RNA-Binding Protein FXR1 Regulates p21 and TERC RNA to Bypass p53-Mediated Cellular Senescence in OSCC

Majumder, Mrinmoyee; House, Reniqua P.; Palanisamy, Nallasivam; Qie, Shuo; Day, Terrence A.; Neskey, David M.; Diehl, J. Alan; Palanisamy, Viswanathan

doi:10.1371/journal.pgen.1006306

Cited by 56 publications

(88 citation statements)

References 62 publications

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“…However, TP53 is frequently mutated in the disease, allowing tumour cells to escape cell cycle arrest and continue proliferating , which can also lead to increased resistance to chemo‐ and radiotherapy . FXR1 may support this evasion of arrest through negative regulation and/or destabilisation of p21 and stabilisation of telomerase RNA component (TERC) activity in vitro .…”

Section: Identification Of Pro‐oncogenic Factors In 3q26‐29mentioning

confidence: 99%

3q26‐29 Amplification in head and neck squamous cell carcinoma: a review of established and prospective oncogenes

Davidson

Shanks

2017

The FEBS Journal

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Head and neck squamous cell carcinoma (HNSCC) is significantly underrepresented in worldwide cancer research, yet survival rates for the disease have remained static for over 50 years. Distant metastasis is often present at the time of diagnosis, and is the primary cause of death in cancer patients. In the absence of routine effective targeted therapies, the standard of care treatment remains chemoradiation in combination with (often disfiguring) surgery. A defining characteristic of HNSCC is the amplification of a region of chromosome 3 (3q26‐29), which is consistently associated with poorer patient outcome. This review provides an overview of the role the 3q26‐29 region plays in HNSCC, in terms of both known and as yet undiscovered processes, which may have potential clinical relevance.

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Section: Identification Of Pro‐oncogenic Factors In 3q26‐29mentioning

confidence: 99%

3q26‐29 Amplification in head and neck squamous cell carcinoma: a review of established and prospective oncogenes

Davidson

Shanks

2017

The FEBS Journal

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“…FXR1 is hypothesized to regulate mRNA translation, localization, and stability (Cook et al, 2014;Davidovic et al, 2013;Majumder et al, 2016;Mientjes et al, 2004;Patzlaff et al, 2017;Vasudevan and Steitz, 2007;Zarnescu and Gregorio, 2013); however, there is little known about the mechanisms of function of FXR1 in physiological or pathological contexts. Here, we show quantitative differences in FXR1 isoforms arising from tissue-specific and developmentally regulated alternative splicing and a functional role for fxr1 splicing in myotube formation and Xenopus development.…”

Section: Discussionmentioning

confidence: 99%

Regulation of FXR1 by alternative splicing is required for muscle development and controls liquid-like condensates in muscle cells

Smith

Curry

Blue

et al. 2019

Preprint

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Fragile-X mental retardation autosomal homolog-1 (FXR1) is a muscle-enriched RNA-binding protein. FXR1 depletion is perinatally lethal in mice, Xenopus, and zebrafish; however, the mechanisms driving these phenotypes remain unclear. The FXR1 gene undergoes alternative splicing, producing multiple protein isoforms and missplicing has been implicated in disease. Furthermore, mutations that cause frameshifts in muscle-specific isoforms result in congenital multi-minicore myopathy. We observed that FXR1 alternative splicing is pronounced in the serine and arginine-rich intrinsicallydisordered domain; these domains are known to promote biomolecular condensation.Here, we show that tissue-specific splicing of fxr1 is required for Xenopus development and alters the disordered domain of FXR1. FXR1 isoforms vary in the formation of RNAdependent biomolecular condensates in cells and in vitro. This work shows that regulation of tissue-specific splicing can influence FXR1 condensates in muscle development and how mis-splicing promotes disease. KEYWORDS FXR1, alternative splicing, biomolecular condensation, myogenesis, Xenopus, muscle HIGHLIGHTS • The muscle-specific exon 15 impacts FXR1 functions • Alternative splicing of FXR1 is tissue-and developmental stage specific • FXR1 forms RNA-dependent condensates • Splicing regulation changes FXR1 condensate properties

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“…However, numerous HNSCCs are HPV-independent, thus underscoring the need to identify additional genetic alterations in HNSCC. In the September 2016 issue of PLOS Genetics , Majumber et al reported that the Fragile X-related protein 1 (FXR1), an RNA-binding protein, suppresses the senescence response in two different HPV-negative HNSCC cell lines [8]. This further supports the requirement for bypassing senescence in both HPV-positive and -negative HNSCC and sheds light on the putative role of FXR1 in promoting HNSCC.…”

mentioning

confidence: 86%

“…In addition to its amplification in lung, breast, and ovarian as well as head and neck cancers [8,9], FXR1 was shown to be down-regulated in other human pathologies such as facioscapulohumeral muscular dystrophy, an inherited myopathy [16]. FXR1 plays an important role in myogenesis in both mouse and Xenopus .…”

Section: Modulating Fxr1 Activity To Treat Hnscc and Facioscapulohumementioning

confidence: 99%

“…FXR1 knockout mice die shortly after birth and display disruption of the cellular architecture of skeletal and cardiac muscle [17]. Majumber et al demonstrated that loss of FXR1 not only leads to senescence in cancer cells, but also in normal cells such as mouse embryonic fibroblasts [8]. Considering that cellular senescence limits the muscle stem cell regenerative capacity [18], it is reasonable to envisage that the phenotype observed following FXR1 dysfunction in facioscapulohumeral muscular dystrophy could be caused by concomitant overstimulation of cellular senescence, thus leading to muscle tissue degeneration.…”

Section: Modulating Fxr1 Activity To Treat Hnscc and Facioscapulohumementioning

confidence: 99%

See 1 more Smart Citation

The Rise of FXR1: Escaping Cellular Senescence in Head and Neck Squamous Cell Carcinoma

Fernández

Mallette

2016

PLoS Genet

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RNA-Binding Protein FXR1 Regulates p21 and TERC RNA to Bypass p53-Mediated Cellular Senescence in OSCC

Cited by 56 publications

References 62 publications

3q26‐29 Amplification in head and neck squamous cell carcinoma: a review of established and prospective oncogenes

3q26‐29 Amplification in head and neck squamous cell carcinoma: a review of established and prospective oncogenes

Regulation of FXR1 by alternative splicing is required for muscle development and controls liquid-like condensates in muscle cells

The Rise of FXR1: Escaping Cellular Senescence in Head and Neck Squamous Cell Carcinoma

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