Intron retention-induced neoantigen load correlates with unfavorable prognosis in multiple myeloma

Dong, Chuanpeng; Cesarano, Annamaria; Bombaci, Giuseppe; Reiter, Jill L.; Yu, Christina Y.; Wang, Yue; Jiang, Zhaoyang; Zaid, Mohammad Abu; Huang, Kun; Lu, Xiongbin; Walker, Brian A; Perna, Fabiana; Liu, Yunlong

doi:10.1038/s41388-021-02005-y

Cited by 22 publications

(22 citation statements)

References 66 publications

(74 reference statements)

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“…Type 1 diabetes is an evolving field of interest where splicing alterations can unveil novel immunogenic epitopes (Wu et al, 2021). In addition, IR is a frequent event in many cancer types, and our recent studies have shown that IR-induced neoantigens may be a useful biomarker for predicting survival in multiple myeloma and pancreatic cancer patients (Dong et al, 2021(Dong et al, , 2022.…”

Section: Discussionmentioning

confidence: 99%

Bioinformatics detection of modulators controlling splicing factor‐dependent intron retention in the human brain

et al. 2022

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Alternative RNA splicing is an important means of genetic control and transcriptome diversity. However, when alternative splicing events are studied independently, coordinated splicing modulated by common factors is often not recognized. As a result, the molecular mechanisms of how splicing regulators promote or repress splice site recognition in a context-dependent manner are not well understood. The functional coupling between multiple gene regulatory layers suggests that splicing is modulated by additional genetic or epigenetic components. Here, we developed a bioinformatics approach to identify causal modulators of splicing activity based on the variation of gene expression in large RNA sequencing datasets. We applied this approach in a neurological context with hundreds of dorsolateral prefrontal cortex samples. Our model is strengthened with the incorporation of genetic variants to impute gene expression in a Mendelian randomization-based approach. We identified novel modulators of the splicing factor SRSF1, including UIMC1 and the long noncoding RNA CBR3-AS1, that function over dozens of SRSF1 intron retention splicing targets. This strategy can be widely used to identify modulators of RNAbinding proteins involved in tissue-specific alternative splicing.

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Section: Discussionmentioning

confidence: 99%

Bioinformatics detection of modulators controlling splicing factor‐dependent intron retention in the human brain

et al. 2022

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“…Recently, recurrent stop codon mutations leading to readthrough into 3’ UTRs have been detected in over 400 cancer-related genes (Dhamija et al, 2020). Further supporting elevated noncanonical ORF translation in cancer, peptides derived from noncoding regions account for the majority of tumor-specific antigens (Laumont et al, 2018; Smart et al, 2018; Xiang et al, 2021), and tend to be associated with unfavorable prognoses for patients (Dong et al, 2021). Similarly, increased intron retention and other aberrant splicing events are associated with aging and neurodegeneration (Adusumalli et al, 2019; Hsieh et al, 2019; Mariotti et al, 2022; Mazin et al, 2013).…”

Section: Introductionmentioning

confidence: 98%

A unified model for the surveillance of translation in diverse noncoding sequences

Kesner

Chen

Aparicio

et al. 2022

Preprint

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Translation is pervasive outside of canonical coding regions, occurring in lncRNAs, UTRs, and introns. While the resulting polypeptides are often non-functional, translation in noncoding regions is nonetheless necessary for the birth of new coding regions. The mechanisms underlying the surveillance of translation in diverse noncoding regions and how escaped polypeptides evolve new functions remain unclear. Intriguingly, noncoding sequence-derived functional peptides often localize to membranes. Here, we show that the intrinsic nucleotide bias in the noncoding genome and in the genetic code frequently results in polypeptides with a hydrophobic C-terminal tail, which is captured by the ribosome-associated BAG6 membrane protein triage complex for either proteasomal degradation or membrane targeting. In contrast, canonical proteins have evolved to deplete C-terminal hydrophobic residues. Our results uncovered a fail-safe mechanism for the surveillance of unwanted translation from diverse noncoding regions and suggest a possible biochemical route for the preferential membrane localization of newly evolved proteins.HighlightsTranslation in diverse noncoding regions is mitigated by proteasomal degradationC-terminal hydrophobicity is a hallmark of noncoding sequence derived polypeptidesA genome-wide CRISPR screen identified the BAG6 membrane protein triage pathwayRibosome-associated BAG6 complex targets C-terminal hydrophobicity for degradation

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“…While an improvement, our intron persistence metric only partially accounts for admixed splicing patterns from different cell types in a mixed-cell sample such as HX1. Like other RI detection studies [15–17, 25, 31, 34, 43], our approach is explicitly linked to annotation (here, GENCODE v35) and therefore reports IR only relative to annotated transcripts, ignoring potential unannotated transcripts. We also did not explore the entanglement of biological and technical effects in the length of persistent introns: shorter introns are more likely to be retained [43, 55, 56], but the length limit of PacBio Iso-Seq reads of up to 10 kilobases means that any molecules with longer persistent introns were not considered in this study.…”

Section: Discussionmentioning

confidence: 99%

Retained introns in long RNA-seq reads are not reliably detected in sample-matched short reads

David

Maden

Wood

et al. 2022

Preprint

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There is growing interest in retained introns in a variety of disease contexts including cancer and aging. Many software tools have been developed to detect retained introns from short RNA-seq reads, but reliable detection is complicated by overlapping genes and transcripts as well as the presence of unprocessed or partially processed RNAs. We compared introns detected by 5 tools using short RNA-seq reads with introns observed in long RNA-seq reads from the same biological specimens and found: (1) significant disagreement among tools (Fleiss' κ = 0.231) such that 52.4% of all detected intron retentions were not called by more than one tool; (2) that no tool achieved greater than 20% precision or 35% recall under generous conditions; and (3) that retained intron detectability was adversely affected by greater intron length and overlap with annotated exons.

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Intron retention-induced neoantigen load correlates with unfavorable prognosis in multiple myeloma

Cited by 22 publications

References 66 publications

Bioinformatics detection of modulators controlling splicing factor‐dependent intron retention in the human brain

Bioinformatics detection of modulators controlling splicing factor‐dependent intron retention in the human brain

A unified model for the surveillance of translation in diverse noncoding sequences

Retained introns in long RNA-seq reads are not reliably detected in sample-matched short reads

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