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生长激素质粒单次肌肉内给药与每日注射生长激素在矮小症小鼠中的生长反应比较。

Growth responses following a single intra-muscular hGH plasmid administration compared to daily injections of hGH in dwarf mice.

机构信息

Biotechnology Department, National Nuclear Energy Commission (IPEN-CNEN), Cidade Universitaria, São Paulo, SP, Brazil.

出版信息

Curr Gene Ther. 2012 Dec;12(6):437-43. doi: 10.2174/156652312803519797.

Abstract

In previous work, sustained levels of circulating human growth hormone (hGH) and a highly significant weight increase were observed after electrotransfer of naked plasmid DNA (hGH-DNA) into the muscle of immunodeficient dwarf mice (lit/scid). In the present study, the efficacy of this in vivo gene therapy strategy is compared to daily injections (5 μg/twice a day) of recombinant hGH (r-hGH) protein, as assessed on the basis of several growth parameters. The slopes of the two growth curves were found to be similar (P > 0.05): 0.095 g/mouse/d for protein and 0.094 g/mouse/d for DNA injection. In contrast, the weight increases averaged 35.5% (P < 0.001) and 23.1% (P < 0.01) for protein and DNA administration, respectively, a difference possibly related to the electroporation methodology. The nose-to-tail linear growth increases were 15% and 9.6% for the protein and DNA treatments, respectively, but mouse insulin-like growth factor I (mIGF-I) showed a greater increase over the control with DNA (5- to 7-fold) than with protein (3- to 4-fold) administration. The weight increases of several organs and tissues (kidneys, spleen, liver, heart, quadriceps and gastrocnemius muscles) were 1.3- to 4.6-fold greater for protein than for DNA administration, which gave a generally more proportional growth. Glucose levels were apparently unaffected, suggesting the absence of effects on glucose tolerance. A gene transfer strategy based on a single hGH-DNA administration thus appears to be comparable to repeated hormone injections for promoting growth and may represent a feasible alternative for the treatment of growth hormone deficiency.

摘要

在以前的工作中,我们观察到将裸质粒 DNA(hGH-DNA)电转移到免疫缺陷小矮人鼠(lit/scid)的肌肉中后,循环中的人类生长激素(hGH)水平持续升高,体重显著增加。在本研究中,我们比较了这种体内基因治疗策略与每天注射(5μg/天两次)重组 hGH(r-hGH)蛋白的疗效,其依据是多项生长参数。我们发现这两种生长曲线的斜率相似(P>0.05):蛋白为 0.095g/只/天,DNA 为 0.094g/只/天。相比之下,蛋白和 DNA 给药的体重增加平均值分别为 35.5%(P<0.001)和 23.1%(P<0.01),这一差异可能与电穿孔方法有关。蛋白和 DNA 治疗的鼻-尾线性生长增加分别为 15%和 9.6%,但 DNA 治疗的小鼠胰岛素样生长因子 I(mIGF-I)比蛋白治疗(3-4 倍)增加了 5-7 倍。几个器官和组织(肾脏、脾脏、肝脏、心脏、四头肌和腓肠肌)的重量增加分别为蛋白治疗的 1.3-4.6 倍,这表明 DNA 治疗的生长更具比例性。葡萄糖水平显然没有受到影响,这表明对葡萄糖耐量没有影响。因此,单次 hGH-DNA 给药的基因转移策略似乎与重复激素注射一样可促进生长,可能是治疗生长激素缺乏症的可行替代方法。

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