The mRNA-capping enzyme localizes to stress granules in the cytoplasm and maintains cap homeostasis of target mRNAs

Author:

Gayen Anakshi12ORCID,Mukherjee Avik1ORCID,Kumar Krishna3ORCID,Majumder Shubhra2ORCID,Chakrabarti Saikat3ORCID,Mukherjee Chandrama1ORCID

Affiliation:

1. Institute of Health Sciences, Presidency University 1 RNABio Lab , , Kolkata, West Bengal 700156 , India

2. Institute of Health Sciences, Presidency University 2 CellBio Lab , , Kolkata, West Bengal 700156 , India

3. Council for Scientific and Industrial Research (CSIR) - Indian Institute of Chemical Biology (IICB) 3 Structural Biology and Bioinformatics Division , , Kolkata, West Bengal 700091 , India

Abstract

ABSTRACT The model of RNA stability has undergone a transformative shift with the revelation of a cytoplasmic capping activity that means a subset of transcripts are recapped autonomously of their nuclear counterparts. The present study demonstrates nucleo-cytoplasmic shuttling of the mRNA-capping enzyme (CE, also known as RNA guanylyltransferase and 5′-phosphatase; RNGTT), traditionally acknowledged for its nuclear localization and functions, elucidating its contribution to cytoplasmic capping activities. A unique nuclear export sequence in CE mediates XPO1-dependent nuclear export of CE. Notably, during sodium arsenite-induced oxidative stress, cytoplasmic CE (cCE) congregates within stress granules (SGs). Through an integrated approach involving molecular docking and subsequent co-immunoprecipitation, we identify eIF3b, a constituent of SGs, as an interactive associate of CE, implying that it has a potential role in guiding cCE to SGs. We measured the cap status of specific mRNA transcripts from U2OS cells that were non-stressed, stressed and recovered from stress, which indicated that cCE-target transcripts lost their caps during stress but remarkably regained cap stability during the recovery phase. This comprehensive study thus uncovers a novel facet of cytoplasmic CE, which facilitates cellular recovery from stress by maintaining cap homeostasis of target mRNAs.

Funder

Department of Biotechnology, Ministry of Science and Technology

Science and Engineering Research Board

Department of Science & Technology and Biotechnology, Government of West Bengal

Publisher

The Company of Biologists

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1. First person – Anakshi Gayen and Avik Mukherjee;Journal of Cell Science;2024-06-01

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