Tissue plasminogen activator enhancing activity of vasopressin analogues in monkeys: structure-activity study.

H Vilhardt, T Barth
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引用次数: 0

Abstract

Marmocets were used in a structure activity study of the ability of vasopressin analogues to activate plasminogen activator (tPA). In evaluation of dDAVP analogues with L-alanine migrating from position 2 to 9 we found [L-Ala4]dDAVP and [L-Ala5]dDAVP to be potent activators of tPA. Double substitutions in dDAVP showed that combinations of a modification in position 4 valine with a change at position 2 (2-O-methyltyrosine) generated tPA releasing activity. On the other hand enlargement of the substituent at position 2 (2-O-ethyltyrosine) completely eliminated the activity of [L-Val4]dDAVP. The tPA activity is dependent on the position of a positively charged group at the amino acid in position 8 of the peptide chain. A shift of the guanido group further away from the backbone (D-arginine to D-homoarginine) resulted in a loss of tPA activating properties.

组织纤溶酶原激活剂增强猴抗利尿激素类似物的活性:结构-活性研究。
用狨猴进行了抗利尿激素类似物激活纤溶酶原激活物(tPA)的结构活性研究。在对l -丙氨酸从2位迁移到9位的dDAVP类似物的评价中,我们发现[L-Ala4]dDAVP和[L-Ala5]dDAVP是tPA的有效激活剂。对dDAVP的双取代表明,4位缬氨酸的修饰与2位(2- o -甲基酪氨酸)的改变组合产生了tPA释放活性。另一方面,2位取代基(2- o -乙基酪氨酸)的扩大完全消除了[L-Val4]dDAVP的活性。tPA活性取决于肽链第8位氨基酸上带正电基团的位置。胍基进一步远离主链(d -精氨酸到d -同型精氨酸)导致tPA激活特性的丧失。
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