IP6K1 upregulates the formation of processing bodies by influencing protein-protein interactions on the mRNA cap

Shah, Akruti ; Bhandari, Rashna (2021) IP6K1 upregulates the formation of processing bodies by influencing protein-protein interactions on the mRNA cap Journal of Cell Science, 134 (24). ISSN 0021-9533

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Official URL: https://doi.org/10.1242/jcs.259117

Related URL: http://dx.doi.org/10.1242/jcs.259117

Abstract

Inositol hexakisphosphate kinase 1 (IP6K1) is a small molecule kinase that catalyzes the conversion of the inositol phosphate IP6 to 5-IP7. We show that IP6K1 acts independently of its catalytic activity to upregulate the formation of processing bodies (P-bodies), which are cytoplasmic ribonucleoprotein granules that store translationally repressed mRNA. IP6K1 does not localise to P-bodies, but instead binds to ribosomes, where it interacts with the mRNA decapping complex – the scaffold protein EDC4, activator proteins DCP1A/B, decapping enzyme DCP2 and RNA helicase DDX6. Along with its partner 4E-T, DDX6 is known to nucleate protein-protein interactions on the 5′ mRNA cap to facilitate P-body formation. IP6K1 binds the translation initiation complex eIF4F on the mRNA cap, augmenting the interaction of DDX6 with 4E-T (also known as EIF4ENIF1) and the cap-binding protein eIF4E. Cells with reduced IP6K1 show downregulated microRNA-mediated translational suppression and increased stability of DCP2-regulated transcripts. Our findings unveil IP6K1 as a novel facilitator of proteome remodelling on the mRNA cap, tipping the balance in favour of translational repression over initiation, thus leading to P-body assembly.

Item Type:Article
Source:Copyright of this article belongs to Company of Biologists Ltd.
Keywords:mRNA Decay; mRNA Metabolism; P-bodies; DDX6
ID Code:141733
Deposited On:22 Jan 2026 06:18
Last Modified:22 Jan 2026 06:18

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