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人血清白蛋白内含子的特定组合可在转染的COS细胞和转基因小鼠的乳汁中指导白蛋白的高水平表达。

Specific combinations of human serum albumin introns direct high level expression of albumin in transfected COS cells and in the milk of transgenic mice.

作者信息

Hurwitz D R, Nathan M, Barash I, Ilan N, Shani M

机构信息

Rhône-Poulenc Rorer Central Research, Collegeville, PA 19426.

出版信息

Transgenic Res. 1994 Nov;3(6):365-75. doi: 10.1007/BF01976768.

Abstract

A new series of expression vectors, each comprised of the beta-lactoglobulin (BLG) promoter driving one of a variety of human serum albumin (HSA) minigenes or the entire gene, were evaluated for their ability to direct expression of HSA in vitro in COS tissue culture cells and into the milk of transgenic mice. Vectors directed a hierarchy of expression levels in vitro, dependent upon the specific complement of HSA introns included. HSA introns acted in a synergistic manner. In addition, minigenes comprised of specific subsets of introns were more efficacious than the entire HSA gene with all of its introns. Transgenic mice expressed as much as 10 mg ml-1 of HSA in their milk. Vectors comprised of specific intron subsets directed levels at 1 mg ml-1 or greater in the milk of 20% of generated transgenics. A statistical correlation between the expression level trend in vitro with the trend of expression in vivo (% which express) at detectable levels (p = 0.0015) and at the level of greater than 0.1 mg ml-1 (p = 0.0156) was demonstrated. A weak correlation existed (p = 0.0526) at in vivo levels of 1 mg ml-1 or greater. These new vectors are expected to direct the production of high levels of HSA in the milk of a large percentage of generated transgenic dairy animals.

摘要

一系列新的表达载体被评估其在体外COS组织培养细胞中以及转基因小鼠乳汁中指导人血清白蛋白(HSA)表达的能力,每个载体都由驱动各种HSA小基因之一或整个基因的β-乳球蛋白(BLG)启动子组成。载体在体外指导了不同层次的表达水平,这取决于所包含的HSA内含子的特定组成。HSA内含子以协同方式起作用。此外,由特定内含子子集组成的小基因比包含所有内含子的完整HSA基因更有效。转基因小鼠乳汁中HSA的表达量高达10 mg/ml。由特定内含子子集组成的载体在20%的转基因小鼠乳汁中指导的表达水平达到1 mg/ml或更高。在可检测水平(p = 0.0015)以及大于0.1 mg/ml的水平(p = 0.0156)下,体外表达水平趋势与体内表达趋势(表达的百分比)之间存在统计学相关性。在体内水平为1 mg/ml或更高时存在弱相关性(p = 0.0526)。预计这些新载体将在很大比例的转基因奶牛的乳汁中指导高水平HSA的产生。

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