foxe1 mutant zebrafish show indications of a hypothyroid phenotype and increased sensitivity to ethanol for craniofacial malformations.

IF 2 3区 生物学 Q2 ANATOMY & MORPHOLOGY Developmental Dynamics Pub Date : 2024-10-03 DOI:10.1002/dvdy.745
Sophie T Raterman, Frank A D T G Wagener, Jan Zethof, Vincent Cuijpers, Peter H M Klaren, Juriaan R Metz, Johannes W Von den Hoff
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Abstract

Background: FOXE1 mutations in humans are associated with cleft palate and hypothyroidism. We previously developed a foxe1 mutant zebrafish demonstrating mineralization defects in larvae. In the present study, we investigate the thyroid status and skeletal phenotype of adult foxe1 mutants.

Results: Mutant fish have increased expression of tshβ in the pituitary, and of hepatic dio1 and dio2. In plasma, we found higher Mg levels. Together these findings are indicative of hypothyroidism. We further observed mineralization defects in scales due to enhanced osteoclast activity as measured by increased expression levels of tracp, ctsk, and rankl. Gene-environment interactions in the etiology of FOXE1-related craniofacial abnormalities remain elusive, which prompts the need for models to investigate genotype-phenotype associations. We here investigated whether ethanol exposure increases the risk of developing craniofacial malformations in foxe1 mutant larvae that we compared to wild types. We found in ethanol-exposed mutants an increased incidence of developmental malformations and marked changes in gene expression patterns of cartilage markers (sox9a), apoptotic markers (casp3b), retinoic acid metabolism (cyp26c1), and tissue hypoxia markers (hifaa, hifab).

Conclusion: Taken together, this study shows that the foxe1 mutant zebrafish recapitulates phenotypes associated with FOXE1 mutations in human patients and a clear foxe1-ethanol interaction.

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foxe1 突变体斑马鱼表现出甲状腺功能减退的表型,对乙醇的敏感性增加,导致颅面畸形。
背景人类的 FOXE1 基因突变与腭裂和甲状腺功能减退症有关。我们之前培育了一种 foxe1 突变体斑马鱼,它在幼体中表现出矿化缺陷。在本研究中,我们调查了成年 foxe1 突变体的甲状腺状态和骨骼表型:结果:突变体鱼垂体中tshβ以及肝脏中dio1和dio2的表达量增加。在血浆中,我们发现镁含量较高。这些发现共同表明甲状腺机能减退。我们进一步观察到,由于破骨细胞活性的增强,鳞片中的矿化缺陷通过tracp、tsk和rankl表达水平的升高来衡量。在与 FOXE1 相关的颅面异常的病因学中,基因与环境之间的相互作用仍然难以捉摸,这促使我们需要建立模型来研究基因型与表型之间的关联。我们在此研究了乙醇暴露是否会增加 foxe1 突变体幼虫颅面畸形的风险,并与野生型幼虫进行了比较。我们发现,在暴露于乙醇的突变体中,发育畸形的发生率增加,软骨标志物(sox9a)、细胞凋亡标志物(casp3b)、维甲酸代谢(cyp26c1)和组织缺氧标志物(hifaa、hifab)的基因表达模式也发生了明显变化:综上所述,本研究表明 foxe1 突变体斑马鱼再现了与人类患者 FOXE1 突变相关的表型,以及 foxe1 与乙醇之间明确的相互作用。
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来源期刊
Developmental Dynamics
Developmental Dynamics 生物-发育生物学
CiteScore
5.10
自引率
8.00%
发文量
116
审稿时长
3-8 weeks
期刊介绍: Developmental Dynamics, is an official publication of the American Association for Anatomy. This peer reviewed journal provides an international forum for publishing novel discoveries, using any model system, that advances our understanding of development, morphology, form and function, evolution, disease, stem cells, repair and regeneration.
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