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Cranial muscle defects of Pitx2 mutants result from specification defects in the first branchial arch

机译:Pitx2突变体的颅肌缺陷是由第一个branch弓中的规范缺陷引起的

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摘要

Pitx2 expression is observed during all states of the myogenic progression in embryonic muscle anlagen and persists in adult muscle. Pitx2 mutant mice form all but a few muscle anlagen. Loss or degeneration in muscle anlagen could generally be attributed to the loss of a muscle attachment site induced by some other aspect of the Pitx2 phenotype. Muscles derived from the first branchial arch were absent, whereas muscles derived from the second branchial arch were merely distorted in Pitx2 mutants at midgestation. Pitx2 was expressed well before, and was required for, initiation of the myogenic progression in the first, but not second, branchial arch mesoderm. Pitx2 was also required for expression of premyoblast specification markers Tbx1, Tcf21, and Msc in the first, but not second, branchial arch. First, but not second, arch mesoderm of Pitx2 mutants failed to enlarge after embryonic day 9.5, well before the onset of the myogenic progression. Thus, Pitx2 contributes to specification of first, but not second, arch mesoderm. The jaw of Pitx2 mutants was vestigial by midgestation, but significant size reductions were observed as early as embryonic day 10.5. The diminutive first branchial arch of mutants could not be explained by loss of mesoderm alone, suggesting that Pitx2 contributes to the earliest specification of jaw itself.
机译:在胚胎肌肉胶原蛋白的成肌过程的所有状态中均观察到Pitx2表达,并在成年肌肉中持续存在。 Pitx2突变小鼠形成除少数肌肉胶原蛋白外的所有胶原蛋白。肌肉胶原蛋白的损失或变性通常可归因于由Pitx2表型的某些其他方面引起的肌肉附着位点的丢失。缺少第一个branch弓的肌肉,而在妊娠中期,Pitx2突变体仅使第二个arch弓的肌肉变形。 Pitx2在第一个(但第二个)branch门中胚层开始生肌进程之前很早就表达了,并且是开始肌原性进程所必需的。在第一个但不是第二个arch弓中表达成肌细胞前体指标标记Tbx1,Tcf21和Msc也需要Pitx2。首先,但不是第二,Pitx2突变体的弓形中胚层在胚胎第9.5天后,即在成肌进程开始之前就未能扩大。因此,Pitx2有助于规范第一但不是第二拱门中胚层。 Pitx2突变体的颌骨在妊娠中期残留,但是在胚胎第10.5天时观察到大小明显减小。仅通过中胚层的丧失不能解释突变体的小第一分支弓,这表明Pitx2有助于颌骨本身的最早规格。

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