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Fgf8基因单倍剂量不足导致成年斑马鱼出现明显的颅面缺陷。

Fgf8 haploinsufficiency results in distinct craniofacial defects in adult zebrafish.

作者信息

Albertson R Craig, Yelick Pamela C

机构信息

Department of Biology, Biological Research Labs, Syracuse University, 130 College Place, Syracuse, NY 13244, USA.

出版信息

Dev Biol. 2007 Jun 15;306(2):505-15. doi: 10.1016/j.ydbio.2007.03.025. Epub 2007 Mar 24.

Abstract

Significant progress has been made toward understanding the role of fgf8 in directing early embryonic patterning of the pharyngeal skeleton. Considerably less is known about the role this growth factor plays in the coordinated development, growth, and remodeling of the craniofacial skeleton beyond embryonic stages. To better understand the contributions of fgf8 in the formation of adult craniofacial architecture, we analyzed the skeletal anatomy of adult ace(ti282a)/fgf8 heterozygous zebrafish. Our results revealed distinct skeletal defects including facial asymmetries, aberrant craniofacial geometry, irregular patterns of cranial suturing, and ectopic bone formation. These defects are similar in presentation to several human craniofacial disorders (e.g., craniosynostosis, hemifacial microsomia), and may be related to increased levels of bone metabolism observed in ace(ti282a)/fgf8 heterozygotes. Moreover, skeletal defects observed in ace(ti282a)/fgf8 heterozygotes are consistent with expression patterns of fgf8 in the mature craniofacial skeleton. These data reveal previously unrecognized roles for fgf8 during skeletogenesis, and provide a basis for future investigations into the mechanisms that regulate craniofacial development beyond the embryo.

摘要

在理解fgf8在引导咽骨骼早期胚胎模式形成中的作用方面已经取得了重大进展。关于这种生长因子在胚胎阶段之后颅面骨骼的协调发育、生长和重塑中所起的作用,人们了解得要少得多。为了更好地理解fgf8在成年颅面结构形成中的作用,我们分析了成年ace(ti282a)/fgf8杂合斑马鱼的骨骼解剖结构。我们的结果揭示了明显的骨骼缺陷,包括面部不对称、异常的颅面几何形状、颅骨缝合的不规则模式和异位骨形成。这些缺陷在表现上与几种人类颅面疾病(如颅缝早闭、半侧颜面发育不全)相似,并且可能与在ace(ti282a)/fgf8杂合子中观察到的骨代谢水平升高有关。此外,在ace(ti282a)/fgf8杂合子中观察到的骨骼缺陷与fgf8在成熟颅面骨骼中的表达模式一致。这些数据揭示了fgf8在骨骼发生过程中以前未被认识到的作用,并为未来研究调节胚胎以外颅面发育的机制提供了基础。

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