Disruption of hedgehog signaling leads to hyoid bone dysplasia during embryogenesis

IF 2.2 3区生物学 Q4 CELL BIOLOGY Differentiation Pub Date : 2023-05-01 DOI:10.1016/j.diff.2023.05.001

Yan Guo , Xingyu Chen , Yongzhen Lai , Meng Lu , Chengyong Wang , Yun Shi , Chengyan Ren , Weihui Chen

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Abstract

The development of the hyoid bone is a complex process that involves the coordination of multiple signaling pathways. Previous studies have demonstrated that disruption of the hedgehog pathway in mice results in a series of structural malformations. However, the specific role and critical period of the hedgehog pathway in the early development of the hyoid bone have not been thoroughly characterized. In this study, we treated pregnant ICR mice with the hedgehog pathway inhibitor vismodegib by oral gavage in order to establish a model of hyoid bone dysplasia. Our results indicate that administration of vismodegib at embryonic days 11.5 (E11.5) and E12.5 resulted in the development of hyoid bone dysplasia. We were able to define the critical periods for the induction of hyoid bone deformity through the use of a meticulous temporal resolution. Our findings suggest that the hedgehog pathway plays a crucial role in the early development of the hyoid bone. Additionally, our research has established a novel and easily established mouse model of synostosis in the hyoid bone using a commercially available pathway-selective inhibitor.

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在胚胎发生过程中，刺猬信号的破坏导致舌骨发育不良

舌骨的发育是一个复杂的过程，涉及多种信号通路的协调。先前的研究表明，小鼠体内刺猬通路的破坏会导致一系列结构畸形。然而，刺猬通路在舌骨早期发育中的具体作用和关键时期尚未完全确定。在本研究中，我们用hedgehog通路抑制剂vismodegib灌胃治疗怀孕的ICR小鼠，以建立舌骨发育不良模型。我们的研究结果表明，在胚胎第11.5天（E11.5）和E12.5天施用vismodegib会导致舌骨发育不良。我们能够通过使用精细的时间分辨率来确定诱导舌骨畸形的关键时期。我们的研究结果表明，刺猬通路在舌骨的早期发育中起着至关重要的作用。此外，我们的研究使用市售的途径选择性抑制剂建立了一种新的、易于建立的舌骨滑膜粘连小鼠模型。

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来源期刊

Differentiation 生物-发育生物学

CiteScore

4.10

自引率

3.40%

发文量

审稿时长

51 days

期刊介绍： Differentiation is a multidisciplinary journal dealing with topics relating to cell differentiation, development, cellular structure and function, and cancer. Differentiation of eukaryotes at the molecular level and the use of transgenic and targeted mutagenesis approaches to problems of differentiation are of particular interest to the journal. The journal will publish full-length articles containing original work in any of these areas. We will also publish reviews and commentaries on topics of current interest. The principal subject areas the journal covers are: • embryonic patterning and organogenesis • human development and congenital malformation • mechanisms of cell lineage commitment • tissue homeostasis and oncogenic transformation • establishment of cellular polarity • stem cell differentiation • cell reprogramming mechanisms • stability of the differentiated state • cell and tissue interactions in vivo and in vitro • signal transduction pathways in development and differentiation • carcinogenesis and cancer • mechanisms involved in cell growth and division especially relating to cancer • differentiation in regeneration and ageing • therapeutic applications of differentiation processes.

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