Dodd I, Nunn B, Robinson J H
Beecham Pharmaceuticals Research Division, Biosciences Research Centre, Epsom, Surrey, UK.
Thromb Haemost. 1988 Jun 16;59(3):523-8.
Purified preparations of recombinant tissue-type plasminogen activator (t-PA) from the recombinant Bowes melanoma cell line TRBM6 were shown to contain multiple species of plasminogen activator. Using a combination of chromatography on Sephadex G25, Sephadex G75 and Heparin Sepharose CL6B we have isolated two fibrinolytically active species, which, under non-reduced SDS PAGE, have apparent Mr = 38,000 and 56,000. Double immunodiffusion studies indicated that both species were closely related to both the t-PA B chain and t-PA itself. N-terminal sequencing identified the Mr = 38,000 species as ala160- t-PA (essentially delta FGKI t-PA) and the Mr = 56,000 species as ser1-tyr2-gln3-glyx-cys51 t-PA (delta F t-PA), the latter probably produced by alternative splicing of the t-PA gene. The pharmacokinetic properties of N,N dimethyl-4-aminobenzoyl (DAB) derivatives of these activators and native t-PA were determined in the guinea pig. Whereas DAB----delta F t-PA showed a similar, rapid plasma disappearance profile to that of DAB----t-PA, DAB----delta FGKI t-PA was cleared significantly slower. These results suggest that a rapid clearance recognition site resides on either the growth factor or kringle 1, or both, domains of t-PA.
从重组的鲍伊斯黑色素瘤细胞系TRBM6中获得的重组组织型纤溶酶原激活剂(t-PA)纯化制剂显示含有多种纤溶酶原激活剂。通过结合使用葡聚糖凝胶G25、葡聚糖凝胶G75和肝素琼脂糖CL6B进行层析,我们分离出了两种具有纤溶活性的物质,在非还原SDS-PAGE条件下,它们的表观分子量分别为38,000和56,000。双向免疫扩散研究表明,这两种物质都与t-PA B链和t-PA本身密切相关。N端测序确定分子量为38,000的物质为ala160 - t-PA(本质上是δFGKI t-PA),分子量为56,000的物质为ser1-tyr2-gln3-glyx-cys51 t-PA(δF t-PA),后者可能是由t-PA基因的可变剪接产生的。在豚鼠中测定了这些激活剂和天然t-PA的N,N-二甲基-4-氨基苯甲酰(DAB)衍生物的药代动力学特性。尽管DAB-δF t-PA的血浆消失曲线与DAB-t-PA相似且迅速,但DAB-δFGKI t-PA的清除明显较慢。这些结果表明,快速清除识别位点位于t-PA的生长因子或kringle 1结构域,或两者上。
