首页> 外文期刊>Developmental dynamics: an official publication of the American Association of Anatomists >Mouse PeP: a novel peroxisomal protein linked to myoblast differentiation and development.
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Mouse PeP: a novel peroxisomal protein linked to myoblast differentiation and development.

机译:小鼠PeP:一种与成肌细胞分化和发育有关的新型过氧化物酶体蛋白。

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摘要

The identification of several peroxisomal proteins in the past decade has deepened our understanding of the biology of peroxisomes and their involvement in human disorders. We report the cloning and expression pattern during the mouse development of a cDNA encoding a novel protein, named PeP, and show that its product is imported specifically to the peroxisome matrix in a variety of cell types. We also demonstrate that PeP is imported to the organelle through the PEX5 receptor pathway, which indicates that the C-terminal tripeptide SKI behaves as a type 1 peroxisomal targeting signal (PTS1). PeP expression is tightly regulated, as shown by Northern and in situ hybridization experiments. Thus during embryonic development in the mouse, PeP mRNA is detected almost exclusively in the skeletal muscle, whereas in adult mice, strong expression is also found in the heart and brain. In addition, PeP mRNA accumulation is induced after myoblast differentiation in vitro, when myotube formation is promoted. Sequence analysis reveals that PeP has no significant homology to any known protein, except for a short stretch of amino acids containing the fingerprint of the fibronectin type III superfamily, a domain present in proteins often related to molecular and cellular recognition and binding processes. Thus our data suggest a connection between the function of PeP and murine cell differentiation and development.
机译:在过去十年中对几种过氧化物酶体蛋白的鉴定,加深了我们对过氧化物酶体生物学及其与人类疾病的关系的了解。我们报告了小鼠的发展过程中编码一种新型蛋白质,称为PeP的cDNA的克隆和表达模式,并表明其产物被特异性导入多种细胞类型的过氧化物酶体基质中。我们还证明了PeP通过PEX5受体途径导入细胞器,这表明C端三肽SKI表现为1型过氧化物酶体靶向信号(PTS1)。 PeP的表达受到严格的调控,如Northern和原位杂交实验所示。因此,在小鼠胚胎发育过程中,几乎只在骨骼肌中检测到了PeP mRNA,而在成年小鼠中,在心脏和大脑中也发现了强表达。另外,当促成肌管形成时,在体外成肌细胞分化后诱导PeP mRNA积累。序列分析表明,PeP与任何已知蛋白质均无显着同源性,只是一小段氨基酸含有纤连蛋白III型超家族的指纹,该家族存在于蛋白质中,通常与分子和细胞识别及结合过程有关。因此,我们的数据表明了PeP的功能与鼠细胞分化和发育之间的联系。

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