Transposable elements are associated with the variable response to influenza infection

Chen, X; Pacis, Alain; Aracena, Katherine A.; Gona, Saideep; Kwan, Tony; Groza, Cristian; Lin, Yen-Lung; Sindeaux, Renata H.M.; Yotova, Vania; Pramatarova, Albéna; Maguire, Simon; Pastinen, Tomi; Barreiro, Luis B.; Bourque, Guillaume

doi:10.1101/2022.05.10.491101

Cited by 7 publications

(5 citation statements)

References 65 publications

(88 reference statements)

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“…Notably, Chen et al. 37 found that SVA families are overrepresented in open chromatin in macrophages infected with influenza and are variable between individuals ( Figure S18 ). Consistent with this, the overwhelming majority of ATAC-seq peaks that lie on SVA polymorphisms were detected in the infected condition (92 of 108 peaks, 85.2%).…”

Section: Resultsmentioning

confidence: 99%

Genome graphs detect human polymorphisms in active epigenomic state during influenza infection

Groza¹,

Chen²,

Pacis³

et al. 2023

Cell Genomics

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Section: Resultsmentioning

confidence: 99%

Genome graphs detect human polymorphisms in active epigenomic state during influenza infection

Groza¹,

Chen²,

Pacis³

et al. 2023

Cell Genomics

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“…A similar trend is observed with TE biomarkers like MER48, and MER54A, suggesting these TEs are accessible in uninfected monocytes but transcriptionally dormant. This leads us to propose that such TEs may be primed to a “poised” state that might correlate to monocyte function [50]. Notably, several of these TEs, previously identified as “poised”, featured prominently among the upregulated TEs.…”

Section: Resultsmentioning

confidence: 99%

MATES: A Deep Learning-Based Model for Locus-specific Quantification of Transposable Elements in Single Cell

Wang,

Zheng,

Zhang

et al. 2024

Preprint

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Transposable elements (TEs) are crucial for genetic diversity and gene regulation. Current single-cell quantification methods often align multi-mapping reads to either `best-mapped' or `random-mapped' locations and categorize them at sub-family levels, overlooking the biological necessity for accurate, locus-specific TE quantification. Moreover, these existing methods are primarily designed for and focused on transcriptomics data, which restricts their adaptability to single-cell data of other modalities. To address these challenges, here we introduce MATES, a novel deep-learning approach that accurately allocates multi-mapping reads to specific loci of TEs, utilizing context from adjacent read alignments flanking the TE locus. When applied to diverse single-cell omics datasets, MATES shows improved performance over existing methods, enhancing the accuracy of TE quantification and aiding in the identification of marker TEs for identified cell populations. This development enables exploring single-cell heterogeneity and gene regulation through the lens of TEs, offering a transformative tool for the single-cell genomics community.

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“…Previous studies have characterized TE expression in response to infection with different viruses and found that infection-induced genome-wide TE expression often occurs in the vicinity of antiviral response genes (Chen et al ., 2023; Macchietto et al ., 2020). Thus, de-repression of TEs might have cis -acting consequences on regulating the expression of these antiviral response genes (Chuong et al , 2017).…”

Section: Discussionmentioning

confidence: 99%

“…Notably, IAV is not the only type of pathogen described to upregulate various host retroelements during infection (Young et al , 2014). Recently published re-analyses of publicly available gene expression datasets showed that infection with a diverse range of viruses can trigger changes in TE expression (Chen et al , 2023; Macchietto et al , 2020), indicating that the insights on molecular mechanisms leading to IAV-induced TE expression and sensing could be broadly applicable to other viruses.…”

Section: Introductionmentioning

confidence: 99%

Influenza A Virus NS1 Limits Recognition of Double-Stranded Transposable Elements by Cytosolic RNA Sensors

Lork,

Childs,

Lieber

et al. 2024

Preprint

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Influenza A virus (IAV) infection triggers de-repression of host transposable elements (TEs), which have the potential to form double-stranded (ds)RNAs and stimulate innate antiviral immunity. However, as wild-type IAV is generally a poor inducer of innate immunity, it remains unclear whether de-repressed TEs actually form dsRNAs recognizable by host cytosolic RNA sensors, or whether IAV might antagonize such sensing. Here, we performed strand-specific total RNA-Seq on nuclear and cytosolic fractions from cells infected with wild-type IAV or a recombinant IAV lacking NS1, a viral dsRNA-binding protein. Both infections led to global increases in host TE RNAs with bioinformatic and experimental evidence for double-strandedness. However, only NS1-deficient IAV infection led to significant amounts of TE-dsRNAs translocating to the cytosol, and co-precipitations identified that wild-type NS1 associates with TE-dsRNAs. Furthermore, a functional screen indicated that TE-dsRNAs can be engaged by various host cytosolic RNA sensors, including RIG-I, MDA5, ZBP1, and PKR. Our data reveal the double-stranded nature of infection-triggered host TEs and suggest an NS1-mediated sequestration mechanism to limit their cytosolic abundance and broad activation of diverse sensors.

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Transposable elements are associated with the variable response to influenza infection

Cited by 7 publications

References 65 publications

Genome graphs detect human polymorphisms in active epigenomic state during influenza infection

Genome graphs detect human polymorphisms in active epigenomic state during influenza infection

MATES: A Deep Learning-Based Model for Locus-specific Quantification of Transposable Elements in Single Cell

Influenza A Virus NS1 Limits Recognition of Double-Stranded Transposable Elements by Cytosolic RNA Sensors

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