Differential Impacts of Alternative Splicing Networks on Apoptosis

Lin, Jung-Chun; Tsao, Mei Fen; Lin, Ying

doi:10.3390/ijms17122097

Cited by 26 publications

(25 citation statements)

References 136 publications

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“…The fact that AS strongly regulates apoptosis is well established and has been recently reviewed. 93,94 It is known that DNA damage, including the ones induced by PT, mainly activates the intrinsic apoptotic pathway, initiated by mitochondrial permeabilization and leading to caspase activation, principally through the activity of caspase-8 and -9. (also known as p47 and DeltaNp53) is an N-terminal truncation of full-length p53 that lacks the first transcriptional activation domain (TAD1).…”

Section: Alternative Splicing In the Regulation Of Pt-induced Apoptmentioning

confidence: 99%

RNA splicing alteration in the response to platinum chemotherapy in ovarian cancer: A possible biomarker and therapeutic target

Pellarin

Belletti

Baldassarre

2020

Medicinal Research Reviews

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Since its discovery, alternative splicing has been recognized as a powerful way for a cell to amplify the genetic information and for a living organism to adapt, evolve, and survive. We now know that a very high number of genes are regulated by alternative splicing and that alterations of splicing have been observed in different types of human diseases, including cancer. Here, we review the accumulating knowledge that links the regulation of alternative splicing to the response to chemotherapy, focusing our attention on ovarian cancer and platinum‐based treatments. Moreover, we discuss how expanding information could be exploited to identify new possible biomarkers of platinum response, to better select patients, and/or to design new therapies able to overcome platinum resistance.

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Section: Alternative Splicing In the Regulation Of Pt-induced Apoptmentioning

confidence: 99%

RNA splicing alteration in the response to platinum chemotherapy in ovarian cancer: A possible biomarker and therapeutic target

Pellarin

Belletti

Baldassarre

2020

Medicinal Research Reviews

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“…Although there is example of splicing isoforms promoting each hallmark of cancer [13,63,64], the phenotype of a [65,66].…”

Section: Functional Genomic Of Splicing Isoformsmentioning

confidence: 99%

Splicing isoform-specific functional genomic in cancer cells

Brosseau

2018

Appl Cancer Res

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Alternative splicing is a regulated process whereby one gene can generate multiple mRNA isoforms susceptible to be translated into protein isoforms of various functions. Several publications report the aberrant expression of splicing isoforms in cancer cells and tissues. However, in most cases, their function remains to be established. In this review article, I will discuss the molecular tool available to perform isoform-specific functional genomics, the methodologies to quantify their effectiveness and the resulting isoform-specific phenotype in human cancer cell lines.

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“…There are seven types of alternative splicing pattern, that is, mutually exclusive exons (ME), retained intron (RI), alternate donor site (AD), alternate acceptor site (AA), alternate promotor (AP), alternate terminator (AT) and exon skip (ES) [11]. Under the physiological condition, AS plays a vitally important regulating effect in the process of development, tissue identity, differentiation, cell-to-cell communication, cell senescence and apoptosis [12][13][14]. AS is accurately regulated by extensive splicing factors which participate in the precise selection of splicing sites and subsequent splicing events [15].…”

Section: Introductionmentioning

confidence: 99%

Comprehensive analysis of alternative splicing and transcriptome related to the prognosis of cervical squamous cell cancer

Yan

Chen

et al. 2020

Preprint

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Background: Cervical squamous cell cancer (CESC) is a common malignancy tumor with high incidence and mortality in women globally. Increasing studies have indicated that there was an indivisible association between alternative mRNA splicing (AS) and multiple types of cancer. However, comprehensive analysis of alternative mRNA splicing events is scarce in CESC. Methods: In this study, alternative mRNA splicing events data and clinical information of 216 CESC patients were downloaded from TCGA SpliceSeq database and TCGA website. We used identified survival-associated splicing events (SASEs) to construct prognostic signatures. Kaplan-Meier survival analysis and receiver operating characteristic (ROC) curve were performed to evaluate the clinical value of prognostic signatures. A nomogram was carried out to quantitatively predict individuals’ survival probability. Regulatory network between splicing factors (SFs) and SASE was analyzed to explore the upstream regulators of a certain SASE. Additionally, we explored potential downstream pathways of a certain SASE. Results: A total of 41776 alternative splicing events in 9961 genes were collected. After sorting out SASEs, multivariable regression analysis was used to acquire 70 SASEs that could be independent prognostic factors for overall survival in CESC. Kaplan-Meier survival analyses showed that the difference was statistically significant (P＜0.01). The area under ROC curve (AUC) for all AS pattern was 0.932. A nomogram was constructed with a concordance index of 0.82 to predict individuals’ survival probability. EIF3A positively regulated SEC23A-27346-AP with highest correlation coefficient (P＜0.001, R=0.69). Besides, the most significant SASEs and KEGG pathways were SEC23A-27346-AP and adherens junction pathway (P=0.02, R=0.65). Conclusions: Prognostic signatures of survival-associated splicing events were independent prognostic factors for overall survival among CESC patients. A nomogram could quantitatively predict individuals’ survival probability. Moreover, we proposed that splicing factor EIF3A positively regulated SEC23A-27346-AP, and adherens junction pathway may be the downstream pathway of SEC23A-27346-AP. The aforementioned signaling pathway could play a crucial role in the development of CESC.

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Differential Impacts of Alternative Splicing Networks on Apoptosis

Cited by 26 publications

References 136 publications

RNA splicing alteration in the response to platinum chemotherapy in ovarian cancer: A possible biomarker and therapeutic target

RNA splicing alteration in the response to platinum chemotherapy in ovarian cancer: A possible biomarker and therapeutic target

Splicing isoform-specific functional genomic in cancer cells

Comprehensive analysis of alternative splicing and transcriptome related to the prognosis of cervical squamous cell cancer

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