PHOSPHONOFORMATE INHIBITS REVERSE-TRANSCRIPTASE

被引:68
作者
SUNDQUIST, B
OBERG, B
机构
[1] ASTRA LAKEMEDEL AB,S-15185 SODERTALJE,SWEDEN
[2] RES & DEV LABS,SODERTALJE,SWEDEN
关键词
D O I
10.1099/0022-1317-45-2-273
中图分类号
Q81 [生物工程学(生物技术)]; Q93 [微生物学];
学科分类号
071005 ; 0836 ; 090102 ; 100705 ;
摘要
The new antiviral substance phosphonoformate (PFS) has been tested in a cell-free system for its effect on reverse transcriptases from an avian retrovirus (avian myeloblastosis virus, AMV) and from mammalian retroviruses (Rauscher leukaemia virus, RMuLV; bovine leukaemia virus; baboon endogenous virus; simian sarcoma virus; visna virus). The observed inhibitory effect of PFA has been compared with that of a structurally related substance, phosphonoacetate (PAA). Phosphonoformate, at a concentration of 100μM, reduced the activities of all the above mentioned polymerases by 90% when (rA)(n).(dT)10 was used as a template/primer. The dose-response curves for AMV and RMuLV polymerases primed with (rA)(n).(dT)10 showed PFA to be a 1000-fold more active than PAA; the RMuLV polymerase activity was reduced to 50% after incubation with 0.7 μM-PFA and 0.7 mM-PAA, respectively. There was no difference in PFA inhibition of virus-associated and purified reverse transcriptase activity. Results with various synthetic templates showed that both the RNA- and the DNA-dependent polymerase activities of reverse transcriptase were inhibited by PFA. The endogenous polymerase activity of AMV was inhibited to 50% at 100 μM-PFA, while PAA had no effect. The PFA inhibition was dependent on whether Mg2+ or Nm2+ was used as divalent cation in the assay. Phosphonoformate arrested DNA synthesis immediately after being added to the assay system. The mechanism of inhibition of the AMV polymerase was non-competitive with respect to substrate and template and the apparent inhibition constants were 16 μM and 9μM, respectively.
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页码:273 / 281
页数:9
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