A dynamic intron retention program enriched in RNA processing genes regulates gene expression during terminal erythropoiesis

Pimentel, Harold; Parra, Marilyn; Gee, Sherry L.; Mohandas, Narla; Pachter, Lior; Conboy, John G.

doi:10.1093/nar/gkv1168

Cited by 163 publications

(232 citation statements)

References 43 publications

(65 reference statements)

Supporting

Mentioning

212

Contrasting

Order By: Relevance

“…In 9980 of these samples with PTC containing IRs, we observed a higher negative correlation coefficient between change in IR and change in expression than that observed for the in-frame IRs (permutation test P = 0.002; Figure 2F). Together, these results suggest a role for IR in sex-biased expression, and are consistent with previous reports indicating that IR can negatively tune gene expression (BRAUNSCHWEIG et al 2014;DVINGE AND BRADLEY 2015;PIMENTEL et al 2016). Finally, GO analysis showed that genes with testis-biased IR were enriched in oogenesis, neurogenesis, female gamete generation, and others (Table S3, hypergeometric test P < 0.001).…”

Section: Introns That Are Differentially Retained In Ovary and Testissupporting

confidence: 91%

“…Intron retention (IR) is a type of AS event in which one or more introns are retained in the mRNA molecule. IR is the dominant AS type in Drosophila (GRAVELEY et al 2011) and affects about half of all introns in mammals (WONG et al 2013;BRAUNSCHWEIG et al 2014;EDWARDS et al 2016;PIMENTEL et al 2016). The "anomalous" mRNA generated by the retention of an intron may contain a premature termination codon (PTC) (JAILLON et al 2008), which can sometimes result in the degradation of the mRNA by the nonsense-mediated mRNA decay (NMD) pathway.…”

Section: Introductionmentioning

confidence: 99%

“…Because of this, mRNAs generated through IR events could be viewed as failures of the splicing process and void of biological function (JAILLON et al 2008;ROY AND IRIMIA 2008). However, recent studies suggested that IR events are involved in multiple cellular and physiological processes, including hematogenesis (WONG et al 2013;EDWARDS et al 2016;PIMENTEL et al 2016), T cell activation (NI et al 2016), neuronal differentiation (BRAUNSCHWEIG et al 2014), and carcinogenesis (DVINGE AND BRADLEY 2015;JUNG et al 2015). Despite these advances, questions remain regarding the extent to which introns are differentially retained between sexes and how sex-biased IR rates are regulated.…”

Section: Introductionmentioning

confidence: 99%

“…Introns fulfilling the following two criteria in any sample were regarded as IR events: first, the intron region was mapped with at least 10 reads (each read overlapped at least 6bps with the intron); second, the intron region had 100% coverage. To quantify IR rates, we used the metric Percent Intron Retention (PIR) as calculated in previous studies (BRAUNSCHWEIG et al 2014;PIMENTEL et al 2016) and briefly described here with minor modifications ( Figure 1A). For ease of description, suppose that the length of the target intron and the trimmed reads were L 1 and L 2 , respectively.…”

Section: Identification Of Ir Events and Calculation Of Intron Retentmentioning

confidence: 99%

“…We mapped reads to the reference Drosophila genome ( Figure 1A) and identified 21,664 IR events ( Figure 1B) in 7,546 genes. We used the metric Percent Intron Retention (PIR, see Methods) as previously implemented (BRAUNSCHWEIG et al 2014;PIMENTEL et al 2016) to represent the percentage of transcripts with the focal intron retained in each sample. From these IR events, 1,304 had been annotated in Flybase (i.e., both IR and intron splicing isoforms being annotated), while the other 20,360 were newly identified.…”

Section: Identifying Intron Retention Events In D Melanogastermentioning

confidence: 99%

See 4 more Smart Citations

The Y Chromosome Modulates Splicing and Sex-Biased Intron Retention Rates in Drosophila

Wang¹,

Branco²,

Lemos³

2018

Genetics

View full text Add to dashboard Cite

The Drosophila Y chromosome is a 40MB segment of mostly repetitive DNA; it harbors a handful of protein coding genes and a disproportionate amount of satellite repeats, transposable elements, and multicopy DNA arrays. Intron retention (IR) is a type of alternative splicing (AS) event by which one or more introns remain within the mature transcript. IR recently emerged as a deliberate cellular mechanism to modulate gene expression levels and has been implicated in multiple biological processes. However, the extent of sex differences in IR and the contribution of the Y chromosome to the modulation of alternative splicing and intron retention rates has not been addressed. Here we showed pervasive intron retention (IR) in the fruit fly Drosophila melanogaster with thousands of novel IR events, hundreds of which displayed extensive sex-bias.

show abstract

Section: Introns That Are Differentially Retained In Ovary and Testissupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Identification Of Ir Events and Calculation Of Intron Retentmentioning

confidence: 99%

Section: Identifying Intron Retention Events In D Melanogastermentioning

confidence: 99%

See 3 more Smart Citations

The Y Chromosome Modulates Splicing and Sex-Biased Intron Retention Rates in Drosophila

Wang¹,

Branco²,

Lemos³

2018

Genetics

View full text Add to dashboard Cite

show abstract

The Emerging Roles ofLIS1 Biomechanics in Cellular and Cortical Homeostasis

Kshirsagarand,

Reiner

2023

Neocortical Neurogenesis in Development and Evolution

View full text Add to dashboard Cite

LAFITE Reveals the Complexity of Transcript Isoforms in Subcellular Fractions

et al. 2022

View full text Add to dashboard Cite

Characterization of the subcellular distribution of RNA is essential for understanding the molecular basis of biological processes. Here, the subcellular nanopore direct RNA‐sequencing (DRS) of four lung cancer cell lines (A549, H1975, H358, and HCC4006) is performed, coupled with a computational pipeline, L ow‐abundance A ware F ull‐length I soform clus TE r (LAFITE), to comprehensively analyze the full‐length cytoplasmic and nuclear transcriptome. Using additional DRS and orthogonal data sets, it is shown that LAFITE outperforms current methods for detecting full‐length transcripts, particularly for low‐abundance isoforms that are usually overlooked due to poor read coverage. Experimental validation of six novel isoforms exclusively identified by LAFITE further confirms the reliability of this pipeline. By applying LAFITE to subcellular DRS data, the complexity of the nuclear transcriptome is revealed in terms of isoform diversity, 3'‐UTR usage, m6A modification patterns, and intron retention. Overall, LAFITE provides enhanced full‐length isoform identification and enables a high‐resolution view of the RNA landscape at the isoform level.

show abstract

A dynamic intron retention program enriched in RNA processing genes regulates gene expression during terminal erythropoiesis

Cited by 163 publications

References 43 publications

The Y Chromosome Modulates Splicing and Sex-Biased Intron Retention Rates in Drosophila

The Y Chromosome Modulates Splicing and Sex-Biased Intron Retention Rates in Drosophila

The Emerging Roles ofLIS1 Biomechanics in Cellular and Cortical Homeostasis

LAFITE Reveals the Complexity of Transcript Isoforms in Subcellular Fractions

Contact Info

Product

Resources

About