首页> 外文期刊>Developmental dynamics: an official publication of the American Association of Anatomists >Kinetics of tamoxifen-regulated Cre activity in mice using a cartilage-specific CreER(T) to assay temporal activity windows along the proximodistal limb skeleton.
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Kinetics of tamoxifen-regulated Cre activity in mice using a cartilage-specific CreER(T) to assay temporal activity windows along the proximodistal limb skeleton.

机译:他莫昔芬调节的Cre活性在小鼠中的动力学,使用软骨特异性CreER(T)分析沿前肢肢体骨骼的时间活性窗口。

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摘要

Cartilage differentiation occurs over a broad time range from early embryonic development, when the mesenchymal condensations that give rise to cartilage models for future bone first appear, and continuing through adult life, when there is ongoing maintenance of articular joint surfaces and re-activation of cartilage formation after fracture. The chondrogenic response also figures in the pathogenesis of degenerative and inflammatory joint diseases. We have generated a transgenic line expressing tamoxifen-dependent Cre recombinase that gives efficient recombination in the chondrogenic lineage, both during embryogenesis and postnatally, and provides a valuable tool for analysis of gene function selectively in chondrogenic cells using conditional genetic approaches. Because the cartilage model of the limb skeleton forms progressively in a proximodistal order during discrete, well-defined time periods, evaluation of the spatial extent of tamoxifen-induced recombination along the limb axis during these timewindows has also enabled us to examine the pharmacokinetics of single-dose tamoxifen injections during pregnancy.
机译:软骨分化发生在很宽的时间范围内,从早期胚胎发育开始,即首次出现形成未来骨的软骨模型的间充质凝结,并持续到成年寿命,此时关节关节表面一直在维护并重新活化软骨。断裂后形成。软骨生成反应还涉及退行性和炎性关节疾病的发病机理。我们已经产生了一种表达他莫昔芬依赖性Cre重组酶的转基因品系,在胚胎发生期间和产后均在软骨生成谱系中提供有效的重组,并为使用条件遗传方法选择性地分析软骨生成细胞中的基因功能提供了有价值的工具。由于肢体骨骼的软骨模型在离散的,定义明确的时间段内以近现代顺序逐渐形成,因此在这些时间窗期间对他莫昔芬诱导的沿着肢体轴的重组的空间范围的评估也使我们能够检查单药的药代动力学。孕期注射他莫昔芬的剂量。

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