缝合间充质干细胞在颅面骨发育、修复和再生中的作用。

IF 1.1 Q4 MEDICINE, RESEARCH & EXPERIMENTAL
Takamitsu Maruyama
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引用次数: 4

摘要

骨骼的发育是通过两种不同的骨化机制介导的。颅面骨主要通过膜内骨化形成,这一机制不同于身体骨骼发育所需的软骨内骨化。两者的骨骼结构非常不同,因此它们可能具有独特的干细胞群。缝合线是颅面骨骼健康发育的重要生长中心。缝合线形态发生的缺陷导致其过早闭合,导致颅缝闭闭,这是一种毁灭性的疾病,每2500人中就有1人患病。缝合间充质被认为是颅骨形态发生所必需的骨骼干细胞的生态位。然而,关于缝合生物学的知识非常有限,缝合干细胞(SuSCs)尚未被分离出来。在这里,我们报告了鉴定和分离居住在缝线中线的干细胞群的第一个证据。在1年的监测期内,SuSCs的遗传标记显示它们具有自我更新和不断产生成熟细胞类型的能力。在颅骨发育和体内平衡维持过程中,它们在生态位中保持定位,不断产生成骨后代。损伤后,SuSCs在成骨间质周围急剧扩张,迁移到受损部位,并以细胞自主的方式直接促进骨骼修复。使用有限稀释移植也可以确定SuSCs的再生、多能性和频率。体内克隆扩增分析表明单个SuSC能够生成骨骼。此外,SuSC移植到受伤的颅骨通过直接植入促进愈合过程。我们的研究结果表明,SuSCs是真正的骨骼干细胞,非常适合于基于细胞的颅面骨治疗,因为它们具有移植、分化的能力。(在2019年4月16日第1980次会议上提交)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Stem cells of the suture mesenchyme in craniofacial bone development, repair and regeneration.

Development of the skeleton is mediated through two distinct ossification mechanisms. Craniofacial bones are formed mainly through intramembranous ossification, a mechanism different from endochondral ossification required for development of the body skeleton. The skeletal structures are quite distinct between the two, thus they are likely to have their unique stem cell populations. The sutures serve as the growth center critical for healthy development of the craniofacial skeleton. Defects in suture morphogenesis cause its premature closure, resulting in development of craniosynostosis, a devastating disease affecting 1 in ~2,500 individuals. The suture mesenchyme has been postulated to act as the niche of skeletal stem cells essential for calvarial morphogenesis. However, very limited knowledge is available for suture biology and suture stem cells (SuSCs) have yet to be isolated. Here we report the first evidence for identification and isolation of a stem cell population residing in the suture midline. Genetic labeling of SuSCs shows their ability to self-renew and continually give rise to mature cell types over a 1-year monitoring period. They maintain their localization in the niches constantly produce skeletogenic descendants during calvarial development and homeostastic maintenance. Upon injury, SuSCs expand drastically surrounding the skeletogenic mesenchyme, migrate to the damaged site and contribute directly to skeletal repair in a cell autonomous fashion. The regeneration, pluripotency and frequency of SuSCs are also determined using limiting dilution transplantation. In vivo clonal expansion analysis demonstrates a single SuSC capable of generating bones. Furthermore, SuSC transplantation into injured calvaria facilitates the healing processes through direct engraftments. Our findings demonstrate SuSCs are bona fide skeletal stem cells ideally suited for cell-based craniofacial bone therapy as they possess abilities to engraft, differentiate.(Presented at the 1980th Meeting, April 16, 2019).

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来源期刊
KEIO JOURNAL OF MEDICINE
KEIO JOURNAL OF MEDICINE MEDICINE, RESEARCH & EXPERIMENTAL-
CiteScore
3.10
自引率
0.00%
发文量
23
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