Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs

Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs

Viral infection leads to a robust cellular response whereby the infected cell produces hundreds of molecular regulators to combat infection. Currently, non-canonical components, e.g., long noncoding RNAs (lncRNAs) have been added to the repertoire of immune regulators involved in the antiviral progr...

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Main Authors: Brandon S. Razooky, Benedikt Obermayer, Joshua Biggs O’May, Alexander Tarakhovsky
Format: Article
Language:English
Published: MDPI AG 2017-08-01
Series:Genes
Subjects:
small open reading frames
micropeptides
ribosome profiling
viral infection
Online Access:https://www.mdpi.com/2073-4425/8/8/206
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spelling doaj-d4489686b8cc4df6a457e5cb3a3d96092020-11-25T02:28:58ZengMDPI AGGenes2073-44252017-08-018820610.3390/genes8080206genes8080206Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAsBrandon S. Razooky0Benedikt Obermayer1Joshua Biggs O’May2Alexander Tarakhovsky3Laboratory of Immune Cell Epigenetics and Signaling, The Rockefeller University, New York, NY 10065, USABerlin Institute for Medical Systems Biology, Max Delbrück Center for Molecular Medicine, 13125 Berlin, GermanyLaboratory of Immune Cell Epigenetics and Signaling, The Rockefeller University, New York, NY 10065, USALaboratory of Virology and Infectious Diseases, The Rockefeller University, New York, NY 10065, USAViral infection leads to a robust cellular response whereby the infected cell produces hundreds of molecular regulators to combat infection. Currently, non-canonical components, e.g., long noncoding RNAs (lncRNAs) have been added to the repertoire of immune regulators involved in the antiviral program. Interestingly, studies utilizing next-generation sequencing technologies show that a subset of the >10,000 lncRNAs in the mammalian genome contain small open reading frames (smORFs) associated with active translation, i.e., many lncRNAs are not noncoding. Here, we use genome-wide high-throughput methods to identify potential micropeptides in smORF-containing lncRNAs involved in the immune response. Using influenza as a viral infection model, we performed RNA-seq and ribosome profiling to track expression and translation of putative lncRNAs that may encode for peptides and identify tens of potential candidates. Interestingly, many of these peptides are highly conserved at the protein level, strongly suggesting biological relevance and activity. By perusing publicly available data sets, four potential peptides of interest seem common to stress induction and/or are highly conserved; potential peptides from the MMP24-AS1, ZFAS1, RP11-622K12.1, and MIR22HG genes. Interestingly, using an antibody against the potential peptide encoded by MIR22HG RNA, we show that the peptide is stably expressed in the absence of infection, and upregulated in response to infection, corroborating the prediction of the ribosome profiling results. These data show the utility of perturbation approaches in identifying potentially relevant novel molecules encoded in the genome.https://www.mdpi.com/2073-4425/8/8/206small open reading framesmicropeptidesribosome profilingviral infection
collection DOAJ
language English
format Article
sources DOAJ
author Brandon S. Razooky
Benedikt Obermayer
Joshua Biggs O’May
Alexander Tarakhovsky
spellingShingle Brandon S. Razooky
Benedikt Obermayer
Joshua Biggs O’May
Alexander Tarakhovsky
Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs
Genes
small open reading frames
micropeptides
ribosome profiling
viral infection
author_facet Brandon S. Razooky
Benedikt Obermayer
Joshua Biggs O’May
Alexander Tarakhovsky
author_sort Brandon S. Razooky
title Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs
title_short Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs
title_full Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs
title_fullStr Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs
title_full_unstemmed Viral Infection Identifies Micropeptides Differentially Regulated in smORF-Containing lncRNAs
title_sort viral infection identifies micropeptides differentially regulated in smorf-containing lncrnas
publisher MDPI AG
series Genes
issn 2073-4425
publishDate 2017-08-01
description Viral infection leads to a robust cellular response whereby the infected cell produces hundreds of molecular regulators to combat infection. Currently, non-canonical components, e.g., long noncoding RNAs (lncRNAs) have been added to the repertoire of immune regulators involved in the antiviral program. Interestingly, studies utilizing next-generation sequencing technologies show that a subset of the >10,000 lncRNAs in the mammalian genome contain small open reading frames (smORFs) associated with active translation, i.e., many lncRNAs are not noncoding. Here, we use genome-wide high-throughput methods to identify potential micropeptides in smORF-containing lncRNAs involved in the immune response. Using influenza as a viral infection model, we performed RNA-seq and ribosome profiling to track expression and translation of putative lncRNAs that may encode for peptides and identify tens of potential candidates. Interestingly, many of these peptides are highly conserved at the protein level, strongly suggesting biological relevance and activity. By perusing publicly available data sets, four potential peptides of interest seem common to stress induction and/or are highly conserved; potential peptides from the MMP24-AS1, ZFAS1, RP11-622K12.1, and MIR22HG genes. Interestingly, using an antibody against the potential peptide encoded by MIR22HG RNA, we show that the peptide is stably expressed in the absence of infection, and upregulated in response to infection, corroborating the prediction of the ribosome profiling results. These data show the utility of perturbation approaches in identifying potentially relevant novel molecules encoded in the genome.
topic small open reading frames
micropeptides
ribosome profiling
viral infection
url https://www.mdpi.com/2073-4425/8/8/206
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