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首页> 外文期刊>Molecular and Cellular Biochemistry: An International Journal for Chemical Biology >Efficient secretion of biologically active Chondroitinase ABC from mammalian cells in the absence of an N-terminal signal peptide.
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Efficient secretion of biologically active Chondroitinase ABC from mammalian cells in the absence of an N-terminal signal peptide.

机译:在没有N端信号肽的情况下,从哺乳动物细胞中有效分泌生物活性软骨素酶ABC。

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摘要

Proteoglycans carrying chondroitin sulfate side chains have been shown to fulfill important biological functions in development, disease, and signaling. One area of considerable interest is the functional importance of chondroitin sulfates as inhibitors of the regeneration of axonal projections in the mammalian central nervous system. In animal models of spinal cord injury, injections of the enzyme Chondroitinase ABC from the bacterium Proteus vulgaris into the lesion site leads to degradation of chondroitin sulfates, and promotes axonal regeneration and significant functional recovery. Here, a mammalian expression system of an epitope-tagged Chondroitinase ABC protein is described. It is demonstrated that the addition of a eukaryotic secretion signal sequence to the N-terminus of the bacterial Chondroitinase ABC sequence allowed secretion, but interfered with function of the secreted enzyme. In contrast, expression of the Chondroitinase ABC gene without N-terminal eukaryotic secretion sequence or bacterial hydrophobic leader sequence led to efficient secretion of a biologically active Chondroitinase ABC protein from both immortalized and primary cells. Moreover, the C-terminal epitope tag could be utilized to follow expression of this protein. This novel Chondroitinase ABC gene is a valuable tool for a better understanding of the in vivo roles of chondroitin sulfates in mammalian development and disease, as well as in gene therapy approaches, including the treatment of spinal chord injuries.
机译:带有硫酸软骨素侧链的蛋白聚糖已被证明在发育,疾病和信号传导中具有重要的生物学功能。令人关注的一个领域是硫酸软骨素作为哺乳动物中枢神经系统中轴突投射的再生抑制剂的功能重要性。在脊髓损伤的动物模型中,从寻常变形杆菌(Proteus vulgaris)向病变部位注射软骨素酶ABC会导致硫酸软骨素降解,并促进轴突再生和显着的功能恢复。在此,描述了具有表位标记的软骨素酶ABC蛋白的哺乳动物表达系统。已经证明,在细菌软骨素酶ABC序列的N末端添加真核分泌信号序列可以分泌,但是会干扰分泌酶的功能。相反,没有N末端真核分泌序列或细菌疏水前导序列的软骨素酶ABC基因的表达导致永生化细胞和原代细胞有效地分泌生物活性软骨素酶ABC蛋白。此外,C末端表位标签可用于追踪该蛋白的表达。这个新的软骨素酶ABC基因是一个有价值的工具,可用于更好地了解硫酸软骨素在哺乳动物发育和疾病以及基因治疗方法(包括治疗脊柱脊髓损伤)中的体内作用。

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