Degradation of the interferon-induced 68,000-M(r) protein kinase by poliovirus requires RNA.

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J Virol. 1993 February; 67(2): 791-800

Degradation of the interferon-induced 68,000-M(r) protein kinase by poliovirus requires RNA.

T L Black, G N Barber and M G Katze

Department of Microbiology, School of Medicine, University of Washington, Seattle 98195.

ABSTRACT

Control of the interferon-induced double-stranded RNA (dsRNA)activated protein kinase (referred to as P68 because of itsM(r) of 68,000 in human cells) by animal viruses is essentialto avoid decreases in protein synthetic rates during infection.We have previously demonstrated that poliovirus establishesa unique way of regulating the protein kinase, namely by inducingthe specific degradation of P68 during infection (T. L. Black,B. Safer, A. Hovanessian, and M. G. Katze, J. Virol. 63:2244-2251,1989). In the present study we investigated the mechanisms bywhich P68 degradation occurred. To do this we used an in vitrodegradation assay which faithfully reproduced the in vivo events.Although viral gene expression was required for P68 degradation,the major poliovirus proteases, 2A and 3C, were found not tobe directly involved with P68 proteolysis. However, the proteaseresponsible for P68 degradation required divalent cations formaximal activity and probably has both an RNA and a proteincomponent since trypsin and ribonuclease abrogated the activity.Despite this requirement for divalent cations and RNA, activationof the kinase was not required for proteolysis since a catalyticallyinactive P68 was still degraded. Mapping of P68 protease-sensitivesites by using in vitro translated truncation and deletion mutantsrevealed that sites required for degradation resided in theamino terminus and colocalized to dsRNA-binding domains. Finally,we found that preincubation of cell extracts with the syntheticdsRNA poly(I-C) largely prevented P68 proteolysis, providingadditional evidence for the critical role of RNA. On the basisof these data, we present a hypothetical model depicting possiblemechanisms of P68 degradation in poliovirus-infected cells.

J Virol. 1993 February; 67(2): 791-800

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