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在转基因小鼠乳腺中生产重组人I型原胶原同三聚体。

Production of recombinant human type I procollagen homotrimer in the mammary gland of transgenic mice.

作者信息

Toman P D, Pieper F, Sakai N, Karatzas C, Platenburg E, de Wit I, Samuel C, Dekker A, Daniels G A, Berg R A, Platenburg G J

机构信息

Cohesion Technologies, Palo Alto, CA 94303, USA.

出版信息

Transgenic Res. 1999;8(6):415-27. doi: 10.1023/a:1008959924856.

Abstract

The large scale production of recombinant collagen for use in biomaterials requires an efficient expression system capable of processing a large (> 400 Kd) multisubunit protein requiring post-translational modifications. To investigate whether the mammary gland of transgenic animals fulfills these requirements, transgenic mice were generated containing the alpha S1-casein mammary gland-specific promoter operatively linked to 37 Kb of the human alpha 1(I) procollagen structural gene and 3' flanking region. The frequency of transgenic lines established was 12%. High levels of soluble triple helical homotrimeric [(alpha 1)3] type I procollagen were detected (up to 8 mg/ml) exclusively in the milk of six out of 9 lines of lactating transgenic mice. The transgene-derived human procollagen chains underwent efficient assembly into a triple helical structure. Although proline or lysine hydroxylation has never been described for any milk protein, procollagen was detected with these post-translational modifications. The procollagen was stable in milk; minimal degradation was observed. These results show that the mammary gland is capable of expressing a large procollagen gene construct, efficiently assembling the individual polypeptide chains into a stable triple helix, and secreting the intact molecule into the milk.

摘要

用于生物材料的重组胶原蛋白的大规模生产需要一个高效的表达系统,该系统能够处理需要进行翻译后修饰的大型(> 400 Kd)多亚基蛋白。为了研究转基因动物的乳腺是否满足这些要求,构建了转基因小鼠,其包含与37 Kb的人α1(I)前胶原结构基因和3'侧翼区域可操作连接的αS1-酪蛋白乳腺特异性启动子。建立转基因品系的频率为12%。仅在9个泌乳转基因小鼠品系中的6个品系的乳汁中检测到高水平的可溶性三螺旋同三聚体[(α1)3] I型前胶原(高达8 mg/ml)。转基因来源的人前胶原链有效地组装成三螺旋结构。尽管从未描述过任何乳蛋白的脯氨酸或赖氨酸羟基化,但检测到的前胶原具有这些翻译后修饰。前胶原在乳汁中稳定;观察到的降解极少。这些结果表明,乳腺能够表达大型前胶原基因构建体,有效地将单个多肽链组装成稳定的三螺旋,并将完整分子分泌到乳汁中。

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