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Ucma is not necessary for normal development of the mouse skeleton

机译:Ucma对于鼠标骨骼的正常发育不是必需的

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摘要

Ucma (Upper zone of growth plate and Cartilage Matrix Associated protein) is a highly conserved tyrosine-sulphated secreted protein of Mw 17 kDa, which is expressed by juvenile chondrocytes. To evaluate the physiological function of this novel cartilage protein, we generated a Ucma-deficient mouse strain by introducing a lacZ/ neoR-cassette into the first exon of the Ucma gene. This mutation results in the complete loss of Ucma mRNA and protein expression. Surprisingly, however, although previous in vitro studies implied a role for Ucma in calcification and ossification, these processes were not affected in Ucma-deficient mice during normal development. Likewise, cartilage development was normal. While in previous works Ucma was mainly detected in the cartilage of embryonic and young mice, we detected Ucma expression also in the adult cartilage of the ribs using the lacZ cassette under the control of the Ucma promoter. Moreover, Ucma protein was specifically detected in adult growth plate cartilage by immunohistochemistry. Considering that skeletal development in Ucma-deficient mice is not significantly impaired, protein expression in adult cartilage indicates that Ucma might be involved in skeletal homeostasis and in the mechanical properties of the skeleton during challenging conditions such as ageing or disease.
机译:Ucma(生长板和软骨基质相关蛋白的上部区域)是Mw 17 kDa高度保守的酪氨酸硫酸盐分泌蛋白,由少年软骨细胞表达。为了评估这种新型软骨蛋白的生理功能,我们通过将lacZ / neoR-cassette导入Ucma基因的第一个外显子,产生了Ucma缺陷的小鼠品系。这种突变导致Ucma mRNA和蛋白质表达完全丧失。然而,令人惊讶的是,尽管先前的体外研究暗示了Ucma在钙化和骨化中的作用,但在正常发育过程中,这些过程在Ucma缺陷小鼠中并未受到影响。同样,软骨发育正常。尽管在以前的工作中,Ucma主要在胚胎和幼鼠的软骨中检测到,但我们使用lacZ盒在Ucma启动子的控制下,在肋骨的成年软骨中也检测到了Ucma表达。此外,通过免疫组织化学在成人生长板软骨中特异性检测到Ucma蛋白。考虑到Ucma缺陷小鼠的骨骼发育未受到明显损害,成年软骨中的蛋白质表达表明Ucma在挑战性条件下(例如衰老或疾病)可能参与骨骼的体内稳态和骨骼的机械特性。

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