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RA 诱导的突起特异性反应导致 Wnt 和骨生成的独特调节。

RA-induced prominence-specific response resulted in distinctive regulation of Wnt and osteogenesis.

机构信息

The Key Laboratory of Virology of Guangzhou, Jinan University, Guangzhou, China.

First Affiliated Hospital, Jinan University, Guangzhou, China.

出版信息

Life Sci Alliance. 2023 Aug 4;6(10). doi: 10.26508/lsa.202302013. Print 2023 Oct.

Abstract

Proper retinoic acid (RA) signaling is essential for normal craniofacial development. Both excessive RA and RA deficiency in early embryonic stage may lead to a variety of craniofacial malformations, for example, cleft palate, which have been investigated extensively. Dysregulated Wnt and Shh signaling were shown to underlie the pathogenesis of RA-induced craniofacial defects. In our present study, we showed a spatiotemporal-specific effect of RA signaling in regulating early development of facial prominences. Although inhibited Wnt activities was observed in E12.5/E13.5 mouse palatal shelves, early exposure of excessive RA induced Wnt signaling and Wnt-related gene expression in E11.5/E12.5 mouse embryonic frontonasal/maxillary processes. A conserved regulatory network of - was identified to play critical roles in RA-regulated craniofacial development using RNA-seq. In addition, subsequent osteogenic/chondrogenic differentiation were differentially regulated in discrete mouse embryonic facial prominences in response to early RA induction, demonstrated using both in vitro and in vivo analyses.

摘要

适当的维甲酸 (RA) 信号对于正常的颅面发育是必不可少的。早期胚胎阶段过多的 RA 和 RA 缺乏都可能导致各种颅面畸形,例如腭裂,已经进行了广泛的研究。失调的 Wnt 和 Shh 信号被证明是 RA 诱导的颅面缺陷发病机制的基础。在本研究中,我们显示 RA 信号在调节面部突起早期发育中的时空特异性作用。尽管在 E12.5/E13.5 鼠腭板中观察到 Wnt 活性受到抑制,但早期过量 RA 诱导在 E11.5/E12.5 鼠胚胎额鼻/上颌突起中 Wnt 信号和 Wnt 相关基因表达。使用 RNA-seq 鉴定了保守的调控网络 - 在 RA 调节颅面发育中发挥关键作用。此外,通过体外和体内分析表明,早期 RA 诱导后,离散的鼠胚胎面部突起中的后续成骨/软骨分化受到不同调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4a49/10403638/4338e9516f46/LSA-2023-02013_Fig1.jpg

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