hnRNP U protein is required for normal pre-mRNA splicing and postnatal heart development and function

Ye, Junqiang; Beetz, Nadine; O’Keeffe, Sean; Tapia, Juan Carlos; Macpherson, Lindsey J.; Chen, Weisheng V.; Bassel‐Duby, Rhonda; Olson, Eric N.; Maniatis, Tom

doi:10.1073/pnas.1508461112

Cited by 95 publications

(115 citation statements)

References 56 publications

(83 reference statements)

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“…To determine if individual transcripts were affected, we analyzed mRNA by next generation sequencing. At 24 hr following depletion, only SAF-A was differentially expressed compared to control cells, while at 48 hr, there were limited changes in cell-cycle-dependent genes (Figure S2D) consistent with other studies (Xiao et al., 2012, Ye et al., 2015). These results were validated by qRT-PCR (Figure 2D) providing overwhelming evidence that transcription is upstream of SAF-A (model 1).…”

Section: Resultsmentioning

confidence: 99%

SAF-A Regulates Interphase Chromosome Structure through Oligomerization with Chromatin-Associated RNAs

Nozawa

Boteva

Soares

et al. 2017

Cell

169

193

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SummaryHigher eukaryotic chromosomes are organized into topologically constrained functional domains; however, the molecular mechanisms required to sustain these complex interphase chromatin structures are unknown. A stable matrix underpinning nuclear organization was hypothesized, but the idea was abandoned as more dynamic models of chromatin behavior became prevalent. Here, we report that scaffold attachment factor A (SAF-A), originally identified as a structural nuclear protein, interacts with chromatin-associated RNAs (caRNAs) via its RGG domain to regulate human interphase chromatin structures in a transcription-dependent manner. Mechanistically, this is dependent on SAF-A’s AAA+ ATPase domain, which mediates cycles of protein oligomerization with caRNAs, in response to ATP binding and hydrolysis. SAF-A oligomerization decompacts large-scale chromatin structure while SAF-A loss or monomerization promotes aberrant chromosome folding and accumulation of genome damage. Our results show that SAF-A and caRNAs form a dynamic, transcriptionally responsive chromatin mesh that organizes large-scale chromosome structures and protects the genome from instability.

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Section: Resultsmentioning

confidence: 99%

SAF-A Regulates Interphase Chromosome Structure through Oligomerization with Chromatin-Associated RNAs

Nozawa

Boteva

Soares

et al. 2017

Cell

169

193

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“…5). hnRNPU has been implicated in many levels of gene regulation including transcription, RNA splicing, and DNA repair (34)(35)(36). Moreover, hnRNPU binds to both Xist RNA and the X chromosome and contributes to X-chromosome inactivation (24).…”

Section: Discussionmentioning

confidence: 99%

Long noncoding RNA #32 contributes to antiviral responses by controlling interferon-stimulated gene expression

Nishitsuji

Ujino

Yoshio

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Despite the breadth of knowledge that exists regarding the function of long noncoding RNAs (lncRNAs) in biological phenomena, the role of lncRNAs in host antiviral responses is poorly understood. Here, we report that lncRNA#32 is associated with type I IFN signaling. The silencing of lncRNA#32 dramatically reduced the level of IFN-stimulated gene (ISG) expression, resulting in sensitivity to encephalomyocarditis virus (EMCV) infection. In contrast, the ectopic expression of lncRNA#32 significantly suppressed EMCV replication, suggesting that lncRNA#32 positively regulates the host antiviral response. We further demonstrated the suppressive function of lncRNA#32 in hepatitis B virus and hepatitis C virus infection. lncRNA#32 bound to activating transcription factor 2 (ATF2) and regulated ISG expression. Our results reveal a role for lncRNA#32 in host antiviral responses.lncRNA | innate immunity | interferon | ISG

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“…61 Interestingly, like SRSF1, SRSF2, and SRFS10, hnRNP U is important for proper splicing of Ca 2+ handling genes such as CamkIIδ, suggesting that alternative splicing of Ca 2+ -handling genes is critical in early postnatal heart development.…”

Section: Splicing Factors In the Developing Heartmentioning

confidence: 99%

RNA Splicing

2016

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RNA splicing, a post-transcriptional process necessary to form a mature mRNA, was discovered in the late 1970s. 1 Two different modes of splicing have been defined, that is, constitutive splicing and alternative splicing. Constitutive splicing is the process of removing introns from the premRNA, and joining the exons together to form a mature mRNA. Alternative splicing, on the other hand, is the process where exons can be included or excluded in different combinations to create a diverse array of mRNA transcripts from a single pre-mRNA and therefore serves as a process to increase the diversity of the transcriptome. The estimated number of alternative splicing events in the human transcriptome has risen sharply over the past decades. In the 1980s, it was thought that about 5% of human genes were subjected to alternative splicing.2 In 2002, this number had risen to 60%, 3 and now, after implementation of next-generation-sequencing technologies, we know that the vast majority, >95% of mRNAs, are subjected to alternative splicing. 4 Nevertheless, the function of a large fraction of these splice isoforms remains to be elucidated. Furthermore, it is anticipated that in different tissues, or in tissues with different disease states, new isoforms still remain to be identified. 5The process of splicing is highly conserved during evolution. Splicing is more prevalent in multicellular than in unicellular eukaryotes because of the lower number of introncontaining genes in the latter. 6 Later in evolution, alternative splicing becomes more prevalent in vertebrates than in invertebrates. Interestingly, just a single exon-skipping event in the RNA-binding protein (RBP), polypyrimidine tract binding protein 1 has been shown to direct numerous alternative splicing changes between species, indicating that a single splicing event can amplify transcriptome diversity between species. 7The recent observation that the total number of protein-coding genes does not differ much between species, fueled the hypothesis that alternative splicing largely contributes to organism diversity. And indeed, as we move up the phylogenetic tree, alternative splicing complexity increases, with the highest complexity in primates. 8,9The aim of this review is to give a comprehensive overview of all aspects of constitutive and alternative splicing and their regulators, as well as the importance of these different aspects in human disease, with a focus on the heart. In addition, we discuss possible therapeutic interventions and try to uncover potential future directions of research. Major and Minor SpliceosomeRNA splicing is performed by the spliceosome, a large and dynamic ribonucleoprotein complex composed of proteins and small nuclear RNAs (snRNAs), which assembles on the pre-mRNA (Figure 1). Ribonucleoproteins consist of 1 or 2 small nuclear RNAs (snRNAs; U1, U2, U4/U6, or U5), and a variable number of complex-specific proteins.

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hnRNP U protein is required for normal pre-mRNA splicing and postnatal heart development and function

Cited by 95 publications

References 56 publications

SAF-A Regulates Interphase Chromosome Structure through Oligomerization with Chromatin-Associated RNAs

SAF-A Regulates Interphase Chromosome Structure through Oligomerization with Chromatin-Associated RNAs

Long noncoding RNA #32 contributes to antiviral responses by controlling interferon-stimulated gene expression

RNA Splicing

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