Plasminogen activator and plasmin-like activities in experimental rat tumours.

J Tözsér, A Hamvas, P Rády, P Kertai, P Elödi
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Abstract

Plasminogen activator activity and plasmin-like amidolytic activity were investigated in two experimental rat tumours, using human plasminogen and chromogenic peptide substrate, S-2251. The invasive hepatocarcinoma and non-invasive nephroma were induced with the same chemical carcinogen, dimethylnitrosamine, in F-344 rats and they were continuously transplanted under the renal capsule. While there was no difference in plasmin-like activities of the tumours, the plasminogen activator activity was very low in the nephroma, but high in the hepatocarcinoma. Since the activator activity was completely inhibited by amiloride, it was considered to be of urokinase-type. These results were in accordance with the assumed role of urokinase in the invasion. However, of the respective control organ, kidney was rich in both activities but rat liver contained only very low activities. Therefore the comparison of the plasminogen activator activity of a tumour to the control organ probably does not provide information concerning the malignant transformation as it is suggested in the literature.

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实验性大鼠肿瘤中的纤溶酶原激活物和纤溶酶样活性。
利用人纤溶酶原和显色肽底物S-2251,研究了两种实验性大鼠肿瘤中纤溶酶原激活剂活性和纤溶酶样酶解活性。用相同的化学致癌物二甲基亚硝胺诱导F-344大鼠浸润性肝癌和非浸润性肾瘤,在肾包膜下连续移植。虽然肿瘤的纤溶酶样活性没有差异,但肾瘤的纤溶酶原激活物活性非常低,而肝癌的纤溶酶原激活物活性很高。由于激活剂活性被阿米洛利完全抑制,因此被认为是尿激酶型。这些结果与假设的尿激酶在侵袭中的作用一致。然而,在各自的对照器官中,肾脏和大鼠肝脏的活性都很丰富,而大鼠肝脏的活性却很低。因此,比较肿瘤与对照器官的纤溶酶原激活物的活性可能不能像文献中所建议的那样提供有关恶性转化的信息。
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