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首页> 外文期刊>Journal of Endocrinological Investigation: Official Journal of the Italian Society of Endocrinology >Potential treatment of hypoparathyroidism with recombinant plasmids encoding preproparathyroid hormone
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Potential treatment of hypoparathyroidism with recombinant plasmids encoding preproparathyroid hormone

机译:用编码甲状旁腺原激素的重组质粒潜在治疗甲状旁腺功能低下

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摘要

Hypoparathyroidism cannot be cured by oral or intravenous calcium supplements. Using molecular biology techniques to induce the production of PTH is an ideal option to treat hypoparathyroidism. In this study, we established a recombinant plasmid encoding a mutant preproPTH with a skeletal muscle creatine kinase promoter (pCKM-mPTH). The sequence of the chimeric pCKM-mPTH gene was fully consistent with the DNA sequence reported previously and the site-directed mutagenesis was completed. Overlapping and nested PCR showed that PTH was highly expressed in and secreted from skeletal muscle cells transfected with the pCKM-mPTH plasmid: the PTH concentration in the culture medium 24 h after transfection was 26.37 pg/l. In the rat hypoparathyroidism model, serum PTH level significantly increased after injection with the pCKM-mPTH plasmid, compared with control groups (p<0.01). The effect lasted for about 30 days. Our results indicated that the recombinant mutant pCKM-mPTH plasmid was successfully constructed and was highly expressed in skeletal muscle cells. In vivo, the plasmid was introduced successfully into rat muscles and could express PTH for a decent period of time.
机译:甲状旁腺功能减退症不能通过口服或静脉内补钙来治愈。使用分子生物学技术诱导PTH的产生是治疗甲状旁腺功能低下的理想选择。在这项研究中,我们建立了一个编码具有骨骼肌肌酸激酶启动子(pCKM-mPTH)的突变体preproPTH的重组质粒。嵌合pCKM-mPTH基因的序列与先前报道的DNA序列完全一致,并且定点诱变完成。重叠和巢式PCR显示PTH在用pCKM-mPTH质粒转染的骨骼肌细胞中高表达和分泌:转染后24小时培养基中的PTH浓度为26.37 pg / l。在大鼠甲状旁腺功能低下模型中,与对照组相比,注射pCKM-mPTH质粒后血清PTH水平显着升高(p <0.01)。效果持续了大约30天。我们的结果表明重组突变体pCKM-mPTH质粒已成功构建并在骨骼肌细胞中高表达。在体内,该质粒已成功导入大鼠肌肉,并可以在相当长的一段时间内表达PTH。

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