A conserved nutrient responsive axis mediates autophagic degradation of miRNA–mRNA hybrids in blood cell progenitors

Author:

Ghosh Sushmit12ORCID,Chakraborti Sreemoyee12ORCID,Devi Devki12ORCID,Sahu Rajesh12ORCID,Mandal Sudip32ORCID,Mandal Lolitika12ORCID

Affiliation:

1. Developmental Genetic Laboratory , 140306 Punjab, India

2. Department of Biological Sciences, Indian Institute of Science Education and Research Mohali (IISER Mohali) , SAS Nagar, Knowledge City, Sector 81, Manauli P.O., 140306 Punjab , India

3. Molecular, Cell and Developmental Biology Laboratory ,140306 Punjab, India

Abstract

Abstract In animals, microRNAs are amongst the primary non-coding RNAs involved in regulating the gene expression of a cell. Most mRNAs in a cell are targeted by one or many miRNAs. Although several mechanisms can be attributed to the degradation of miRNA and mRNA within a cell, but the involvement of autophagy in the clearance of miRNA and its target mRNA is not known. We discover a leucine-responsive axis in blood cell progenitors that can mediate an autophagy-directed degradation of miRNA-bound mRNA in Drosophila melanogaster and Homo sapiens. This previously unknown miRNA clearance axis is activated upon amino acid deprivation that can traffic miRNA–mRNA-loaded Argonaute for autophagic degradation in a p62-dependent manner. Thus, our research not only reports a novel axis that can address the turnover of a catalytically active miRISC but also elucidates a slicer-independent mechanism through which autophagy can selectively initiate the clearance of target mRNA.

Funder

Council of Scientific and Industrial Research

KVPY Scholarship

DBT

SERB

DBT Wellcome-Trust India Alliance Senior Fellowship

DST-SERB Power

Indian Institute of Science Education and Research Mohali

Publisher

Oxford University Press (OUP)

Subject

Genetics

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