Therapeutic Targeting of RNA Splicing in Cancer

Bonner, Elizabeth; Lee, Stanley Chun-Wei

doi:10.3390/genes14071378

Cited by 12 publications

(5 citation statements)

References 130 publications

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“…In the realm of therapeutics, small molecule agents like Pladienolide B and its analogs, which target SF3B1 and analogous splicing factors, are being rigorously investigated for their potential e cacy in treating malignancies characterized by SF3B1 mutations [27,28]. Additionally, in the context of nonsmall cell lung cancer (NSCLC), the use of small molecule inhibitors like H3B-8800, targeting splicing events associated with mutations in splicing factors such as SRSF2, SF3B1, and U2AF1, represents a novel strategy to disrupt the splicing apparatus and attenuate the proliferation of neoplastic cells [29,30].…”

Section: Discussionmentioning

confidence: 99%

Assessment of molecular and morphological dynamics during long-time in vitro cultivation of cryopreserved human ovarian tissue: risk of genetic alterations

Wang,

Todorov,

Isachenko

et al. 2024

Preprint

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Cryopreservation of human ovarian tissue is a technology for protection of reproductive potential in patients undergoing aggressive anticancer treatments. This technology includes the following stages: saturation by permeable cryoprotectants, freezing, thawing, removal of cryoprotectants, and tissues in vitro or in situ culture. The aim of our investigations was the evaluation of genetic risks and molecular alterations in human ovarian tissue during in vitro culture. Ovarian tissue was frozen in 6% ethylene glycol and 6% dimethyl sulfoxide with speed of cooling 0.3°C/min and thawed at 100°C. After removal of cryoprotectants tissue fragments were in vitro cultured with the soluble extract of basement membrane protein (Matrigel) 3-D culture system for 7 days. Morphological and functional assessments were conducted using microscopic observation and RNA-Seq. Comparative analysis of tissue morphology before and after culture was performed with bioinformatics for gene expression and variant analysis, including functional annotation and study of protein-protein interaction. DNA and RNA analyses after cultivation indicated a rise in gene fusion and alternative splicing events, potentially affecting gene expression and cellular functions. It was concluded that long-time in vitro culture of human ovarian tissue results in substantial changes in its morphology and genetic alteration.

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Section: Discussionmentioning

confidence: 99%

Assessment of molecular and morphological dynamics during long-time in vitro cultivation of cryopreserved human ovarian tissue: risk of genetic alterations

Wang,

Todorov,

Isachenko

et al. 2024

Preprint

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“…Irregularities in splicing factor genes, encompassing alterations in expression levels or the presence of mutations, have the capacity to produce abnormal mRNA splicing patterns on a genome-wide scale 12 . This phenomenon is a prevalent characteristic observed in various cancer types, spanning from haematological to solid cancers 13 . Numerous splicing factors alterations have been identified in PDAC.…”

Section: Introductionmentioning

confidence: 93%

Exploring Splicing Modulation as an Innovative Approach to Combat Pancreatic Cancer: SF3B1 Emerges as a Prognostic Indicator and Therapeutic Target

Sciarrillo,

Terrana,

Comandatore

et al. 2024

Int. J. Biol. Sci.

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“…There are compounds used for aberrant splicing-related cancers, including GEX1 [ 118 ], spliceostatins, sudemycins, FD-895, E7107 and FR901464, which all act directly on the core spliceosomal component SF3B1, of which accounts for 10% splicing events [ 119 ]. The use of protein arginine methyltransferases (PRMTs) is an attractive approach to targeting splicing.…”

Section: Therapeutic Interventionsmentioning

confidence: 99%

“…The use of protein arginine methyltransferases (PRMTs) is an attractive approach to targeting splicing. They catalyze arginine dimethylation of various substrates, including RBPs and splicing factors [ 118 ]. GSK3368715 and PF06939999, GSK3326595 and JNJ-64619178 are type I and PRMT5 inhibitors currently in clinical trials, respectively.…”

Section: Therapeutic Interventionsmentioning

confidence: 99%

Immunomodulatory Gene-Splicing Dysregulation in Tumorigenesis: Unmasking the Complexity

Maebele,

Mulaudzi,

Yasasve

et al. 2023

Molecules

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Cancer is a global health concern with rising incidence, morbidity, and mortality. The interaction between the tumor and immune cells within the tumor microenvironment is facilitated by signaling pathways driven by immunomodulatory proteins. Alternative splicing regulates the production of multiple immunomodulatory proteins with diverse functionality from a single mRNA transcript. Splicing factors are pivotal in modulating alternative splicing processes but are also subject to regulation. The dysregulation of alternative splicing may result from splicing factor (SF) abnormal expression levels and mutations in the cis and trans-acting elements and small nuclear RNA (snRNA) molecules. Aberrant splicing may generate abnormal mRNA transcripts encoding isoforms with altered functions that contribute to tumorigenesis or cancer progression. This review uncovers the complexity of immunomodulatory genes splicing dysregulation in oncogenesis. Identifying specific immunomodulatory splicing isoforms that contribute to cancer could be utilized to improve current immunotherapeutic drugs or develop novel therapeutic interventions for cancer.

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Therapeutic Targeting of RNA Splicing in Cancer

Cited by 12 publications

References 130 publications

Assessment of molecular and morphological dynamics during long-time in vitro cultivation of cryopreserved human ovarian tissue: risk of genetic alterations

Assessment of molecular and morphological dynamics during long-time in vitro cultivation of cryopreserved human ovarian tissue: risk of genetic alterations

Exploring Splicing Modulation as an Innovative Approach to Combat Pancreatic Cancer: SF3B1 Emerges as a Prognostic Indicator and Therapeutic Target

Immunomodulatory Gene-Splicing Dysregulation in Tumorigenesis: Unmasking the Complexity

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