REGULATION OF A DOUBLE-STRANDED-RNA MODIFICATION ACTIVITY IN HUMAN-CELLS

被引：9

作者：

MORRISSEY, LM

KIRKEGAARD, K

机构：

[1] UNIV COLORADO,HOWARD HUGHES MED INST,BOULDER,CO 80309

[2] UNIV COLORADO,DEPT MOLEC CELLULAR & DEV BIOL,BOULDER,CO 80309

来源：

MOLECULAR AND CELLULAR BIOLOGY | 1991年 / 11卷 / 07期

关键词：

D O I：

10.1128/MCB.11.7.3719

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：

A double-stranded RNA (dsRNA)-specific modification activity from Xenopus oocytes and human cells (dsRNA modifier) converts adenosine residues present in dsRNA to inosines. The function of the dsRNA modifier is unknown, although it has been suggested that it may be part of the cellular antiviral response. We investigated the relationship between the activity of the dsRNA modifier, viral infection, and the antiviral response in human cells induced by poly(rI)-poly(rC) [poly(I.C)] treatment. We found, unexpectedly, that treatment of HeLa cells with poly(I.C) or other dsRNA molecules resulted in the dramatic inhibition of the dsRNA modifier. Mixing experiments, reconstruction experiments, and pretreatment of extracts with RNases indicated that inhibition of the dsRNA modifier did not result from the continued presence of a soluble inhibitor (such as dsRNA) in the in vitro modification reactions. Treatment of cells with cyclohexamide or dactinomycin simultaneously with the poly(I.C) demonstrated that in vivo inhibition of the dsRNA modifier did not require new transcription or translation. The dsRNA modification activity was also substantially inhibited in cells infected with poliovirus and was slightly inhibited in cells infected with adenovirus. The inhibition of the dsRNA modifier during the antiviral state is thus not consistent with an antiviral function, and instead suggests another cellular function for dsRNA modification.

引用

页码：3719 / 3725

页数：7

共 47 条

[1] SYNTHETIC POLYNUCLEOTIDES AND AMINO ACID CODE .5.
BASILIO, C
WAHBA, AJ
OCHOA, S
SPEYER, JF
LENGYEL, P
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1962, 48 (04) : 613 - &
[2] AN UNWINDING ACTIVITY THAT COVALENTLY MODIFIES ITS DOUBLE-STRANDED-RNA SUBSTRATE
BASS, BL
WEINTRAUB, H
[J]. CELL, 1988, 55 (06) : 1089 - 1098
[3] A DEVELOPMENTALLY REGULATED ACTIVITY THAT UNWINDS RNA DUPLEXES
BASS, BL
WEINTRAUB, H
[J]. CELL, 1987, 48 (04) : 607 - 613
[4] BIASED HYPERMUTATION OF VIRAL-RNA GENOMES COULD BE DUE TO UNWINDING MODIFICATION OF DOUBLE-STRANDED-RNA
BASS, BL
WEINTRAUB, H
CATTANEO, R
BILLETER, MA
[J]. CELL, 1989, 56 (03) : 331 - 331
[5] BASS BL, 1991, IN PRESS ANTISENSE R
[6] POLIOVIRUS MUTANT THAT DOES NOT SELECTIVELY INHIBIT HOST-CELL PROTEIN-SYNTHESIS
BERNSTEIN, HD
SONENBERG, N
BALTIMORE, D
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1985, 5 (11) : 2913 - 2923
[7] THE CELLULAR 68,000-MR PROTEIN-KINASE IS HIGHLY AUTOPHOSPHORYLATED AND ACTIVATED YET SIGNIFICANTLY DEGRADED DURING POLIOVIRUS INFECTION - IMPLICATIONS FOR TRANSLATIONAL REGULATION
BLACK, TL
SAFER, B
HOVANESSIAN, A
KATZE, MG
[J]. JOURNAL OF VIROLOGY, 1989, 63 (05) : 2244 - 2251
[8] MUTATED AND HYPERMUTATED GENES OF PERSISTENT MEASLES VIRUSES WHICH CAUSED LETHAL HUMAN-BRAIN DISEASES
CATTANEO, R
SCHMID, A
SPIELHOFER, P
KAELIN, K
BACZKO, K
TERMEULEN, V
PARDOWITZ, J
FLANAGAN, S
RIMA, BK
UDEM, SA
BILLETER, MA
[J]. VIROLOGY, 1989, 173 (02) : 415 - 425
[9] BIASED HYPERMUTATION AND OTHER GENETIC CHANGES IN DEFECTIVE MEASLES VIRUSES IN HUMAN-BRAIN INFECTIONS
CATTANEO, R
SCHMID, A
ESCHLE, D
BACZKO, K
TERMEULEN, V
BILLETER, MA
[J]. CELL, 1988, 55 (02) : 255 - 265
[10] ACTIVATION OF THE HUMAN INTERFERON-BETA GENE REQUIRES AN INTERFERON-INDUCIBLE FACTOR
ENOCH, T
ZINN, K
MANIATIS, T
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1986, 6 (03) : 801 - 810

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