MECHANISM OF DNA POLYMERASE-ALPHA INHIBITION BY APHIDICOLIN

被引:95
作者
SHEAFF, R [1 ]
ILSLEY, D [1 ]
KUCHTA, R [1 ]
机构
[1] UNIV COLORADO,DEPT CHEM & BIOCHEM,BOULDER,CO 80309
关键词
D O I
10.1021/bi00099a014
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
Synthetic oligonucleotides of defined sequence were used to examine the mechanism of calf thymus DNA polymerase alpha-inhibition by aphidicolin. Aphidicolin competes with each of the four dNTPs for binding to a pol alpha.DNA binary complex and thus should not be viewed as a dCTP analogue. Kinetic evidence shows that inhibition proceeds through the formation of a pol alpha.DNA.aphidicolin ternary complex, while DNase I protection experiments provide direct physical evidence. When deoxyguanosine is the next base to be replicated, K(i) = 0.2-mu-M. In contrast, the K(i) is 10-fold higher when the other dNMPs are at this position. Formation of a pol alpha.DNA.aphidicolin ternary complex did not inhibit the primase activity of the pol alpha.primase complex. Neither the rate of primer synthesis nor the size distribution of primers 2-10 nucleotides long was changed. Elongation of the primase-synthesized primers by pol a was inhibited both by ternary complex formation using exogenously added DNA and by aphidicolin alone.
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页码:8590 / 8597
页数:8
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