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Prickle1 调节额骨成骨细胞的分化。

Prickle1 regulates differentiation of frontal bone osteoblasts.

机构信息

Center for Craniofacial Regeneration, Department of Oral Biology, School of Dental Medicine, University of Pittsburgh, Pittsburgh, PA, USA.

Department of Developmental Biology, School of Medicine, University of Pittsburgh, Pittsburgh, PA, USA.

出版信息

Sci Rep. 2018 Dec 21;8(1):18021. doi: 10.1038/s41598-018-36742-0.

Abstract

Enlarged fontanelles and smaller frontal bones result in a mechanically compromised skull. Both phenotypes could develop from defective migration and differentiation of osteoblasts in the skull bone primordia. The Wnt/Planar cell polarity (Wnt/PCP) signaling pathway regulates cell migration and movement in other tissues and led us to test the role of Prickle1, a core component of the Wnt/PCP pathway, in the skull. For these studies, we used the missense allele of Prickle1 named Prickle1 (Prickle1). The Prickle1 mutants are microcephalic and develop enlarged fontanelles between insufficient frontal bones, while the parietal bones are normal. Prickle1 mutants have several other craniofacial defects including a midline cleft lip, incompletely penetrant cleft palate, and decreased proximal-distal growth of the head. We observed decreased Wnt/β-catenin and Hedgehog signaling in the frontal bone condensations of the Prickle1 mutants. Surprisingly, the smaller frontal bones do not result from defects in cell proliferation or death, but rather significantly delayed differentiation and decreased expression of migratory markers in the frontal bone osteoblast precursors. Our data suggests that Prickle1 protein function contributes to both the migration and differentiation of osteoblast precursors in the frontal bone.

摘要

囟门增大和额骨变小导致颅骨结构不稳定。这两种表型都可能是由于颅骨原基中的成骨细胞迁移和分化缺陷所致。Wnt/平面细胞极性(Wnt/PCP)信号通路调节其他组织中的细胞迁移和运动,这促使我们研究 Wnt/PCP 通路的核心组成部分之一 Prickle1 在颅骨中的作用。在这些研究中,我们使用了命名为 Prickle1(Prickle1)的错义等位基因的 Prickle1 突变体。Prickle1 突变体头部短小,额骨之间的囟门增大,而顶骨正常。Prickle1 突变体还有其他几种颅面缺陷,包括中线唇裂、不完全穿透性腭裂以及头部近-远轴生长减少。我们观察到 Prickle1 突变体的额骨骨化中心中的 Wnt/β-连环蛋白和 Hedgehog 信号减少。令人惊讶的是,较小的额骨并不是由于细胞增殖或死亡缺陷引起的,而是额骨成骨细胞前体细胞的分化明显延迟和迁移标志物的表达减少。我们的数据表明,Prickle1 蛋白功能有助于额骨成骨细胞前体的迁移和分化。

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