Identification of a small molecule splicing inhibitor targeting UHM domains

Kobayashi, Asaki; Clément, Marie‐Jeanne; Craveur, Pierrick; Hage, Krystel El; Salone, Jean de Matha; Bollot, Guillaume; Pastré, David; Maucuer, Alexandre

doi:10.1111/febs.16199

Cited by 10 publications

(17 citation statements)

References 53 publications

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“…Recently, a high throughput screening identified a small molecule, UHMCP1, which prevents the SF3B1/U2AF65 interaction. UHMCP1 interacts with the hydrophobic pocket of the U2AF65 UHM domain, thus strongly impacting RNA splicing and cell viability of cancer cells [ 80 ]. Another study identified phenothiazine derivatives, such as 7,8-dihydroxyperphenazine and 7,8-dimethoxyperphenazine, as molecules targeting the early assembly of the spliceosome [ 81 ].…”

Section: Splicing-based Therapeutic Strategiesmentioning

confidence: 99%

Somatic Mutations in Core Spliceosome Components Promote Tumorigenesis and Generate an Exploitable Vulnerability in Human Cancer

Sette

Paronetto

2022

Cancers

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Alternative pre-mRNA processing enables the production of distinct mRNA and protein isoforms from a single gene, thus greatly expanding the coding potential of eukaryotic genomes and fine-tuning gene expression programs. Splicing is carried out by the spliceosome, a complex molecular machinery which assembles step-wise on mRNA precursors in the nucleus of eukaryotic cells. In the last decade, exome sequencing technologies have allowed the identification of point mutations in genes encoding splicing factors as a recurrent hallmark of human cancers, with higher incidence in hematological malignancies. These mutations lead to production of splicing factors that reduce the fidelity of the splicing process and yield splicing variants that are often advantageous for cancer cells. However, at the same time, these mutations increase the sensitivity of transformed cells to splicing inhibitors, thus offering a therapeutic opportunity for novel targeted strategies. Herein, we review the recent literature documenting cancer-associated mutations in components of the early spliceosome complex and discuss novel therapeutic strategies based on small-molecule spliceosome inhibitors that exhibit strong anti-tumor effects, particularly against cancer cells harboring mutations in spliceosomal components.

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Section: Splicing-based Therapeutic Strategiesmentioning

confidence: 99%

Somatic Mutations in Core Spliceosome Components Promote Tumorigenesis and Generate an Exploitable Vulnerability in Human Cancer

Sette

Paronetto

2022

Cancers

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“…UHMCP1 ( 1 ) and analogs ( 2 – 7 ) were prepared via a reaction sequence of reductive amination and subsequent deprotection of Boc group using HCl or hydrolysis of an ester group as shown in Scheme . Note that UHMCP1 ( 1 ) and 4 have four stereoisomers according to the report, whereas 2 , 3 , and 5 – 7 have two stereoisomers, respectively.…”

mentioning

confidence: 92%

“…The binding affinity of UHMCP1 to other three UHM domains was much weaker. Based on the microplate assay, UHMCP1 had an IC 50 value of 30 μM to U2AF2-UHM . When the amine group was positioned in the fused diazabicyclo-octane ring, the IC 50 values of 2 to SPF45-UHM, RBM39-UHM and PUF60-UHM were not markedly changed but were ∼5-fold lower with U2AF1-UHM.…”

mentioning

confidence: 97%

“…In addition to the ULMs from splicing factors, we included a recently discovered ULM in Rev HIV-1 and a less well-characterized ULM in ATXN1. Small-molecule inhibitors targeting the UHM domains have recently been reported. − We synthesized seven analogous compounds based on the tryptophan scaffold and characterized the selectivity of these inhibitors against different UHM domains.…”

mentioning

confidence: 99%

“…Another study by Hanzawa et al identified a PUF60-UHM inhibitor, DS89092425, and reported that a terminal amine group in DS89092425 contributed importantly to the binding affinity. Recently, Kobayashi et al combined virtual screening and in vitro assays to discover an indole containing small-molecule inhibitor (UHMCP1, Figure ) of the U2AF2-UHM domain (IC 50 ∼ 30 μM) . UHMCP1 and cmp9 were reported to induce splicing pattern changes in selective genes by inhibiting the UHM domains in HEK293 cells and a reconstituted minigene assay respectively.…”

mentioning

confidence: 99%

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Profiling the Binding Activities of Peptides and Inhibitors to the U2 Auxiliary Factor Homology Motif (UHM) Domains

Yuan

Howie

Sabzvar

et al. 2023

ACS Med. Chem. Lett.

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RNA splicing is a biological process to generate mature mRNA (mRNA) by removing introns and annexing exons in the nascent RNA transcript and is executed by a multiprotein complex called spliceosome. To aid RNA splicing, a class of splicing factors use an atypical RNA recognition domain (UHM) to bind with U2AF ligand motifs (ULMs) in proteins to form modules that recognize splice sites and splicing regulatory elements on mRNA. Mutations of UHM containing splicing factors have been found frequently in myeloid neoplasms. To profile the selectivity of UHMs for inhibitor development, we established binding assays to measure the binding activities between UHM domains and ULM peptides and a set of small-molecule inhibitors. Additionally, we computationally analyzed the targeting potential of the UHM domains by small-molecule inhibitors. Our study provided the binding assessment of UHM domains to diverse ligands that may guide development of selective UHM domain inhibitors in the future.

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Targeting RNA‐binding proteins with small molecules: Perspectives, pitfalls and bifunctional molecules

Kang

2023

FEBS Letters

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RNA‐binding proteins (RBPs) play vital roles in organisms through binding with RNAs to regulate their functions. Small molecules affecting the function of RBPs have been developed, providing new avenues for drug discovery. Herein, we describe the perspectives on developing small molecule regulators of RBPs. The following types of small molecule modulators are of great interest in drug discovery: small molecules binding to RBPs to affect interactions with RNA molecules, bifunctional molecules binding to RNA or RBP to influence their interactions, and other types of molecules that affect the stability of RNA or RBPs. Moreover, we emphasize that the bifunctional molecules may play important roles in small molecule development to overcome the challenges encountered in the process of drug discovery.

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Identification of a small molecule splicing inhibitor targeting UHM domains

Cited by 10 publications

References 53 publications

Somatic Mutations in Core Spliceosome Components Promote Tumorigenesis and Generate an Exploitable Vulnerability in Human Cancer

Somatic Mutations in Core Spliceosome Components Promote Tumorigenesis and Generate an Exploitable Vulnerability in Human Cancer

Profiling the Binding Activities of Peptides and Inhibitors to the U2 Auxiliary Factor Homology Motif (UHM) Domains

Targeting RNA‐binding proteins with small molecules: Perspectives, pitfalls and bifunctional molecules

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