identif… Show more

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Cited by 10 publications
(22 citation statements)
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“…No clinical conditions have been associated with this variant thus far. None of the five patients presented rare SNVs or likely pathogenic or pathogenic CNVs previously studied (Bragagnolo et al, 2018; Zamariolli et al, 2019), reinforcing that this variant could play a role in the development of the disease in these patients. Although common features are observed between the five patients who carried this SNV, there is no consistency among them for many of the phenotypic characteristics observed (Table 2).…”
Section: Discussionmentioning
confidence: 56%
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“…No clinical conditions have been associated with this variant thus far. None of the five patients presented rare SNVs or likely pathogenic or pathogenic CNVs previously studied (Bragagnolo et al, 2018; Zamariolli et al, 2019), reinforcing that this variant could play a role in the development of the disease in these patients. Although common features are observed between the five patients who carried this SNV, there is no consistency among them for many of the phenotypic characteristics observed (Table 2).…”
Section: Discussionmentioning
confidence: 56%
“…Filtered SNVs were annotated using the WGSA annotation pipeline (v0.85; Liu et al, 2016) and functional relevance was ascertained based on prediction from in silico tools as described in Zamariolli et al (2019). Briefly, SNVs were considered likely deleterious when simultaneously predicted as deleterious by four queried algorithms for non‐synonymous variants (SIFT, Polyphen‐2, FATHMM‐XF, and Mutation Taster) and two algorithms for synonymous variants (FATHMM‐XF, and Mutation Taster).…”
Section: Methodsmentioning
confidence: 99%
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“…We then performed a literature-based gene prioritization: first, we screened our gene-associated deregulations by intersecting the gene lists with those confirmed or candidates to be causative of OAVS that emerged from both genetic (exome sequencing) or cytogenetic (SNP-array) studies. No epigenetic deregulations were found to be associated to MYT1 gene [ 22 , 23 ] or others proposed loci including ZYG11B [ 25 ], AMIGO2 [ 24 ], OTX2 / YPEL1 / CRKL [ 21 , 37 ], and NKX3-2 ( BAPX1 ) [ 29 ]. The only positive matching was found for the gene Xyloside Xylosyltransferase1 ( XXYLT1 ) localized in a region previously reported for a de novo microduplication on chromosome 3 (3q29) in an OAVS patient [ 38 ].…”
Section: Resultsmentioning
confidence: 99%
“…In addition, maternal allele variants of YPEL1 , when with incomplete penetration trait associated with genetic and/or environmental factors, could lead to OAVS phenotype. Clinical features have not been associated with neither MAPK1 nor YPEL1 (Zamariolli et al, 2019). Within the cases included in our review, both genes were always simultaneously deleted when cited (dos Santos et al, 2014; Spineli‐Silva et al, 2018; Xu et al, 2008).…”
Section: Discussionmentioning
confidence: 99%