Summary information and primary citation
- PDB-id
-
4hor;
DSSR-derived features in text and
JSON formats; DNAproDB
- Class
- RNA binding protein-RNA
- Method
- X-ray (1.861 Å)
- Summary
- Crystal structure of full-length human ifit5 with
5`-triphosphate oligocytidine
- Reference
-
Abbas YM, Pichlmair A, Gorna MW, Superti-Furga G, Nagar B
(2013): "Structural
basis for viral 5'-PPP-RNA recognition by human IFIT
proteins." Nature, 494,
60-64. doi: 10.1038/nature11783.
- Abstract
- Interferon-induced proteins with tetratricopeptide
repeats (IFITs) are innate immune effector molecules that
are thought to confer antiviral defence through disruption
of protein-protein interactions in the host
translation-initiation machinery. However, it was recently
discovered that IFITs can directly recognize viral RNA
bearing a 5'-triphosphate group (PPP-RNA), which is a
molecular signature that distinguishes it from host RNA.
Here we report crystal structures of human IFIT5, its
complex with PPP-RNAs, and an amino-terminal fragment of
IFIT1. The structures reveal a new helical domain that
houses a positively charged cavity designed to specifically
engage only single-stranded PPP-RNA, thus distinguishing it
from the canonical cytosolic sensor of double-stranded
viral PPP-RNA, retinoic acid-inducible gene I (RIG-I, also
known as DDX58). Mutational analysis, proteolysis and
gel-shift assays reveal that PPP-RNA is bound in a
non-sequence-specific manner and requires a 5'-overhang of
approximately three nucleotides. Abrogation of PPP-RNA
binding in IFIT1 and IFIT5 was found to cause a defect in
the antiviral response by human embryonic kidney cells.
These results demonstrate the mechanism by which IFIT
proteins selectively recognize viral RNA, and lend insight
into their downstream effector function.
