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组织型纤溶酶原激活物转基因大鼠的构建与鉴定。

Generation and characterization of tissue-type plasminogen activator transgenic rats.

机构信息

Rare Disease & LCM Laboratories, Daiichi Sankyo Co., Ltd., 1-2-58 Hiromachi, Shinagawa-ku, Tokyo, 140-8710, Japan.

Pharmacovigilance Department, Daiichi Sankyo Co., Ltd., Tokyo, Japan.

出版信息

J Thromb Thrombolysis. 2018 Jan;45(1):77-87. doi: 10.1007/s11239-017-1582-1.

Abstract

To address a species difference in the responsiveness to human recombinant tissue-type plasminogen activator (rt-PA) between rats and humans, tPA transgenic (Tg) rats were generated and characterized. In the rats, transcriptional regulation of tPA was designed under the control of the endogenous tPA promoter. There were no significant differences in hematological parameters between the tPA Tg and non Tg rats. Plasma tPA concentration was significantly increased and serum free PAI-1 was significantly decreased in the tPA Tg rats. Significant overexpression of tPA mRNA in five major organs was also confirmed in the tPA Tg rats. In contrast, the extent of tPA mRNA induction by pathophysiological stimuli (focal cerebral ischemia) was comparable in the two strains. Earlier increase in the plasma D-Dimer level was observed in the tPA Tg rats in a model of thromboembolism compared with the non Tg rats. On the other hand, there was no statistically significant prolongation of bleeding time in a rat model of bleeding between the two strains. rt-PA showed dose-related blood flow restoration in a rat model of thromboembolic stroke in the tPA Tg rats from a dose (1 mg/kg, i.v.) similar to clinical doses for human stroke patients. In conclusion, tPA Tg rats, in which tPA is overexpressed and endogenous fibrinolytic activity is enhanced without hemostatic abnormality, were generated. tPA Tg rats would be beneficial for the pharmacological and the toxicological evaluation of rt-PA and other various fibrinolytic enhancers.

摘要

为了解决大鼠和人类对人重组组织型纤溶酶原激活剂(rt-PA)反应的种属差异,我们生成并鉴定了 tPA 转基因(Tg)大鼠。在大鼠中,tPA 的转录调控受内源性 tPA 启动子的控制。Tg 大鼠和非 Tg 大鼠之间的血液学参数没有显著差异。tPA Tg 大鼠的血浆 tPA 浓度显著升高,血清游离 PAI-1 显著降低。还证实 tPA Tg 大鼠的五个主要器官中 tPA mRNA 的表达显著增加。相比之下,两种品系中 tPA mRNA 的诱导程度相当。与非 Tg 大鼠相比,在血栓栓塞模型中,tPA Tg 大鼠的血浆 D-二聚体水平更早升高。另一方面,两种品系之间在出血模型中的出血时间没有统计学上的显著延长。rt-PA 在 tPA Tg 大鼠的血栓栓塞性中风模型中表现出剂量相关性的血流恢复,其剂量(1mg/kg,iv)与人类中风患者的临床剂量相似。总之,生成了 tPA 过表达且内源性纤溶活性增强而无止血异常的 tPA Tg 大鼠。tPA Tg 大鼠将有利于 rt-PA 和其他各种纤溶增强剂的药理学和毒理学评价。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cd82/5756269/7192b196977d/11239_2017_1582_Fig1_HTML.jpg

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