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骨骼组织和结缔组织形态发生的解偶联:软骨祖细胞中的条件性缺失揭示了 Lmx1b 在四肢背腹模式形成中具有细胞自主的需求。

Uncoupling skeletal and connective tissue patterning: conditional deletion in cartilage progenitors reveals cell-autonomous requirements for Lmx1b in dorsal-ventral limb patterning.

机构信息

Program in Genes and Development, University of Texas Health Sciences Center, Houston Graduate School of Biomedical Sciences, Houston, TX 77030, USA.

出版信息

Development. 2010 Apr;137(7):1181-8. doi: 10.1242/dev.045237.

DOI:10.1242/dev.045237
PMID:20215352
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2835331/
Abstract

Integration of muscle, connective tissue and skeletal patterning during development is essential for proper functioning of the musculoskeletal system. How this integration is achieved is poorly understood. There is ample evidence suggesting that skeletal pattern is programmed autonomously, whereas muscle pattern is, for the most part, programmed non-cell-autonomously. Connective tissues depend upon both muscle and skeletal tissues for their proper survival and development. Here, we employed a novel approach to dissect the coordination of musculoskeletal patterning during mouse limb development. Using both conditional gain- and loss-of-function approaches, we selectively deleted or activated the LIM-homeodomain transcription factor Lmx1b in skeletal progenitors using a Sox9-Cre knock-in allele. As Lmx1b is both necessary and sufficient to specify dorsal pattern, this approach allowed us to investigate the effect of selectively deleting or activating Lmx1b in skeletal progenitors on muscle, connective and skeletal tissues during limb development. Our results indicate that whereas Lmx1b activity is required autonomously in skeletal progenitors to direct dorsal pattern, loss or gain of Lmx1b activity in skeletal progenitors has no effect on muscle or connective tissue patterning. Hence, we show for the first time that skeletal and connective tissue patterning can be uncoupled, indicating a degree of autonomy in the formation of the musculoskeletal system.

摘要

在发育过程中,肌肉、结缔组织和骨骼形态的整合对于骨骼肌肉系统的正常功能至关重要。这种整合是如何实现的还知之甚少。有充分的证据表明,骨骼形态是自主编程的,而肌肉形态在很大程度上是非细胞自主编程的。结缔组织的正常生存和发育依赖于肌肉和骨骼组织。在这里,我们采用了一种新的方法来剖析小鼠肢体发育过程中骨骼肌肉形态的协调。我们使用条件性获得和缺失功能的方法,利用 Sox9-Cre 敲入等位基因,在骨骼祖细胞中选择性地缺失或激活 LIM 同源域转录因子 Lmx1b。由于 Lmx1b 对于指定背侧模式是必需的和充分的,因此这种方法使我们能够研究在肢体发育过程中,选择性地缺失或激活骨骼祖细胞中的 Lmx1b 对肌肉、结缔组织和骨骼组织的影响。我们的结果表明,尽管 Lmx1b 活性在骨骼祖细胞中自主地指导背侧模式,但骨骼祖细胞中 Lmx1b 活性的缺失或获得对肌肉或结缔组织形态没有影响。因此,我们首次表明骨骼和结缔组织形态可以解耦,这表明骨骼肌肉系统的形成具有一定的自主性。

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