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在乳腺特异性牛α-乳白蛋白调控序列驱动下,转基因小鼠乳汁中生物活性人凝血因子VIII的时空表达

Temporal and spatial expression of biologically active human factor VIII in the milk of transgenic mice driven by mammary-specific bovine alpha-lactalbumin regulation sequences.

作者信息

Chen Chuan-Mu, Wang Chih-Hong, Wu Shinn-Chih, Lin Chih-Cheng, Lin Shwu-Hwa, Cheng Winston T K

机构信息

Department of Zoology, National Chung Hsing University, Taichung, Taiwan, ROC.

出版信息

Transgenic Res. 2002 Jun;11(3):257-68. doi: 10.1023/a:1015651302674.

DOI:10.1023/a:1015651302674
PMID:12113458
Abstract

Hemophilia A is one of the major inherited bleeding disorders caused by a deficiency or abnormality in coagulation factor VIII (FVIII). Hemophiliacs have been treated with whole plasma or purified FVIII concentrates. The risk of transmitting blood-borne viruses and the cost of highly purified FVIII are the major factors that restrict prophylaxis in hemophilia therapy. One of the challenges created by the biotechnology revolution is the development of methods for the economical production of highly purified proteins in large scales. Recent developments indicate that manipulating milk composition using transgenesis has focused mainly on the mammary gland as a bioreactor to produce pharmaceuticals. In the present study, a hybrid gene containing bovine alpha-lactalbumin and human FVIII cDNA was constructed for microinjection into the pronuclei of newly fertilized mouse eggs. The alphaLA-hFVIII hybrid gene was confirmed to be successfully integrated and stably germ-line transmitted in 12 (seven females/five males) lines. Western-blot analysis of milk samples obtained from eight of the transgenic founders and F1 offspring indicated that the recombinant hFVIII was secreted into the milk of the transgenic mice. The concentrations of rFVIII ranged from 7.0 to 50.2 microg/ml, over 35-200-fold higher than that in normal human plasma. Up to 13.4 U/ml of rFVIII was detected in an assay in which rFVIII restored normal clotting activity to FVIII-deficient human plasma.

摘要

甲型血友病是由凝血因子VIII(FVIII)缺乏或异常引起的主要遗传性出血性疾病之一。血友病患者一直用全血或纯化的FVIII浓缩物进行治疗。传播血源性病毒的风险和高纯度FVIII的成本是限制血友病治疗中预防性治疗的主要因素。生物技术革命带来的挑战之一是开发大规模经济生产高纯度蛋白质的方法。最近的进展表明,利用转基因技术操纵乳汁成分主要集中在将乳腺作为生物反应器来生产药物。在本研究中,构建了一个包含牛α-乳白蛋白和人FVIII cDNA的杂交基因,用于显微注射到新受精的小鼠卵原核中。αLA-hFVIII杂交基因在12个品系(7只雌性/5只雄性)中被证实成功整合并稳定地通过种系传递。对从8只转基因奠基者和F1后代获得的乳汁样本进行的蛋白质印迹分析表明,重组人FVIII分泌到了转基因小鼠的乳汁中。重组FVIII的浓度范围为7.0至50.2微克/毫升,比正常人血浆中的浓度高35至200倍以上。在一项检测中,重组FVIII恢复了FVIII缺陷型人血浆的正常凝血活性,检测到的重组FVIII高达13.4国际单位/毫升。

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Interleukin 11 significantly increases plasma von Willebrand factor and factor VIII in wild type and von Willebrand disease mouse models.白细胞介素11可显著提高野生型和血管性血友病小鼠模型的血浆血管性血友病因子及凝血因子VIII水平。
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