Sequences within the poliovirus internal ribosome entry segment control viral RNA synthesis.

AM Borman, FG Deliat, KM Kean - The EMBO journal, 1994 - embopress.org
AM Borman, FG Deliat, KM Kean
The EMBO journal, 1994embopress.org
The 5′ untranslated region of poliovirus RNA has been reported to possess two functional
elements:(i) the 5′ proximal 88 nucleotides form a cloverleaf structure implicated in positive‐
strand RNA synthesis during viral replication, and (ii) nucleotides 134 to at least 556 function
as a highly structured internal ribosome entry segment (IRES) during cap‐independent,
internal initiation of translation. We show here that the IRES itself is bifunctional and contains
sequences necessary for viral RNA synthesis per se. For this purpose, we used a dicistronic …
The 5′ untranslated region of poliovirus RNA has been reported to possess two functional elements: (i) the 5′ proximal 88 nucleotides form a cloverleaf structure implicated in positive‐strand RNA synthesis during viral replication, and (ii) nucleotides 134 to at least 556 function as a highly structured internal ribosome entry segment (IRES) during cap‐independent, internal initiation of translation. We show here that the IRES itself is bifunctional and contains sequences necessary for viral RNA synthesis per se. For this purpose, we used a dicistronic poliovirus RNA in which the translation of the viral non‐structural (replication) proteins is uncoupled from the poliovirus IRES. In this system, RNA synthesis is readily detectable in transfected cells, even when the poliovirus IRES is inactivated by point mutation. However, deletion of the major part of the poliovirus IRES renders viral‐specific RNA synthesis undetectable. Using the same system, we show that a three nucleotide deletion at position 500 in the 5′ untranslated region drastically affects both translation efficiency and RNA synthesis. Furthermore, disruption of the secondary structure of the IRES around nucleotide 343 has minimal effects on IRES function, but dramatically reduces viral RNA replication. Taken together, these results provide direct evidence that sequences essential for viral RNA synthesis are located in the 3′ region of the poliovirus IRES.
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