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Cellular mRNA recruits the ribosome via eIF3-PABP bridge to initiate internal translation.


ABSTRACT: IRES-mediated translation of key cell fate regulating genes has been implicated in tumorigenesis. Concerted action of canonical eukaryotic initiation factors and IRES transacting factors (ITAFs) was shown to regulate cellular IRES mediated translation; however, the precise molecular mechanism of ribosome recruitment to cellular IRESes remains unclear. Here we show that the X-linked inhibitor of apoptosis (XIAP) IRES operates in an evolutionary conserved viral like mode and the structural integrity, particularly in the vicinity of AUG, is critical for ribosome recruitment. The binding of eIF3 together with PABP potentiates ribosome recruitment to the IRES. Our data support the model in which eIF3 binds directly to the XIAP IRES RNA in a structure-dependent manner and acts as a scaffold for IRES RNA, PABP and the 40S ribosome.

SUBMITTER: Thakor N 

PROVIDER: S-EPMC5449081 | biostudies-other | 2017 May

REPOSITORIES: biostudies-other

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Cellular mRNA recruits the ribosome via eIF3-PABP bridge to initiate internal translation.

Thakor Nehal N   Smith M Duane MD   Roberts Luc L   Faye Mame Daro MD   Patel Harshil H   Wieden Hans-Joachim HJ   Cate Jamie H D JHD   Holcik Martin M  

RNA biology 20160201 5


IRES-mediated translation of key cell fate regulating genes has been implicated in tumorigenesis. Concerted action of canonical eukaryotic initiation factors and IRES transacting factors (ITAFs) was shown to regulate cellular IRES mediated translation; however, the precise molecular mechanism of ribosome recruitment to cellular IRESes remains unclear. Here we show that the X-linked inhibitor of apoptosis (XIAP) IRES operates in an evolutionary conserved viral like mode and the structural integri  ...[more]

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