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引用次数: 33
摘要
我们最近描述了一种肿瘤相关胰蛋白酶抑制剂(TATI)的纯化和特性。对其n端序列的研究表明其与胰腺分泌型胰蛋白酶抑制剂(PSTI)同源。,佩索宁,K., Kalkkinen, N.和斯坦曼,u - h .。(1982) [j]。化学,257,13713-13716)。我在此报告在人类精浆中出现的一种tti样活性。该抑制剂在精浆中的浓度变化很大(4-500 ng/ml, n = 50)。在放射免疫分析中,新的精浆抑制剂与纯化的TATI的剂量-反应曲线是平行的。通过凝胶过滤、反相液相色谱和离子交换色谱等方法验证了两种抑制剂的相似性。离子交换色谱法可将该抑制剂从主要精浆胰蛋白酶抑制剂中分离出来。纯化后的TATI可有效抑制人的顶蛋白。
Demonstration of a new acrosin inhibitor in human seminal plasma.
We have recently described the purification and characterization of a tumor-associated trypsin inhibitor (TATI). Studies on its N-terminal sequence suggested identity with the pancreatic secretory trypsin inhibitor (PSTI) (Huhtala, M.-L., Pesonen, K., Kalkkinen, N. & Stenman, U.-H. (1982) J. Biol. Chem. 257, 13713-13716). I report here the occurrence of a TATI-like activity in human seminal plasma. Concentrations of this inhibitor in seminal plasma varied considerably (4-500 ng/ml, n = 50). In radioimmunoassay the dose-response curves of the new seminal plasma inhibitor and purified TATI were parallel. The similarity between these two inhibitors was demonstrated by gel filtration, reverse phase liquid chromatography and ion-exchange chromatography. By ion exchange chromatography the new inhibitor could be separated from the main seminal plasma trypsin inhibitors. Purified TATI was shown to inhibit human acrosin effectively.
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