PHOSPHOROTHIOATE ANALOGS OF (2'-5')(A)4 - AGONIST AND ANTAGONIST ACTIVITIES IN INTACT-CELLS

被引:21
作者
CHARACHON, G
SOBOL, RW
BISBAL, C
SALEHZADA, T
SILHOL, M
CHARUBALA, R
PFLEIDERER, W
LEBLEU, B
SUHADOLNIK, RJ
机构
[1] TEMPLE UNIV,HLTH SCI CTR,SCH MED,DEPT BIOCHEM,PHILADELPHIA,PA 19140
[2] UNIV CONSTANCE,FAK CHEM,W-7750 CONSTANCE,GERMANY
关键词
D O I
10.1021/bi00462a017
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
Metabolically stable phosphorothioate tetramer analogues of (2’-5’)(A)n with Rp and/or Sp chirality in the 2’-5’-phosphodiester linkages constitute a new class of antiviral agents since they mimic the effects of interferons. Three of the diastereomeric 5’-monophosphates (i.e., pRpRpRp, pSpRpRp, and pRpSpSp) bind to and activate RNase L from extracts of HeLa cells. However, the pSpSpSp (2’-5’)- (A)4-phosphorothioate is unique in that it binds to, but cannot activate, RNase L to cleave rRNA. When microinjected into the cytoplasm of HeLa cells followed by virus infection, the pRpRpRp, pSpRpRp, and pRpSpSp (2’-5’)(A)4-phosphorothioates demonstrate antiviral activity, as does (2’-5’)(A)4ox-red, an active (2’-5’)(A)n analogue. When microinjected simultaneously with (2’-5’)(A)n ox-red, the pSpSpSp (2’- 5’)(A)4-phosphorothioate inhibits activation of RNase L in HeLa cells, thereby blocking direct protection of vesicular stomatitis virus. The agonist and antagonist properties of pRpRpRp and pSpSpSp, respectively, are transient probably as a consequence of the hydrolysis of the 5’-monophosphate and formation of the less active (2’-5’)(A)4-phosphorothioate cores. The possible use of these (2’-5’)(A)4-phosphorothioates as tools for dissecting the biological significance of the (2’-5’)(A)n system or in antiviral chemotherapy is discussed. © 1990, American Chemical Society. All rights reserved.
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页码:2550 / 2556
页数:7
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