Bi-allelic variants in<i>WNT7B</i>disrupt the development of multiple organs in humans

Bouasker, Samir; Patel, Nisha; Greenlees, Rebecca; Wellesley, Diana; Taie, Lucas Fares; Almontashiri, Naif A M; Baptista, Júlia; Alghamdi, Malak; Boissel, Sarah; Martinovic, Jéléna; Prokudin, Ivan; Holden, Samantha; Mudhar, Hardeep-Singh; Riley, Lisa G.; Nassif, Christina; Attié‐Bitach, Tania; Miguet, Marguerite; Delous, Marion; Ernest, Sylvain; Plaisancié, Julie; Calvas, Patrick; Rozet, Jean–Michel; Khan, Arif O.; Hamdan, Fadi F.; Jamieson, Robyn V; Alkuraya, Fowzan S.; Michaud, Jacques L.; Chassaing, Nicolas

doi:10.1136/jmedgenet-2022-108475

Cited by 3 publications

(8 citation statements)

References 29 publications

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“…17,20,21 It is worth mentioning that we have previously shown that this role seems to be conserved in zebrafish where wnt7bb mutants display abnormal development of the swimbladder, the lung equivalent in zebrafish. 4 Abnormal tracheal development is another PDAC phenotype that is recapitulated in mice with WNT7B deficiency, which display incomplete cartilaginous rings. 21 Macrophage-induced apoptosis mediated by Wnt7b has been proposed as the mechanism for why Wnt7b deficient mice display pulmonary vascular defects and persistence of the hyaloid artery in the developing eye.…”

Section: Discussionmentioning

confidence: 99%

“…Besides the compelling human genetics data, WNT7B was an attractive candidate biologically. Indeed, we have shown that wnt7bb mutant zebrafish recapitulated a key phenotypic aspect of PDAC syndrome, that is, malformed swimbladder, the equivalent of lung hypoplasia in humans 4 . However, this association is not yet listed in OMIM pending independent confirmation and the current classification of the link between WNT7B and PDAC syndrome remains “Moderate” according to the ClinGen guidelines 5 .…”

Section: Introductionmentioning

confidence: 97%

“…Recently, we reported three families in which biallelic missense and nonsense variants in WNT7B were associated with a PDAC spectrum. 4 Besides the compelling human genetics data, WNT7B was an attractive candidate biologically. Indeed, we have shown that wnt7bb mutant zebrafish recapitulated a key phenotypic aspect of PDAC syndrome, that is, malformed swimbladder, the equivalent of lung hypoplasia in humans.…”

Section: Introductionmentioning

confidence: 99%

“…Indeed, we have shown that wnt7bb mutant zebrafish recapitulated a key phenotypic aspect of PDAC syndrome, that is, malformed swimbladder, the equivalent of lung hypoplasia in humans. 4 However, this association is not yet listed in OMIM pending independent confirmation and the current classification of the link between WNT7B and PDAC syndrome remains "Moderate" according to the ClinGen guidelines. 5 Here, we describe two new families that share a founder missense variant in WNT7B with a deleterious impact on WNT7B signaling.…”

Section: Introductionmentioning

confidence: 99%

“…Recently, we reported three families in which biallelic missense and nonsense variants in WNT7B were associated with a PDAC spectrum 4 . Besides the compelling human genetics data, WNT7B was an attractive candidate biologically.…”

Section: Introductionmentioning

confidence: 99%

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A founder variant expands the phenotype of WNT7B‐related PDAC syndrome

AlAbdi,

Rahbeeni,

Maddirevula

et al. 2024

Clinical Genetics

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Pulmonary hypoplasia, Diaphragmatic anomalies, Anophthalmia/microphthalmia, and Cardiac defects (PDAC) syndrome is a genetically heterogeneous multiple congenital malformation syndrome. Although pathogenic variants in RARB and STRA6 are established causes of PDAC, many PDAC cases remain unsolved at the molecular level. Recently, we proposed biallelic WNT7B variants as a novel etiology based on several families with typical features of PDAC syndrome albeit with variable expressivity. Here, we report three patients from two families that share a novel founder variant in WNT7B (c.739C > T; Arg247Trp). The phenotypic expression of this variant ranges from typical PDAC features to isolated genitourinary anomalies. Similar to previously reported PDAC‐associated WNT7B variants, this variant was found to significantly impair WNT7B signaling activity further corroborating its proposed pathogenicity. This report adds further evidence to WNT7B‐related PDAC and expands its variable expressivity.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 97%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

A founder variant expands the phenotype of WNT7B‐related PDAC syndrome

AlAbdi,

Rahbeeni,

Maddirevula

et al. 2024

Clinical Genetics

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LncRNA H19-EZH2 interaction promotes liver fibrosis via reprogramming H3K27me3 profiles

Zhou

Xue

et al. 2023

Acta Pharmacol Sin

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Clinical, genetic and biochemical signatures ofRBP4-related ocular malformations

Plaisancié¹,

Martinovic

Chesneau

et al. 2023

J Med Genet

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BackgroundThe retinoic acid (RA) pathway plays a crucial role in both eye morphogenesis and the visual cycle. Individuals with monoallelic and biallelic pathogenic variants inretinol-binding protein 4(RBP4), encoding a serum retinol-specific transporter, display variable ocular phenotypes. Although few families have been reported worldwide, recessive inherited variants appear to be associated with retinal degeneration, while individuals with dominantly inherited variants manifest ocular development anomalies, mainly microphthalmia, anophthalmia and coloboma (MAC).MethodsWe report here seven new families (13 patients) with isolated and syndromic MAC harbouring heterozygousRBP4variants, of whom we performed biochemical analyses.ResultsFor the first time, malformations that overlap the clinical spectrum of vitamin A deficiency are reported, providing a link with other RA disorders. Our data support two distinct phenotypes, depending on the nature and mode of inheritance of the variants: dominantly inherited, almost exclusively missense, associated with ocular malformations, in contrast to recessive, mainly truncating, associated with retinal degeneration. Moreover, we also confirm the skewed inheritance and impact of maternalRBP4genotypes on phenotypical expression in dominant forms, suggesting that maternalRBP4genetic status and content of diet during pregnancy may modify MAC occurrence and severity. Furthermore, we demonstrate that retinol-binding protein blood dosage in patients could provide a biological signature crucial for classifyingRBP4variants. Finally, we propose a novel hypothesis to explain the mechanisms underlying the observed genotype–phenotype correlations inRBP4mutational spectrum.ConclusionDominant missense variants inRBP4are associated with MAC of incomplete penetrance with maternal inheritance through a likely dominant-negative mechanism.

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Bi-allelic variants inWNT7Bdisrupt the development of multiple organs in humans

Cited by 3 publications

References 29 publications

A founder variant expands the phenotype of WNT7B‐related PDAC syndrome

A founder variant expands the phenotype of WNT7B‐related PDAC syndrome

LncRNA H19-EZH2 interaction promotes liver fibrosis via reprogramming H3K27me3 profiles

Clinical, genetic and biochemical signatures ofRBP4-related ocular malformations

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