Impact of spliceosome mutations on RNA splicing in myelodysplasia: dysregulated genes/pathways and clinical associations

Pellagatti, Andrea; Armstrong, Richard N.; Steeples, Violetta; Sharma, Eshita; Repapi, Emmanouela; Singh, Shalini; Sanchi, Andrea; Radujkovic, Aleksandar; Horn, Patrick; Dolatshad, Hamid; Roy, S.; Broxholme, John; Lockstone, Helen; Taylor, Stephen; Giagounidis, Aristoteles; Vyas, Paresh; Schuh, Anna; Hamblin, Angela; Papaemmanuil, Elli; Killick, Sally; Malcovati, Luca; Hennrich, Marco L.; Gavin, Anne‐Claude; Ho, Anthony D.; Luft, Thomas; Hellström‐Lindberg, Eva; Cazzola, Mario; Smith, Christopher W.J.; Smith, S. K.; Boultwood, Jacqueline

doi:10.1182/blood-2018-04-843771

Cited by 185 publications

(253 citation statements)

References 105 publications

(134 reference statements)

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“…39 30 Liang et al also observed that the SRSF2 P95H mutation affected splicing of several members of the hnRNP and SR families of proteins. Importantly, EZH2 is located at chromosome 7q36, a region frequently deleted (−7 and 7q-) in MDS.…”

Section: Mis-spliced Events In Srsf2 Del and P95h Mutated Mdsmentioning

confidence: 98%

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Distinct and convergent consequences of splice factor mutations in myelodysplastic syndromes

Madan

Zhou

et al. 2019

American J Hematol

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Myelodysplastic syndromes (MDS) are characterized by recurrent somatic alterations often affecting components of RNA splicing machinery. Mutations of splice factors SF3B1, SRSF2, ZRSR2 and U2AF1 occur in >50% of MDS. To assess the impact of spliceosome mutations on splicing and to identify common pathways/genes affected by distinct mutations, we performed RNA-sequencing of MDS bone marrow samples harboring spliceosome mutations (including hotspot alterations of SF3B1, SRSF2 and

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Section: Mis-spliced Events In Srsf2 Del and P95h Mutated Mdsmentioning

confidence: 98%

“…30 More recently, splicing changes and transcriptional consequences of abnormal RNA splicing were also investigated in a large cohort of MDS samples. 30 More recently, splicing changes and transcriptional consequences of abnormal RNA splicing were also investigated in a large cohort of MDS samples.…”

Section: Mis-spliced Events In Srsf2 Del and P95h Mutated Mdsmentioning

confidence: 99%

Distinct and convergent consequences of splice factor mutations in myelodysplastic syndromes

Madan

Zhou

et al. 2019

American J Hematol

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“…In addition, the mechanistic basis of how splicing factor mutations confer selective advantage during the evolution of MDS pathogenesis remains a mystery. Although recent large‐scale transcriptomic analysis of mutations affecting SF3B1 , SRSF2 , and U2AF1 revealed global splicing dysregulation consistent with their predicted effects, there was minimal overlap between mis‐spliced transcripts altered by each of the mutant proteins . To identify key splicing abnormalities induced by mutant splicing factors, several studies provided functional evidence that expression of the abnormal splice isoforms in normal cells, or reintroduction of the canonical isoforms in spliceosomal mutant cells, can only partially phenocopy or rescue the effects of mutant spliceosome proteins .…”

Section: Effects Of Somatic Mutations In Splicing Factorsmentioning

confidence: 99%

“…These findings suggest that the pathological effects of spliceosome mutations are imparted through multiple mis‐spliced products simultaneously. In parallel, pathway analyses followed by functional validation revealed that splicing factor mutations distinctly converge on key cellular pathways to drive disease pathogenesis, including defects in DNA damage response and aberrant innate immune signaling . Further studies will be required to systematically address these fundamental questions, and more importantly, to identify the key players and pathways that can potentially be exploited for therapeutic purposes.…”

Section: Effects Of Somatic Mutations In Splicing Factorsmentioning

confidence: 99%

“…73 Although recent large-scale transcriptomic analysis of mutations affecting SF3B1, SRSF2, and U2AF1 revealed global splicing dysregulation consistent with their predicted effects, there was minimal overlap between mis-spliced transcripts altered by each of the mutant proteins. 93,94 To identify key splicing abnormalities induced by mutant splicing factors, several studies provided functional evidence that expression of the abnormal splice isoforms in normal cells, or reintroduction of the canonical isoforms in spliceosomal mutant cells, can only partially phenocopy or rescue the effects of mutant spliceosome proteins. 72,80,95,96 These findings suggest that the pathological effects of spliceosome mutations are imparted through multiple mis-spliced products simultaneously.…”

Section: Srsf2 Mutationsmentioning

confidence: 99%

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Mutations in spliceosome genes and therapeutic opportunities in myeloid malignancies

Taylor

Lee

2019

Genes Chromosomes & Cancer

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Since the discovery of RNA splicing more than 40 years ago, our comprehension of the molecular events orchestrating constitutive and alternative splicing has greatly improved. Dysregulation of pre‐mRNA splicing has been observed in many human diseases including neurodegenerative diseases and cancer. The recent identification of frequent somatic mutations in core components of the spliceosome in myeloid malignancies and functional analysis using model systems has advanced our knowledge of how splicing alterations contribute to disease pathogenesis. In this review, we summarize our current understanding on the mechanisms of how mutant splicing factors impact splicing and the resulting functional and pathophysiological consequences. We also review recent advances to develop novel therapeutic approaches targeting splicing catalysis and splicing regulatory proteins, and discuss emerging technologies using oligonucleotide‐based therapies to modulate pathogenically spliced isoforms.

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Reduced PLCG1 expression is associated with inferior survival for myelodysplastic syndromes

et al. 2019

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The PLCG1 gene, which encodes the phospholipase C γ1 isoform, is located within the commonly deleted region of the long arm of chromosome 20 (del(20q)) observed in myelodysplastic syndromes (MDS). Phospholipase C is involved in diverse physiological and pathological cellular processes through inositide signaling. We hypothesized that reduced PLCG1 expression because of haploinsufficiency by del(20q) plays a role in the molecular pathogenesis of MDS. Therefore, we analyzed PLCG1 expression in bone marrow mononuclear cells at diagnosis in 116 MDS patients with or without del(20q) by quantitative RT‐PCR to evaluate its clinical significance. The expression level of PLCG1 was significantly lower not only in MDS patients with del(20q) but also in those without del(20q) compared to that of the controls, which suggests that reduced PLCG1 expression is a common molecular event in MDS. Patients in the lowest quartile (Q4) group for PLCG1 expression had lower overall survival (OS) compared to that of other patients (Q1‐Q3) (log‐rank test, P = .0004) with estimated median OS times of 22 in the Q4 group and 106 months in the Q1‐3 group. Univariate and multivariate analysis indicated reduced PLCG1 expression (Q4) was associated with lower OS (hazard ratio 2.58, 95% CI 1.35‐4.84, P = .0049), which suggests that reduced PLCG1 expression is an independent prognostic factor for OS. In addition, patients were well‐stratified for OS by combining PLCG1 expression level (Q4 vs Q1‐3) and bone marrow blast percentage (5% or more vs less than 5%). Thus, the level of PLCG1 expression at time of diagnosis is a prognostic biomarker for MDS.

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Impact of spliceosome mutations on RNA splicing in myelodysplasia: dysregulated genes/pathways and clinical associations

Cited by 185 publications

References 105 publications

Distinct and convergent consequences of splice factor mutations in myelodysplastic syndromes

Distinct and convergent consequences of splice factor mutations in myelodysplastic syndromes

Mutations in spliceosome genes and therapeutic opportunities in myeloid malignancies

Reduced PLCG1 expression is associated with inferior survival for myelodysplastic syndromes

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