Your search keyword '"Kazuhiro Fukumura"' showing total 18 results

1. RNPS1 in PSAP complex controls periodic pre-mRNA splicing over the cell cycle

Author

Kazuhiro Fukumura, Akio Masuda, Jun-ichi Takeda, Osfamu Nagano, Hideyuki Saya, Kinji Ohno, and Akila Mayeda

Subjects

Cell biology, Cellular physiology, Molecular biology, Properties of biomolecules, Science

Abstract

Summary: Cell cycle progression requires periodic gene expression through splicing control. However, the splicing factor that directly controls this cell cycle-dependent splicing remains unknown. Cell cycle-dependent expression of the AURKB (aurora kinase B) gene is essential for chromosome segregation and cytokinesis. We previously reported that RNPS1 is essential to maintain precise splicing in AURKB intron 5. Here we show that RNPS1 plays this role in PSAP complex with PNN and SAP18, but not ASAP complex with ACIN1 and SAP18. Whole-transcriptome sequencing of RNPS1- and PNN-deficient cells indicated that RNPS1, either alone or as PSAP complex, is an essential splicing factor for a subset of introns. Remarkably, protein expression of RNPS1, but not PNN, is coordinated with cyclical splicing in PSAP-controlled introns including AURKB intron 5. The ubiquitin-proteasome pathway is involved in the periodic decrease of RNPS1 protein level. RNPS1 is a key factor that controls periodic splicing during the cell cycle.

Published

2024

2. SPF45/RBM17-dependent, but not U2AF-dependent, splicing in a distinct subset of human short introns

Author

Kazuhiro Fukumura, Rei Yoshimoto, Luca Sperotto, Hyun-Seo Kang, Tetsuro Hirose, Kunio Inoue, Michael Sattler, and Akila Mayeda

Subjects

Science

Abstract

The length distribution of human pre-mRNA introns is very extensive. The authors demonstrate that splicing in a subset of short introns is dependent on SPF45 (RBM17), which replaces authentic U2AF-heterodimer on the truncated poly-pyrimidine tracts and interacts with the U2 snRNP protein SF3b155.

Published

2021

3. SPF45/RBM17-dependent splicing and multidrug resistance to cancer chemotherapy

Author

Kazuhiro Fukumura, Julian P. Venables, and Akila Mayeda

Subjects

pre-mrna splicing, short intron, spf45 (rbm17), u2af heterodimer, anticancer drug resistance, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The early splicing complex A occupies at least eighty nucleotides of intron, in which U2AF covers the polypyrimidine tract. SPF45 (RBM17) functionally substitutes for U2AF on a subset of short introns. Since SPF45 expression confers resistance to various anticancer drugs, SPF45-dependent splicing may play a critical role in multidrug resistance.

Published

2021

4. RBM17 expression is associated with the efficacy of immune checkpoint inhibitor monotherapy in non-small cell lung cancer with low PD-L1 expression

Author

Hiroaki Nagamine, Masakazu Yashiro, Naoki Yoshimoto, Motohiro Izumi, Akira Sugimoto, Kenji Nakahama, Koichi Ogawa, Yoshiya Matsumoto, Kenji Sawa, Yoko Tani, Hiroyasu Kaneda, Shigeki Mitsuoka, Kazuhiro Yamada, Tetsuya Watanabe, Kazuhisa Aasai, Kazuhiro Fukumura, Akila Mayeda, and Tomoya Kawaguchi

Abstract

Immune checkpoint inhibitors (ICIs) are currently a standard treatment tool for non-small cell lung cancer (NSCLC). RNA-binding motif protein 17 (RBM17), a splicing factor,is frequently overexpressed in NSCLC, but little is known about the role of RBM17 in the efficacy of ICIs for NSCLC. Thus, we investigated the correlations between RBM17 expression and ICI efficacy in NSCLC. We collected biopsy or surgical specimens from patients with advanced or recurrent NSCLC who received ICI monotherapy or chemo-immunotherapy in a first-line setting. RBM17 expression was examined by immunohistochemistry. We evaluated the correlation between the efficacy of ICI monotherapy or chemo-immunotherapy and RBM17 expression. Among the 218 cases, 115 (52.8%) cases were positive for RBM17 expression. RBM17 expression was not associated with the objective response rate (ORR) or progression-free survival (PFS) in either of the ICI monotherapy or chemo-immunotherapy groups. However, among those with a low PD-L1 expression level (PD-L1 < 50%; n = 86), RBM17 expression was significantly associated with a better ORR (p = 0.045) and a better PFS (p < 0.001) in the ICI monotherapy group, and was significantly associated with a poor ORR in the chemo-immunotherapy group (p = 0.041). In conclusion, RBM17 might be a useful predictive marker for a higher efficacy of ICI monotherapy in NSCLC patients with a low PD-L1 expression level.

Published

2023

5. Novel LAMC2 fusion protein has tumor‐promoting properties in ovarian carcinoma

Author

Hisamori Kato, Kazuhiro Fukumura, Naohiko Koshikawa, Akila Mayeda, Yohei Miyagi, Motoharu Seiki, and Hoshino Daisuke

Subjects

Cancer Research, Oncogene Proteins, Fusion, extracellular matrix, Cell, Mice, Nude, Chromosomal translocation, laminin‐γ2, Extracellular matrix, Fusion gene, Cell, Molecular, and Stem Cell Biology, Ovarian carcinoma, Cell Line, Tumor, Nuclear Receptor Subfamily 6, Group A, Member 1, medicine, Animals, Humans, Ovarian Neoplasms, Mice, Inbred BALB C, Cocarcinogenesis, Chemistry, Cancer, General Medicine, Original Articles, medicine.disease, Fusion protein, Xenograft Model Antitumor Assays, Cell biology, ovarian carcinoma, Gene Expression Regulation, Neoplastic, Protein Subunits, medicine.anatomical_structure, Oncology, fusion gene, Original Article, Female, RNA Interference, Laminin, Ovarian cancer

Abstract

Laminins are heterotrimeric ECM proteins composed of α, β, and γ chains. The γ2 chain (Lm‐γ2) is a frequently expressed monomer and its expression is closely associated with cancer progression. Laminin‐γ2 contains an epidermal growth factor (EGF)‐like domain in its domain III (DIII or LEb). Matrix metalloproteinases can cleave off the DIII region of Lm‐γ2 that retains the ligand activity for EGF receptor (EGFR). Herein, we show that a novel short form of Lm‐γ2 (Lm‐γ2F) containing DIII is generated without requiring MMPs and chromosomal translocation between LAMC2 on chromosome 1 and NR6A1 gene locus on chromosome 9 in human ovarian cancer SKOV3 cells. Laminin‐γ2F is expressed as a truncated form lacking domains I and II, which are essential for its association with Lm‐α3 and ‐β3 chains of Lm‐332. Secreted Lm‐γ2F can act as an EGFR ligand activating the EGFR/AKT pathways more effectively than does the Lm‐γ2 chain, which in turn promotes proliferation, survival, and motility of ovarian cancer cells. LAMC2‐NR6A1 translocation was detected using in situ hybridization, and fusion transcripts were expressed in ovarian cancer cell tissues. Overexpression and suppression of fusion transcripts significantly increased and decreased the tumorigenic growth of cells in mouse models, respectively. To the best of our knowledge, this is the first report regarding a fusion gene of ECM showing that translocation of LAMC2 plays a crucial role in the malignant growth and progression of ovarian cancer cells and that the consequent product is a promising therapeutic target against ovarian cancers., Expression of LAMC2‐NR6A1 fusion transcripts in human ovarian carcinomas.

Published

2021

6. SAP30BP interacts with RBM17/SPF45 to promote splicing in a subset of human short introns

Author

Kazuhiro Fukumura, Luca Sperotto, Stefanie Seuß, Hyun-Seo Kang, Rei Yoshimoto, Michael Sattler, and Akila Mayeda

Abstract

SUMMARYHuman pre-mRNA splicing requires the removal of introns with highly variable lengths, from tens to over a million nucleotides. Therefore, mechanisms of intron recognition and splicing are likely not universal. Recently, we reported that splicing in a subset of human short introns with truncated polypyrimidine tracts depends on RBM17 (SPF45), instead of the canonical splicing factor U2AF heterodimer. Here, we demonstrate that SAP30BP, a factor previously implicated in transcriptional control, is an essential splicing cofactor for RBM17.In vitrobinding and NMR analyses demonstrate that a U2AF-homology motif (UHM) in RBM17 binds directly to a newly identified UHM-ligand motif (ULM) in SAP30BP. We show that this RBM17–SAP30BP interaction is required to specifically recruit RBM17 to phosphorylated SF3B1 (SF3b155), a U2 snRNP component in active spliceosomes. We propose a unique mechanism for splicing in a subset of short introns, in which SAP30BP guides RBM17 in the assembly of active spliceosomes.

Published

2022

7. SPF45/RBM17-dependent splicing and multidrug resistance to cancer chemotherapy

Author

Akila Mayeda, Julian P. Venables, and Kazuhiro Fukumura

Subjects

Multiple drug resistance, Cancer Research, Cancer chemotherapy, RNA splicing, Cancer research, Author’s Views, Molecular Medicine, Biology

Abstract

The early splicing complex A occupies at least eighty nucleotides of intron, in which U2AF covers the polypyrimidine tract. SPF45 (RBM17) functionally substitutes for U2AF on a subset of short introns. Since SPF45 expression confers resistance to various anticancer drugs, SPF45-dependent splicing may play a critical role in multidrug resistance.

Published

2022

8. Rbm38 Reduces the Transcription Elongation Defect of the SMEK2 Gene Caused by Splicing Deficiency

Author

Shintaro Muraoka, Akila Mayeda, Megumi Hayashi, Kazuhiro Fukumura, Naoyuki Kataoka, and Daisuke Kaida

Subjects

Transcription elongation, RNA Splicing, Rbm38, RNA-binding protein, Biology, Catalysis, Article, Inorganic Chemistry, Transcriptome, lcsh:Chemistry, Phosphoprotein Phosphatases, RNA Precursors, Humans, RNA, Messenger, Physical and Theoretical Chemistry, transcription elongation, Molecular Biology, Gene, lcsh:QH301-705.5, Spectroscopy, Messenger RNA, Binding Sites, Organic Chemistry, RNA-Binding Proteins, General Medicine, Computer Science Applications, Cell biology, HEK293 Cells, lcsh:Biology (General), lcsh:QD1-999, spliceostatin A, RNA splicing, Mutation, pre-mRNA splicing, Molecular mechanism, Pre-mRNA splicing, RNA-Binding Motifs, HeLa Cells, Protein Binding

Abstract

Pre-mRNA splicing is an essential mechanism for ensuring integrity of the transcriptome in eukaryotes. Therefore, splicing deficiency might cause a decrease in functional proteins and the production of nonfunctional, aberrant proteins. To prevent the production of such aberrant proteins, eukaryotic cells have several mRNA quality control mechanisms. In addition to the known mechanisms, we previously found that transcription elongation is attenuated to prevent the accumulation of pre-mRNA under splicing-deficient conditions. However, the detailed molecular mechanism behind the defect in transcription elongation remains unknown. Here, we showed that the RNA binding protein Rbm38 reduced the transcription elongation defect of the SMEK2 gene caused by splicing deficiency. This reduction was shown to require the N- and C-terminal regions of Rbm38, along with an important role being played by the RNA-recognition motif of Rbm38. These findings advance our understanding of the molecular mechanism of the transcription elongation defect caused by splicing deficiency.

Published

2020

9. SPF45/RBM17-dependent, but not U2AF-dependent, splicing in human short introns

Author

Hyun-Seo Kang, Michael Sattler, Kazuhiro Fukumura, Luca Sperotto, Kunio Inoue, Tetsuro Hirose, Rei Yoshimoto, and Akila Mayeda

Subjects

Splicing factor, Alternative splicing, RNA splicing, Regulator, Intron, snRNP, splice, Computational biology, Biology, Nuclear protein

Abstract

Human pre-mRNA introns vary in size from under fifty to over a million nucleotides. We searched for essential factors specifically involved in the splicing of human short introns by screening siRNAs against 154 human nuclear proteins for activity on a model short 56-nucleotide intron-containing HNRNPH1 pre-mRNA. We identified a known alternative splicing regulator SPF45 (RBM17) as a general splicing factor that is essential to splice out this 56-nt intron. Whole-transcriptome sequencing of SPF45-deficient cells revealed that SPF45 is specifically required for the efficient splicing of many short introns. Our crosslinking and biochemical analyses demonstrate that SPF45 specifically replaces the U2AF heterodimer on the truncated poly-pyrimidine tracts in these short intron. To initiate splicing, the U2AF-homology motif (UHM) of the replaced SPF45 interacts with the UHM-ligand motif (ULM) of the U2 snRNP protein SF3b155 (SF3B1). We propose that splicing in a distinct subset of human short introns depends on SPF45 but not U2AF heterodimer.

Published

2020

10. Splicing activator RNPS1 suppresses errors in pre-mRNA splicing: A key factor for mRNA quality control

Author

Kunio Inoue, Kazuhiro Fukumura, and Akila Mayeda

Subjects

Quality Control, 0301 basic medicine, RNA Splicing, Biophysics, Biology, Biochemistry, 03 medical and health sciences, Exon, RNA Precursors, Aurora Kinase B, Humans, RNA, Messenger, Genes, Suppressor, Molecular Biology, Messenger RNA, Gene knockdown, Alternative splicing, Intron, Cell Biology, Cell biology, 030104 developmental biology, Ribonucleoproteins, RNA splicing, Exon junction complex, Ectopic expression, HeLa Cells

Abstract

Human RNPS1 protein was first identified as a pre-mRNA splicing activator in vitro and RNPS1 regulates alternative splicing in cellulo. RNPS1 was also known as a peripheral factor of the exon junction complex (EJC). Here we show that cellular knockdown of RNPS1 induced a reduction of the wild-type aurora kinase B (AURKB) protein due to the induced aberrant pre-mRNA splicing events, indicating that the fidelity of AURKB pre-mRNA splicing was reduced. The major aberrant AURKB mRNA was derived from the upstream pseudo 5' and 3' splice sites in intron 5, which resulted in the production of the non-functional truncated AURKB protein. AURKB, is an essential mitotic factor, whose absence is known to cause multiple nuclei, and this multinucleation phenotype was recapitulated in RNPS1-knockdown cells. Importantly this RNPS1-knockdown phenotype was rescued by ectopic expression of AURKB, implying it is a major functional target of RNPS1. We found RNPS1 protein, not as a component of the EJC, binds directly to a specific element in the AURKB exon upstream of the authentic 5' splice site, and this binding is required for normal splicing. RNPS1-knockdown induces a parallel aberrant splicing pattern in a fully distinct pre-mRNA, MDM2, suggesting that RNPS1 is a global guardian of splicing fidelity. We conclude that RNPS1 is a key factor for the quality control of mRNAs that is essential for the phenotypes including cell division.

Published

2018

11. Control of the heat stress-induced alternative splicing of a subset of genes by hnRNP K

Author

Tetsuro Hirose, Arisa Kawamura, Tomoko Yamada, Hiroshi Sakamoto, Kunio Inoue, Kazuhiro Fukumura, Hitoshi Suzuki, Koichi Yamamoto, and Mari T. Furukawa

Subjects

0301 basic medicine, Biology, Heterogeneous-Nuclear Ribonucleoprotein K, HeLa, 03 medical and health sciences, Exon, RNA interference, Exon array, RNA Precursors, Genetics, Humans, HSP110 Heat-Shock Proteins, PTB-Associated Splicing Factor, Gene, 030102 biochemistry & molecular biology, Alternative splicing, Nuclear Proteins, RNA-Binding Proteins, Exons, Cell Biology, biology.organism_classification, Molecular biology, Heat stress, Alternative Splicing, 030104 developmental biology, Ribonucleoproteins, RNA splicing, Heat-Shock Response, HeLa Cells

Abstract

Pre-mRNA splicing is widely repressed upon heat shock in eukaryotic cells. However, it has been shown that HSP105 pre-mRNA is alternatively spliced in response to heat stress. Using RNAi screening in HeLa cells, we found that RNA-binding proteins hnRNP K and PSF/SFPQ are necessary for the exon 12 exclusion of HSP105 during heat stress. Moreover, exon array analyses showed that a group of genes is alternatively spliced during heat stress in an hnRNP K-dependent manner, whereas hnRNP K is not necessary for the stress-induced alternative splicing of the remaining genes. Among the latter group, we found that SRp38/SRSF10 and SC35/SRSF2 are necessary for the inclusion of exon 13 of TNRC6A during heat stress. Thus, our study clearly showed that several RNA-binding proteins are involved in the splicing regulation in response to heat stress in mammalian cells.

Published

2016

12. The Exon Junction Complex Controls the Efficient and Faithful Splicing of a Subset of Transcripts Involved in Mitotic Cell-Cycle Progression

Author

Kunio Inoue, Hiroshi Sakamoto, Kazuhiro Fukumura, Akila Mayeda, Yutaka Suzuki, Shunichi Wakabayashi, Kenta Nakai, and Naoyuki Kataoka

Subjects

0301 basic medicine, RNA Splicing, Mitosis, Cell Cycle Proteins, Biology, Catalysis, Article, Inorganic Chemistry, Transcriptome, lcsh:Chemistry, 03 medical and health sciences, Mitotic cell cycle, Gene expression, RNA Precursors, Humans, RNA, Messenger, Physical and Theoretical Chemistry, Molecular Biology, Gene, lcsh:QH301-705.5, Spectroscopy, Genetics, Models, Genetic, Organic Chemistry, Intron, General Medicine, Exons, Introns, Computer Science Applications, Cell biology, mitotic cell-cycle, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Gene Knockdown Techniques, RNA splicing, exon junction complex (EJC), Y14, pre-mRNA splicing, Exon junction complex, HeLa Cells

Abstract

The exon junction complex (EJC) that is deposited onto spliced mRNAs upstream of exon–exon junctions plays important roles in multiple post-splicing gene expression events, such as mRNA export, surveillance, localization, and translation. However, a direct role for the human EJC in pre-mRNA splicing has not been fully understood. Using HeLa cells, we depleted one of the EJC core components, Y14, and the resulting transcriptome was analyzed by deep sequencing (RNA-Seq) and confirmed by RT–PCR. We found that Y14 is required for efficient and faithful splicing of a group of transcripts that is enriched in short intron-containing genes involved in mitotic cell-cycle progression. Tethering of EJC core components (Y14, eIF4AIII or MAGOH) to a model reporter pre-mRNA harboring a short intron showed that these core components are prerequisites for the splicing activation. Taken together, we conclude that the EJC core assembled on pre-mRNA is critical for efficient and faithful splicing of a specific subset of short introns in mitotic cell cycle-related genes.

Published

2016

13. Involvement of the Spliceosomal U4 Small Nuclear RNA in Heterochromatic Gene Silencing at Fission Yeast Centromeres

Author

Tokio Tani, Kazuhiro Fukumura, Misato Morita, and Madoka Chinen

Subjects

RNA-induced transcriptional silencing, Chromosomal Proteins, Non-Histone, Heterochromatin, Centromere, Biology, Biochemistry, Chromosome Segregation, Gene Expression Regulation, Fungal, RNA, Small Nuclear, Schizosaccharomyces, Constitutive heterochromatin, Gene Silencing, Molecular Biology, Genetics, fungi, Intron, RNA, RNA, Fungal, DNA-Directed RNA Polymerases, Cell Biology, Introns, RNA silencing, Heterochromatin protein 1, Schizosaccharomyces pombe Proteins, Chromosomes, Fungal, Small nuclear RNA

Abstract

prp13-1 is one of the mutants isolated in a screen for defective pre-mRNA splicing at a nonpermissive temperature in fission yeast Schizosaccharomyces pombe. We cloned the prp13(+) gene and found that it encodes U4 small nuclear RNA (snRNA) involved in the assembly of the spliceosome. The prp13-1 mutant produced elongated cells, a phenotype similar to cell division cycle mutants, and displays a high incidence of lagging chromosomes on anaphase spindles. The mutant is hypersensitive to the microtubule-destabilizing drug thiabendazole, supporting that prp13-1 has a defect in chromosomal segregation. We found that the prp13-1 mutation resulted in expression of the ura4(+) gene inserted in the pericentromeric heterochromatin region and reduced recruitment of the heterochromatin protein Swi6p to that region, indicating defects in the formation of pericentromeric heterochromatin, which is essential for the segregation of chromosomes, in prp13-1. The formation of centromeric heterochromatin is induced by the RNA interference (RNAi) system in S. pombe. In prp13-1, the processing of centromeric noncoding RNAs to siRNAs, which direct the heterochromatin formation, was impaired and unprocessed noncoding RNAs were accumulated. These results suggest that U4 snRNA is required for the RNAi-directed heterochromatic gene silencing at the centromeres. In relation to the linkage between the spliceosomal U4 snRNA and the RNAi-directed formation of heterochromatin, we identified a mRNA-type intron in the centromeric noncoding RNAs. We propose a model in which the assembly of the spliceosome or a sub-spliceosome complex on the intron-containing centromeric noncoding RNAs facilitates the RNAi-directed formation of heterochromatin at centromeres, through interaction with the RNA-directed RNA polymerase complex.

Published

2010

14. Role and mechanism of U1-independent pre-mRNA splicing in the regulation of alternative splicing

Author

Kazuhiro Fukumura and Kunio Inoue

Subjects

Genetics, Alternative splicing, Exonic splicing enhancer, Eukaryota, Cell Biology, Computational biology, Biology, Models, Biological, Ribonucleoprotein, U1 Small Nuclear, Alternative Splicing, Splicing factor, SR protein, RNA splicing, RNA Precursors, Animals, Humans, Precursor mRNA, Molecular Biology, Minigene, Ribonucleoprotein

Abstract

In metazoan organisms, alternative splicing is a central mechanism for the regulation of gene expression. However, many questions remain about the underlying molecular mechanisms. Our recent work suggests that U1 snRNP-independent premRNA splicing occurs in humans, which contributes to the regulation of alternative splicing. So far it has been reported that several pre-mRNAs were spliced efficiently in a U1 snRNP-independent manner in vitro. Although the molecular mechanism and functional significance of U1-independent pre-mRNA splicing are not well understood, a model of how the 5' splice site is recognized U1-independently has been proposed. In this review, we first overview a model in which the 5' splice site is recognized by SR proteins and U6 snRNA. We then discuss our novel model and the functional significance of U1-independent pre-mRNA splicing in the regulation of alternative splicing, based on our recent work.

Published

2009

15. Tissue-specific splicing regulator Fox-1 induces exon skipping by interfering E complex formation on the downstream intron of human F1 gene

Author

Hiroshi Sakamoto, Kazuhiro Fukumura, Toshinobu Fujiwara, Ayako Kato, Kunio Inoue, Takashi Ideue, Yui Jin, Tetsuro Hirose, and Naoyuki Kataoka

Subjects

RNA Splicing Factors, Exonic splicing enhancer, Regulatory Sequences, Nucleic Acid, Biology, Cell Line, Mice, Exon, parasitic diseases, RNA Precursors, Genetics, Animals, Humans, RNA, Messenger, Binding Sites, Muscles, Alternative splicing, Intron, RNA-Binding Proteins, food and beverages, Exons, Molecular biology, Introns, Exon skipping, Protein Structure, Tertiary, Repressor Proteins, Alternative Splicing, Proton-Translocating ATPases, Spliceosomes, RNA, Tissue-Specific Splicing, Minigene

Abstract

Fox-1 is a regulator of tissue-specific splicing, via binding to the element (U)GCAUG in mRNA precursors, in muscles and neuronal cells. Fox-1 can regulate splicing positively or negatively, most likely depending on where it binds relative to the regulated exon. In cases where the (U)GCAUG element lies in an intron upstream of the alternative exon, Fox-1 protein functions as a splicing repressor to induce exon skipping. Here we report the mechanism of exon skipping regulated by Fox-1, using the hF1gamma gene as a model system. We found that Fox-1 induces exon 9 skipping by repressing splicing of the downstream intron 9 via binding to the GCAUG repressor elements located in the upstream intron 8. In vitro splicing analyses showed that Fox-1 prevents formation of the pre-spliceosomal early (E) complex on intron 9. In addition, we located a region of the Fox-1 protein that is required for inducing exon skipping. Taken together, our data show a novel mechanism of how RNA-binding proteins regulate alternative splicing.

Published

2007

16. [Molecular mechanism of exon definition and alternative splicing]

Author

Kazuhiro, Fukumura and Kunio, Inoue

Subjects

Alternative Splicing, Animals, Humans, Exons, RNA, Messenger, Introns, Ribonucleoprotein, U1 Small Nuclear

Published

2010

17. U1-independent pre-mRNA splicing contributes to the regulation of alternative splicing

Author

Hiroshi Sakamoto, Ichiro Taniguchi, Kazuhiro Fukumura, Mutsuhito Ohno, and Kunio Inoue

Subjects

Xenopus, Exonic splicing enhancer, Biology, Ribonucleoprotein, U1 Small Nuclear, Splicing factor, Genetics, RNA Precursors, Animals, Humans, RNA, Messenger, Alternative splicing, Intron, RNA-Binding Proteins, Group II intron, Exons, Cell biology, Alternative Splicing, Proton-Translocating ATPases, Polypyrimidine tract, RNA splicing, Spliceosomes, RNA, RNA Splice Sites, Minigene, HeLa Cells

Abstract

U1 snRNP plays a crucial role in the 5' splice site recognition during splicing. Here we report the first example of naturally occurring U1-independent U2-type splicing in humans. The U1 components were not included in the pre-spliceosomal E complex formed on the human F1gamma (hF1gamma) intron 9 in vitro. Moreover, hF1gamma intron 9 was efficiently spliced even in U1-disrupted Xenopus oocytes as well as in U1-inactivated HeLa nuclear extracts. Finally, hF1gamma exon 9 skipping induced by an alternative splicing regulator Fox-1 was impaired when intron 9 was changed to the U1-dependent one. Our results suggest that U1-independent splicing contributes to the regulation of alternative splicing of a class of pre-mRNAs.

Published

2009

18. The Exon Junction Complex Controls the Efficient and Faithful Splicing of a Subset of Transcripts Involved in Mitotic Cell-Cycle Progression.

Author

Kazuhiro Fukumura, Shunichi Wakabayashi, Naoyuki Kataoka, Hiroshi Sakamoto, Yutaka Suzuki, Kenta Nakai, Akila Mayeda, and Kunio Inoue

Subjects

*EXONS (Genetics), *GENE expression, *MESSENGER RNA, *RNA sequencing, *CELL cycle

Abstract

The exon junction complex (EJC) that is deposited onto spliced mRNAs upstream of exon--exon junctions plays important roles in multiple post-splicing gene expression events, such as mRNA export, surveillance, localization, and translation. However, a direct role for the human EJC in pre-mRNA splicing has not been fully understood. Using HeLa cells, we depleted one of the EJC core components, Y14, and the resulting transcriptome was analyzed by deep sequencing (RNA-Seq) and confirmed by RT--PCR. We found that Y14 is required for efficient and faithful splicing of a group of transcripts that is enriched in short intron-containing genes involved in mitotic cell-cycle progression. Tethering of EJC core components (Y14, eIF4AIII or MAGOH) to a model reporter pre-mRNA harboring a short intron showed that these core components are prerequisites for the splicing activation. Taken together, we conclude that the EJC core assembled on pre-mRNA is critical for efficient and faithful splicing of a specific subset of short introns in mitotic cell cycle-related genes. [ABSTRACT FROM AUTHOR]

Published

2016