Craniofacial studies in chicken embryos confirm the pathogenicity of human FZD2 variants associated with Robinow syndrome.

IF 4 3区 医学 Q2 CELL BIOLOGY Disease Models & Mechanisms Pub Date : 2024-06-01 Epub Date: 2024-07-05 DOI:10.1242/dmm.050584
Shruti S Tophkhane, Katherine Fu, Esther M Verheyen, Joy M Richman
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Abstract

Robinow syndrome is a rare disease caused by variants of seven WNT pathway genes. Craniofacial features include widening of the nasal bridge and jaw hypoplasia. We used the chicken embryo to test whether two missense human FZD2 variants (1301G>T, p.Gly434Val; 425C>T, p.Pro142Lys) were sufficient to change frontonasal mass development. In vivo, the overexpression of retroviruses with wild-type or variant human FZD2 inhibited upper beak ossification. In primary cultures, wild-type and variant human FZD2 significantly inhibited chondrogenesis, with the 425C>T variant significantly decreasing activity of a SOX9 luciferase reporter compared to that for the wild type or 1301G>T. Both variants also increased nuclear shuttling of β-catenin (CTNNB1) and increased the expression of TWIST1, which are inhibitory to chondrogenesis. In canonical WNT luciferase assays using frontonasal mass cells, the variants had dominant-negative effects on wild-type FZD2. In non-canonical assays, the 425C>T variant failed to activate the reporter above control levels and was unresponsive to exogenous WNT5A. This is the first single amino acid change to selectively alter ligand binding in a FZD receptor. Therefore, FZD2 missense variants are pathogenic and could lead to the altered craniofacial morphogenesis seen in Robinow syndrome.

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鸡胚胎颅面研究证实了与罗宾诺综合征相关的人类 FZD2 变体的致病性。
罗宾诺综合征是一种罕见疾病,由七个 WNT 通路基因变异引起。颅面特征包括鼻梁增宽和颌骨发育不良。我们利用鸡胚胎测试了两个错义人类 FZD2 变体(1301G>T,p.Gly434Val;425C>T,p.Pro142Lys)是否足以改变前鼻骨块的发育。在体内,野生型或变异型人类 FZD2 的逆转录病毒的过表达抑制了上喙骨化。在原代培养物中,野生型和变异型人FZD2显著抑制软骨形成,与野生型或1301G>T相比,425C>T变异型显著降低了SOX9荧光素酶报告物的活性。这两种变体还增加了β-catenin(CTNNB1)的核穿梭,并增加了TWIST1的表达,而这两种变体对软骨形成都有抑制作用。在使用前鼻质细胞进行的典型 WNT 荧光素酶试验中,变体对野生型 FZD2 具有显性负效应。在非规范性试验中,425C>T变体未能激活超过对照水平的报告物,并且对外源 WNT5A 无反应。这是第一个选择性改变 FZD 受体配体结合的单个氨基酸变化。因此,FZD2 错义变体具有致病性,可能导致罗宾诺综合征中出现的颅面形态发生改变。
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来源期刊
Disease Models & Mechanisms
Disease Models & Mechanisms 医学-病理学
CiteScore
6.60
自引率
7.00%
发文量
203
审稿时长
6-12 weeks
期刊介绍: Disease Models & Mechanisms (DMM) is an online Open Access journal focusing on the use of model systems to better understand, diagnose and treat human disease.
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