Antitumorigenic potential of STAT3 alternative splicing modulation

Zammarchi, Francesca; Stanchina, Elisa de; Bournazou, Eirini; Supakorndej, Teerawit; Martires, Kathryn J.; Riedel, Elyn; Corben, Adriana D.; Bromberg, Jacqueline; Cartegni, Luca

doi:10.1073/pnas.1108482108

Cited by 140 publications

(128 citation statements)

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“…More recent studies have demonstrated that STAT3b may activate a specific set of genes and possess non-redundant functions to STAT3a. Zammarchi et al used morpholino oligomers to redirect endogenous STAT3 alternative splicing from STAT3a to STAT3b (Zammarchi et al, 2011). This study showed that inducing the STAT3b isoform in MDA-MB-435 cells caused cell death and tumor regression in the xenograft models.…”

Section: Discussionmentioning

confidence: 83%

“…The same study showed that STAT3 canonical target genes were not affected by the switch from STAT3a to STAT3b. Rather, a unique expression signature seems to be associated with the physiological a-to-b splicing shift (Zammarchi et al, 2011). In mammary gland development, it has become clear that STAT3 regulates a complex series of processes involving alveolar epithelial cell death during involution by maintaining the balance of inflammatory and anti-inflammatory signaling (Pensa et al, 2009).…”

Section: Discussionmentioning

confidence: 99%

“…Since STAT3 transcription factors were reported to play key roles in mammary epithelial cell apoptosis at the onset of involution, we explored the role of miR146b in regulating STAT3 isoforms. STAT3 has two main isoforms: the full-length STAT3a and the truncated STAT3b, by alternative mRNA splicing of exon 23 (Huang et al, 2007;Zammarchi et al, 2011). In STAT3b, the 55-amino acid C-terminal acidic transactivation domain of STAT3a is replaced by seven unique amino acid residues (Zammarchi et al, 2011).…”

Section: Discussionmentioning

confidence: 99%

“…STAT3 has two main isoforms: the full-length STAT3a and the truncated STAT3b, by alternative mRNA splicing of exon 23 (Huang et al, 2007;Zammarchi et al, 2011). In STAT3b, the 55-amino acid C-terminal acidic transactivation domain of STAT3a is replaced by seven unique amino acid residues (Zammarchi et al, 2011). An important factor in STAT3 functional heterogeneity may be the existence of these two alternatively spliced isoforms.…”

Section: Discussionmentioning

confidence: 99%

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Novel role of microRNA146b in promoting mammary alveolar progenitor cell maintenance

Elsarraj

Valdez

et al. 2013

Journal of Cell Science

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SummaryIn this report, we have shown that miR146b promotes the maintenance of pregnancy-derived mammary luminal alveolar progenitors. MiR146b expression was significantly higher in the mammary glands of pregnant and lactating mice than in virgin mice. Furthermore, miR146b levels were significantly higher in mouse mammary glands exposed to the sex hormones, estrogen and progesterone, compared with those of untreated control animals. Pregnancy-derived primary mouse mammary epithelial cells in which miR146b was knocked down showed a significant reduction in the number of hollow acinar organoid structures formed on three-dimensional Matrigel and in bcasein expression. This demonstrates that miR146b promotes the maintenance of pregnancy-derived mammary luminal alveolar progenitors. It has been shown that mouse mammary luminal progenitors give rise to hollow organoid structures, whereas solid organoid structures are derived from stem cells. Among several miR146b targets, miR146b knockdown resulted in preferential STAT3b overexpression. In the primary mouse mammary epithelial cells, overexpression of STAT3b isoform caused mammary epithelial cell death and a significant reduction in b-casein mRNA expression. Therefore, we conclude that during pregnancy miR146b is involved in luminal alveolar progenitor cell maintenance, at least partially, by regulating STAT3b.

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Section: Discussionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Novel role of microRNA146b in promoting mammary alveolar progenitor cell maintenance

Elsarraj

Valdez

et al. 2013

Journal of Cell Science

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“…STAT3 is of particular interest because of its pleiotropic and uncertain functionality, with conflicting reports on whether it acts as an oncoprotein or tumor suppressor in cancer (reviewed in reference 33 ). Differences in STAT3 α and β splice variant function had been characterized previously 34,35 , and our protocol facilitated a knock-down/re-expression analysis that suggests a need for an optimal ratio of S and ΔS transcripts 19 .…”

Section: Discussionmentioning

confidence: 99%

Merging Absolute and Relative Quantitative PCR Data to Quantify STAT3 Splice Variant Transcripts

Turton

Esnault

Delain

et al. 2016

JoVE

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Human signal transducer and activator of transcription 3 (STAT3) is one of many genes containing a tandem splicing site. Alternative donor splice sites 3 nucleotides apart result in either the inclusion (S) or exclusion (ΔS) of a single residue, Serine-701. Further downstream, splicing at a pair of alternative acceptor splice sites result in transcripts encoding either the 55 terminal residues of the transactivation domain (α) or a truncated transactivation domain with 7 unique residues (β). As outlined in this manuscript, measuring the proportions of STAT3's four spliced transcripts (Sα, Sβ, ΔSα and ΔSβ) was possible using absolute qPCR (quantitative polymerase chain reaction). The protocol therefore distinguishes and measures highly similar splice variants. Absolute qPCR makes use of calibrator plasmids and thus specificity of detection is not compromised for the sake of efficiency. The protocol necessitates primer validation and optimization of cycling parameters. A combination of absolute qPCR and efficiency-dependent relative qPCR of total STAT3 transcripts allowed a description of the fluctuations of STAT3 splice variants' levels in eosinophils treated with cytokines. The protocol also provided evidence of a co-splicing interdependence between the two STAT3 splicing events. The strategy based on a combination of the two qPCR techniques should be readily adaptable to investigation of cosplicing at other tandem splicing sites.

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Splicing Modulation as Therapy for Human Genetic Disease

Srirangalingam

Khoo

2015

Encyclopedia of Life Sciences

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The sequencing of the human genome has led to a greater appreciation of the contribution that genetic abnormalities and splicing errors make to the burden of human disease. The modulation of splicing using antisense oligonucleotides provides an attractive therapeutic option for tailored interventions in rare genetic disease. In this review, we outline the various approaches to splicing modulation and provide examples of each strategy. Finally, we address some of the practical issues facing the field in trying to bring this technology towards clinical application using the treatment of Duchenne muscular dystrophy and spinal muscular atrophy as examples. Key Concepts Ninety‐five percent of human genes undergo splicing. An estimated 50% of all human genetic diseases result from splicing abnormalities. Splicing modulation using antisense oligonucleotide (ASO) technology offers the future prospect of personalised medicine tailored to specific mutations. Strategies to modulate splicing include suppression of an aberrant splice isoform, switching between known splicing variants or generating a novel variant with a potential therapeutic attribute. ASO chemistries are varied and have been optimised to improve target binding and resist nuclease degradation. ASO targets include all pre‐mRNA sites which influence the splicing process. Splicing events can be complex and unpredictable. Therefore an iterative method of design and test is required to optimise ASO efficacy. ASO side‐effects are likely to stem from the ASO chemistry, off‐target effects as the result of nonspecific binding, and ASO distribution to organs when given in vivo. Optimising tissue delivery of ASO remains a significant challenge.

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Antitumorigenic potential of STAT3 alternative splicing modulation

Cited by 140 publications

References 38 publications

Novel role of microRNA146b in promoting mammary alveolar progenitor cell maintenance

Novel role of microRNA146b in promoting mammary alveolar progenitor cell maintenance

Merging Absolute and Relative Quantitative PCR Data to Quantify STAT3 Splice Variant Transcripts

Splicing Modulation as Therapy for Human Genetic Disease

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