EFFECTIVE INTRACELLULAR INHIBITION OF THE CAMP-DEPENDENT PROTEIN-KINASE BY MICROINJECTION OF A MODIFIED FORM OF THE SPECIFIC INHIBITOR PEPTIDE PKI IN LIVING FIBROBLASTS

被引:27
作者
FERNANDEZ, A [1 ]
MERY, J [1 ]
VANDROMME, M [1 ]
BASSET, M [1 ]
CAVADORE, JC [1 ]
LAMB, NJC [1 ]
机构
[1] CNRS,INSERM,CTR RECH BIOCHIM MACROMOLEC,CELL BIOL UNIT,BP 5051,F-34033 MONTPELLIER,FRANCE
来源
EXPERIMENTAL CELL RESEARCH | 1991年 / 195卷 / 02期
关键词
D O I
10.1016/0014-4827(91)90398-E
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
In order to obtain a peptide retaining its biological activity following microinjection into living cells, we have modified a synthetic peptide [PKi(m)(6-24)], derived from the specific inhibitor protein of the cAMP-dependent protein kinase (A-kinase) in two ways: (1) substitution of the arginine at position 18 for a d-arginine; (2) blockade of the side chain on the C-terminal aspartic acid by a cyclohexyl ester group. In an in vitro assay, PKi(m) has retained a specific inhibitory activity against A-kinase as assessed against six other kinases, with similar efficiency to that of the unmodified PKi(5-24) peptide. Microinjection of PKi(m) into living fibroblasts reveals its capacity to prevent the changes in cell morphology and cytoskeleton induced by drugs which activate endogenous A-kinase, whereas the original PKi peptide failed to do so. This inhibition of A-kinase in vivo by PKi(m) lasts between 4 and 6 h after injection. In light of its effective half-life, this modified peptide opens a route for the use of biologically active peptides in vivo, an approach which has been hampered until now by the exceedingly short half-life of peptides inside living cells. By providing a direct means of inhibiting A-kinase activity for sufficiently long periods to observe effects on cellular functions in living cells, PKi(m) represents a powerful tool in studying the potential role of cAMP-dependent phosphorylation in vivo. © 1991.
引用
收藏
页码:468 / 477
页数:10
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