Deep Transcriptional Sequencing of Mucosal Challenge Compartment from Rhesus Macaques Acutely Infected with Simian Immunodeficiency Virus Implicates Loss of Cell Adhesion Preceding Immune Activation

Barrenäs, Fredrik; Palermo, Robert E.; Agricola, Brian A.; Agy, Michael B.; Aicher, Lauri; Carter, Victoria; Flanary, Leon; Green, Richard; McLain, Randy; Li, Qingsheng; Lu, Weifang; Murnane, Robert D.; Peng, Xinxia; Thomas, Matthew; Weiss, Jeffrey M.; Anderson, David; Katze, Michael G.

doi:10.1128/jvi.00543-14

Cited by 9 publications

(10 citation statements)

References 55 publications

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“…Any loss of tight junction proteins (i.e., claudin-3), due to cell death or internalization via endocytosis in response to infection would be indicative of a loss of mucosal integrity [60]. In SIV-infected RMs, claudin-3 staining has been used to measure the breakdown in mucosal epithelium continuity, while expression of claudin-encoding genes (i.e., CLDN3) has been shown to be downregulated as early as 3 dpi [132], similar to experimentally-induced IBD [95]. Importantly, at no timepoint post SIVsab infection in AGMs, did we find increases in mucosal apoptosis, proliferation or loss of the mucosal epithelium integrity, in stark contrast with reduced mucosal epithelium integrity in chronically…”

Section: Plos Pathogensmentioning

confidence: 99%

African green monkeys avoid SIV disease progression by preventing intestinal dysfunction and maintaining mucosal barrier integrity

Raehtz

Barrenäs

et al. 2020

PLoS Pathog

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Unlike HIV infection, SIV infection is generally nonpathogenic in natural hosts, such as African green monkeys (AGMs), despite lifelong high viral replication. Lack of disease progression was reportedly based on the ability of SIV-infected AGMs to prevent gut dysfunction, avoiding microbial translocation and the associated systemic immune activation and chronic inflammation. Yet, the maintenance of gut integrity has never been documented, and the mechanism(s) by which gut integrity is preserved are unknown. We sought to investigate the early events of SIV infection in AGMs, specifically examining the impact of SIVsab infection on the gut mucosa. Twenty-nine adult male AGMs were intrarectally infected with SIV-sab92018 and serially sacrificed at well-defined stages of SIV infection, preramp-up (1-3 days post-infection (dpi)), ramp-up (4-6 dpi), peak viremia (9-12 dpi), and early chronic SIV infection (46-55 dpi), to assess the levels of immune activation, apoptosis, epithelial damage and microbial translocation in the GI tract and peripheral lymph nodes. Tissue viral loads, plasma cytokines and plasma markers of gut dysfunction were also measured

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Section: Plos Pathogensmentioning

confidence: 99%

African green monkeys avoid SIV disease progression by preventing intestinal dysfunction and maintaining mucosal barrier integrity

Raehtz

Barrenäs

et al. 2020

PLoS Pathog

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“…We also identified thousands of transcript sequences that are partially or completely ‘missing’ from current macaque genome assemblies ( 2 ). Many newly identified transcripts were differentially expressed during Ebola virus infection of cynomolgus macaques ( 2 ) or simian immunodeficiency virus infection of rhesus macaques ( 2 , 16 ).…”

Section: Additional Updatesmentioning

confidence: 99%

“…Also, because the rhesus macaque is a widely used as a model to study HIV/AIDS, we provide a centralized pointer to macaque RNA-seq datasets released by the NHP Functional Genomics Core recently established by NIAID ( http://nhp-fgc.org ). This includes publically released data such as an mRNA-seq dataset of macaque rectal samples from multiple baseline and SIV-infected animals ( 16 ).…”

Section: Additional Updatesmentioning

confidence: 99%

Tissue-specific transcriptome sequencing analysis expands the non-human primate reference transcriptome resource (NHPRTR)

Peng

Thierry‐Mieg

Thierry-Mieg

et al. 2014

Nucleic Acids Research

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The non-human primate reference transcriptome resource (NHPRTR, available online at http://nhprtr.org/) aims to generate comprehensive RNA-seq data from a wide variety of non-human primates (NHPs), from lemurs to hominids. In the 2012 Phase I of the NHPRTR project, 19 billion fragments or 3.8 terabases of transcriptome sequences were collected from pools of ∼20 tissues in 15 species and subspecies. Here we describe a major expansion of NHPRTR by adding 10.1 billion fragments of tissue-specific RNA-seq data. For this effort, we selected 11 of the original 15 NHP species and subspecies and constructed total RNA libraries for the same ∼15 tissues in each. The sequence quality is such that 88% of the reads align to human reference sequences, allowing us to compute the full list of expression abundance across all tissues for each species, using the reads mapped to human genes. This update also includes improved transcript annotations derived from RNA-seq data for rhesus and cynomolgus macaques, two of the most commonly used NHP models and additional RNA-seq data compiled from related projects. Together, these comprehensive reference transcriptomes from multiple primates serve as a valuable community resource for genome annotation, gene dynamics and comparative functional analysis.

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“…The three RNA-Seq and two DNA-Seq datasets to prove the mis-assembly of rheMac3 genome on subsection “Mis-assembly of rheMac3 genome leads to mis-annotations in RefSeq-rheMac3” are from NCBI SRA. The accession numbers for RNA-Seq datasets are SRX424026 [ 31 ], SRX209571 [ 32 ] and SRX518478 [ 33 ]; and the accession number for DNA-Seq datasets are SRX489030 [ 34 ], SRX480828 [ 34 ].…”

Section: Discussionmentioning

confidence: 99%

GASS: genome structural annotation for Eukaryotes based on species similarity

et al. 2015

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BackgroundWith the development of high-throughput sequencing techniques, more and more genomes were sequenced and assembled. However, annotating a genome’s structure rapidly and expressly remains challenging. Current eukaryotic genome annotations require various, abundant supporting data, such as: species-specific and cross-species protein sequences, ESTs, cDNA and RNA-Seq data. Collecting those data and merging their analytical results to achieve a consistent complete annotation is a complex, time and cost consuming task.ResultsIn our study, we proposed a fast and easy-to-use computational tool: GASS (Genome Annotation based on Species Similarity). It annotates a eukaryotic genome based on only the annotations from another similar species. With aligning the exons’ sequences of an annotated similar species to the un-annotated genome, GASS detects the optimal transcript annotations with a shortest-path model. In our study, GASS was used to achieve the rhesus annotations based on the human annotations. The produced annotations were evaluated by comparing them to the two existing rhesus annotation databases (RefSeq and Ensembl) directly and being aligned with three RNA-Seq data of rhesus. The experiment results showed that more than 65% RefSeq exons and splicing junctions were exactly found by GASS. GASS’s sensitivity was higher than RefSeq’s, and was close to Ensembl’s. GASS had higher specificities than Ensembl at gene, transcript, exon and splicing junction levels. We also found the mis-assemblies of rheMac3 genome, which led to the 2 bp shifts in annotating position on exons’ boundary and then the incomplete splicing canonical sites in Refseq annotations. These detections were further supported by various data sources.ConclusionsGASS quickly produces structural genome annotations in sufficient abundance and accuracy. With simple and rapid running of GASS, small labs can create quick views of genome annotations for an un-annotated species, without the necessity to create, collect, analyze and synthesize extra various data sources, or wait several months for the annotations from professional organizations. GASS can be applied to many study occasions, such as the analysis of RNA-Seq datasets from the unannotated species whose genome drafts are available but the annotations are not.Electronic supplementary materialThe online version of this article (doi:10.1186/s12864-015-1353-3) contains supplementary material, which is available to authorized users.

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Deep Transcriptional Sequencing of Mucosal Challenge Compartment from Rhesus Macaques Acutely Infected with Simian Immunodeficiency Virus Implicates Loss of Cell Adhesion Preceding Immune Activation

Cited by 9 publications

References 55 publications

African green monkeys avoid SIV disease progression by preventing intestinal dysfunction and maintaining mucosal barrier integrity

African green monkeys avoid SIV disease progression by preventing intestinal dysfunction and maintaining mucosal barrier integrity

Tissue-specific transcriptome sequencing analysis expands the non-human primate reference transcriptome resource (NHPRTR)

GASS: genome structural annotation for Eukaryotes based on species similarity

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