Pth1r Signal in Gli1+ Cells Maintains Postnatal Cranial Base Synchondrosis.

IF 8.3 2区 材料科学 Q1 MATERIALS SCIENCE, MULTIDISCIPLINARY ACS Applied Materials & Interfaces Pub Date : 2023-10-01 Epub Date: 2023-08-14 DOI:10.1177/00220345231184405
K Amano, Y Kitaoka, S Kato, M Fujiwara, D Okuzaki, T Aikawa, M Kogo, S Iida
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Abstract

Cranial base synchondroses are the endochondral ossification centers for cranial base growth and thus indispensable for proper skull, brain, and midfacial development. The synchondroses are composed of mirror-image growth plates that are continuously maintained from the embryonic to postnatal stage through chondrocyte differentiation. Several factors, including Pth1r signaling, are known to control fetal synchondrosis development. However, there are currently no reports regarding any role for Pth1r signaling in postnatal cranial base and synchondrosis development. Also, the mesenchymal cells that source Pth1r signaling for synchondroses are not known. Here, we employed an inducible mouse model, a hedgehog-responsive Gli1-CreERT2 driver, focusing on the postnatal study. We performed 2 inducible protocols using Gli1-CreERT2;Tomatofl/+ mice that uncovered distinct patterning of Gli1-positive and Gli1-negative chondrocytes in the synchondrosis cartilage. Moreover, we generated Gli1-CreERT2;Pth1rfl/fl;Tomatofl/+ mice to assess their functions in postnatal synchondrosis and found that the mutants had survived postnatally. The mutant skulls morphologically presented unambiguous phenotypes where we noticed the shortened cranial base and premature synchondrosis closure. Histologically, gradual disorganization in mutant synchondroses caused an uncommon remaining central zone between hypertrophic zones on both sides while the successive differentiation of round, flat, and hypertrophic chondrocytes was observed in control sections. These mutant synchondroses disappeared and were finally replaced by bone. Of note, the mutant fusing synchondroses lost their characteristic patterning of Gli1-positive and Gli1-negative chondrocytes, suggesting that loss of Pth1r signaling alters the distribution of hedgehog-responsive chondrocytes. Moreover, we performed laser microdissection and RNA sequencing to characterize the flat proliferative and round resting chondrocytes where we found flat chondrocytes have a characteristic feature of both chondrocyte proliferation and maturation. Taken together, these data demonstrate that Pth1r signaling in Gli1-positive cells is essential for postnatal development and maintenance in cranial base synchondroses. Our findings will elucidate previously unknown aspects of Pth1r functions in cranial biology and development.

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Gli1+细胞中的Pth1r信号维持产后颅底软骨病。
颅底同步软骨是颅底生长的软骨内骨化中心,因此对于颅骨、大脑和面中部的正常发育是必不可少的。同步软骨细胞由镜像生长板组成,通过软骨细胞分化,从胚胎到出生后一直保持生长。已知包括Pth1r信号传导在内的几个因素可以控制胎儿软骨结合的发育。然而,目前还没有关于Pth1r信号在出生后颅底和软骨发育中的任何作用的报道。此外,还不知道为同步玫瑰提供Pth1r信号的间充质细胞。在这里,我们采用了一种诱导型小鼠模型,一种对刺猬有反应的Gli1-CreERT2驱动器,专注于产后研究。我们使用Gli1-CreERT2进行了2种诱导型方案;Tomatofl/+小鼠在软骨结合软骨中发现了Gli1阳性和Gli1阴性软骨细胞的不同模式。此外,我们生成了Gli1-CreERT2;Pth1rfl/fl;Tomatofl/+小鼠评估其在出生后软骨结合中的功能,发现突变体在出生后存活。突变头骨在形态上表现出明确的表型,我们注意到颅底缩短和软骨结合过早闭合。组织学上,突变同步软骨细胞的逐渐紊乱导致两侧肥大区之间罕见的剩余中心区,而在对照切片中观察到圆形、扁平和肥大软骨细胞的连续分化。这些突变的同步软骨玫瑰消失了,最后被骨头取代了。值得注意的是,融合同步软骨细胞的突变体失去了Gli1阳性和Gli1阴性软骨细胞的特征模式,这表明Pth1r信号的缺失改变了刺猬反应性软骨细胞的分布。此外,我们进行了激光显微切割和RNA测序,以表征扁平增殖和圆形静止软骨细胞,我们发现扁平软骨细胞具有软骨细胞增殖和成熟的特征。总之,这些数据表明,Gli1阳性细胞中的Pth1r信号传导对于出生后颅底同步软骨的发育和维持至关重要。我们的发现将阐明Pth1r功能在颅骨生物学和发育中以前未知的方面。
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来源期刊
ACS Applied Materials & Interfaces
ACS Applied Materials & Interfaces 工程技术-材料科学:综合
CiteScore
16.00
自引率
6.30%
发文量
4978
审稿时长
1.8 months
期刊介绍: ACS Applied Materials & Interfaces is a leading interdisciplinary journal that brings together chemists, engineers, physicists, and biologists to explore the development and utilization of newly-discovered materials and interfacial processes for specific applications. Our journal has experienced remarkable growth since its establishment in 2009, both in terms of the number of articles published and the impact of the research showcased. We are proud to foster a truly global community, with the majority of published articles originating from outside the United States, reflecting the rapid growth of applied research worldwide.
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