CLK-dependent exon recognition and conjoined gene formation revealed with a novel small molecule inhibitor

Funnell, Tyler; Tasaki, Shinya; Oloumi, Arusha; Araki, Shinsuke; Kong, Esther; Yap, Damian; Nakayama, Yusuke; Hughes, Christopher S.; Cheng, Soo‐Chen; Tozaki, Hirokazu; Iwatani, Misa; Sasaki, Satoshi; Ohashi, Taiki; Miyazaki, T.; Morishita, Nao; Morishita, Daisuke; Ogasawara-Shimizu, Mari; Ohori, Momoko; Nakao, Shigetomi; Karashima, Masatoshi; Sano, Mitsuhiko; Murai, Aiko; Nomura, Toshiyuki; Uchiyama, Noriko; Kawamoto, Takahiro; Hara, Ryujiro; Nakanishi, Osamu; Shumansky, Karey; Rosner, Jamie; Wan, Adrian; McKinney, Steven; Morin, Gregg B.; Nakanishi, Atsushi; Shah, Sohrab P.; Toyoshiba, Hiroyoshi; Aparicio, Samuel

doi:10.1038/s41467-016-0008-7

Cited by 87 publications

(105 citation statements)

References 62 publications

(90 reference statements)

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“…Interestingly, our RNA-Seq data suggested that cellular status of MYC slightly affected the determination of downstream AS events in response to CLK inhibition because T-025 caused similar AS in four tested solid cancer cell lines, including MYC-amplified COLO320HSR cells. The finding that MYC slightly affected CLK inhibitor-dependent AS events was also supported by a previous finding that CLK inhibitor, T3-dependent AS events mostly (~75%) overlapped between the hTERT un-transformed fibroblast cells and MYC-amplified HCT116 colorectal cancer cells (Funnell et al, 2017). We also show that transcriptional regulation of CLK2 and other CLK kinases were independent on MYC activation, degree of T-025-mediated SE was similar regardless MYC induction, and AS events regulated by MYC induction or T-025 rarely overlapped.…”

Section: Discussionsupporting

confidence: 81%

“…of three independent experiments ( n = 3). IC 50 values and 95% CI were determined by using Prism. Data information: The chemical structure of T3, the result of enzymatic assay of T3, and AS events modulated by T3 in HCT116 are cited from a previous article (Funnell et al , ).…”

Section: Resultsmentioning

confidence: 99%

“…First, the different chemical scaffold CLK inhibitor T3 exhibited similar effects to T‐025 in terms of AS and the profile of growth inhibition, including MYC induction‐dependent higher activity. Notably, AS caused by T3 has been reported to be largely overlapped with that caused by CLK1/2/3/4 siRNA (Funnell et al , ), suggesting that AS caused by T‐025 was also similar to that caused by the depletion of CLKs. Second, we show that expression level of CLK2 is responsible for the T‐025‐mediated effects on the induction of AS and the suppression of cell proliferation; The SE type AS caused by T‐025 was larger in CLK2 high expressing NCI‐H1048 cells, and smaller in CLK2 low expressing 786‐O cells.…”

Section: Discussionmentioning

confidence: 95%

“…2018 Takeda Pharmaceutical Company EMBO Molecular Medicine 10: e8289 | 2018effects to T-025 in terms of AS and the profile of growth inhibition, including MYC induction-dependent higher activity. Notably, AS caused by T3 has been reported to be largely overlapped with that caused by CLK1/2/3/4 siRNA(Funnell et al, 2017), suggesting that AS caused by T-025 was also similar to that caused by the depletion of CLKs. Second, we show that expression level of CLK2 is responsible for the T-025-mediated effects on the induction of AS and the suppression of cell proliferation; The SE type AS caused by T-025 MYC activation and T-025 treatment synergistically induced apoptosis.A, B Dox treatment-induced/activated MYC in MYC-inducible SK-MEL-28 cells.…”

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confidence: 95%

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Anti‐tumor efficacy of a novel CLK inhibitor via targeting RNA splicing and MYC‐dependent vulnerability

et al. 2018

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The modulation of pre‐mRNA splicing is proposed as an attractive anti‐neoplastic strategy, especially for the cancers that exhibit aberrant pre‐mRNA splicing. Here, we discovered that T‐025 functions as an orally available and potent inhibitor of Cdc2‐like kinases (CLKs), evolutionally conserved kinases that facilitate exon recognition in the splicing machinery. Treatment with T‐025 reduced CLK‐dependent phosphorylation, resulting in the induction of skipped exons, cell death, and growth suppression in vitro and in vivo. Further, through growth inhibitory characterization, we identified high CLK2 expression or MYC amplification as a sensitive‐associated biomarker of T‐025. Mechanistically, the level of CLK2 expression correlated with the magnitude of global skipped exons in response to T‐025 treatment. MYC activation, which altered pre‐mRNA splicing without the transcriptional regulation of CLKs, rendered cancer cells vulnerable to CLK inhibitors with synergistic cell death. Finally, we demonstrated in vivo anti‐tumor efficacy of T‐025 in an allograft model of spontaneous, MYC‐driven breast cancer, at well‐tolerated dosage. Collectively, our results suggest that the novel CLK inhibitor could have therapeutic benefits, especially for MYC‐driven cancer patients.

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Section: Discussionsupporting

confidence: 81%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 95%

mentioning

confidence: 95%

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Anti‐tumor efficacy of a novel CLK inhibitor via targeting RNA splicing and MYC‐dependent vulnerability

et al. 2018

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“…However, SRPK family members exhibit highly tissue-specific expression profiles (Nakagawa et al, 2005; Wang et al, SRPKIN-1 (Hatcher et al, 2018) (Figure 1A). In contrast, treatment of mESCs with T3, a selective inhibitor of the closely related CLK kinases (Funnell et al, 2017), which have also been shown to phosphorylate splicing factors (Colwill et al, 1996), leads to near complete inhibition of SR-protein phosphorylation ( Figure 1A). Our results suggest that SRPKs are not the major SRSF protein kinases in mESCs, and may have acquired other developmental function(s) during metazoan evolution.…”

Section: Introductionmentioning

confidence: 95%

Functional diversification of Ser-Arg rich protein kinases to control ubiquitin-dependent neurodevelopmental signalling

Bustos

Segarra-Fas

Nardocci

et al. 2020

Preprint

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Conserved protein kinases with core cellular functions have been frequently redeployed during metazoan evolution to regulate specialized developmental processes. Ser-Arg Repeat Protein Kinase (SRPK) is one such conserved eukaryotic kinase, which controls mRNA splicing.Surprisingly, we show that SRPK has acquired a novel function in regulating a neurodevelopmental ubiquitin signalling pathway. In mammalian embryonic stem cells, SRPK phosphorylates Ser-Arg motifs in RNF12/RLIM, a key developmental E3 ubiquitin ligase that is mutated in an intellectual disability syndrome. Processive phosphorylation by SRPK stimulates RNF12-dependent ubiquitylation of transcription factor substrates, thereby acting to restrain a neural gene expression programme that is aberrantly expressed in intellectual disability. SRPK family genes are also mutated in intellectual disability disorders, and patient-derived SRPK point mutations impair RNF12 phosphorylation. Our data reveal unappreciated functional diversification of SRPK to regulate ubiquitin signalling that ensures correct regulation of neurodevelopmental gene expression. 1998), suggesting that these protein kinases may indeed perform specialized functions required for multicellular development.Here, we show that SRPKs have undergone functional diversification to acquire a critical new role during mammalian development. Surprisingly, SRPK activity is largely dispensable for phosphorylation of Ser-Arg rich splicing factors (SRSFs) in mammalian embryo-derived stem cells.

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2D Materials Based on Main Group Element Compounds: Phases, Synthesis, Characterization, and Applications

Neupane

Jia

et al. 2020

Adv Funct Materials

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2D materials based on main group element compounds have recently attracted significant attention because of their rich stoichiometric ratios and structure motifs. This review focuses on the phases in various 2D binary materials including III-VI, IV-VI, V-VI, III-V, IV-V, and V-V materials. Reducing 3D materials to 2D introduces confinement and surface effects as well as stabilizes unstable 3D phases in their 2D form. Their crystal structures, stability, preparation, and applications are summarized based on theoretical predictions and experimental explorations. Moreover, various properties of 2D materials, such as ferroelectric effect, anisotropic optical and electrical properties, ultralow thermal conductivity, and topological state are discussed. Finally, a few perspectives and an outlook are given to inspire readers toward exploring 2D materials with new phases and properties.

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CLK-dependent exon recognition and conjoined gene formation revealed with a novel small molecule inhibitor

Cited by 87 publications

References 62 publications

Anti‐tumor efficacy of a novel CLK inhibitor via targeting RNA splicing and MYC‐dependent vulnerability

Anti‐tumor efficacy of a novel CLK inhibitor via targeting RNA splicing and MYC‐dependent vulnerability

Functional diversification of Ser-Arg rich protein kinases to control ubiquitin-dependent neurodevelopmental signalling

2D Materials Based on Main Group Element Compounds: Phases, Synthesis, Characterization, and Applications

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