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A distal 594 bp ECR specifies Hmx1 expression in pinna and lateral facial morphogenesis and is regulated by the Hox-Pbx-Meis complex

机译:远端594 bp ECR指示耳廓和侧面面部形态发生中的Hmx1表达并受Hox-Pbx-Meis复合体调控

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摘要

Hmx1 encodes a homeodomain transcription factor expressed in the developing lateral craniofacial mesenchyme, retina and sensory ganglia. Mutation or mis-regulation of Hmx1 underlies malformations of the eye and external ear in multiple species. Deletion or insertional duplication of an evolutionarily conserved region (ECR) downstream of Hmx1 has recently been described in rat and cow, respectively. Here, we demonstrate that the impact of Hmx1 loss is greater than previously appreciated, with a variety of lateral cranioskeletal defects, auriculofacial nerve deficits, and duplication of the caudal region of the external ear. Using a transgenic approach, we demonstrate that a 594 bp sequence encompassing the ECR recapitulates specific aspects of the endogenous Hmx1 lateral facial expression pattern. Moreover, we show that Hoxa2, Meis and Pbx proteins act cooperatively on the ECR, via a core 32 bp sequence, to regulate Hmx1 expression. These studies highlight the conserved role for Hmx1 in BA2-derived tissues and provide an entry point for improved understanding of the causes of the frequent lateral facial birth defects in humans.
机译:Hmx1编码在发育中的外侧颅面间充质,视网膜和感觉神经节中表达的同源域转录因子。 Hmx1的突变或失调是多种物种的眼睛和外耳畸形的基础。 Hmx1下游的进化保守区(ECR)的删除或插入重复最近已分别在大鼠和牛中进行了描述。在这里,我们证明了Hmx1丢失的影响大于以前的认识,并伴有各种外侧颅骨骨骼缺损,耳面神经缺损以及外耳尾区重复。使用转基因方法,我们证明了包含ECR的594 bp序列概括了内源性Hmx1侧面面部表情模式的特定方面。此外,我们显示Hoxa2,Meis和Pbx蛋白通过核心32 bp序列协同作用于ECR,以调节Hmx1表达。这些研究突显了Hmx1在BA2来源的组织中的保守作用,并为更好地理解人类常见的面部侧面出生缺陷的原因提供了切入点。

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