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MAKING TISSUE-TYPE PLASMINOGEN-ACTIVATOR MORE FIBRIN SPECIFIC

被引:27
作者
PAONI, NF [1 ]
CHOW, AM [1 ]
PENA, LC [1 ]
KEYT, BA [1 ]
ZOLLER, MJ [1 ]
BENNETT, WF [1 ]
机构
[1] GENENTECH INC,DEPT PROT ENGN,S SAN FRANCISCO,CA 94080
来源
PROTEIN ENGINEERING | 1993年 / 6卷 / 05期
关键词
FIBRIN; FIBRINOLYSIS; MUTAGENESIS; TPA;
D O I
10.1093/protein/6.5.529
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
The fibrin specificity of tissue-type plasminogen activator can be increased by mutagenesis within at least four sites in the protease domain. These sites include residue 1276, the new N-terminus formed by conversion to a two-chain structure, residues on either side of the active site cleft, KHRR 296-299 or DDD 364-366, a charged surface involved in fibrin interactions, which includes residues H432, R434, D460, R462 and a loop structure, PQANL 466-470, near the fibrin-binding patch. Variants with mutations at any of these sites have low fibrinogen-stimulated activity, whereas fibrin-stimulated activity is at least normal. Kinetic analysis reveals that mutations at these positions reduce the k(cat) in the presence of fibrinogen, but leave the molecules with normal kinetic constants in the presence of fibrin. A significant exception is found at positions 296-299, where the presence of fibrin manifests significant increases in both k(cat) and K(m). Combinations of mutations at these sites appear to be additive with respect to fibrin specificity.
引用
收藏
页码:529 / 534
页数:6
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