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Query: UMLS:C0279530 (
bone cancer
)
1,036
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Ewing sarcoma (EwS) is an aggressive pediatric
bone cancer
in need of more effective therapies than currently available. Most research into novel targeted therapeutic approaches is focused on the fusion oncogene
EWSR1
-FLI1
, which is the genetic hallmark of this disease. In this study, a broad range of 3,325 experimental compounds, among them FDA approved drugs and natural products, were screened for their effect on EwS cell viability depending on EWS-FLI1 expression. In a network-based approach we integrated the results from drug perturbation screens and RNA sequencing, comparing EWS-FLI1-high (normal expression) with EWS-FLI1-low (knockdown) conditions, revealing novel interactions between compounds and EWS-FLI1 associated biological processes. The top candidate list of druggable EWS-FLI1 targets included genes involved in translation, histone modification, microtubule structure, topoisomerase activity as well as apoptosis regulation. We confirmed our
in silico
results using viability and apoptosis assays, underlining the applicability of our integrative and systemic approach. We identified differential sensitivities of Ewing sarcoma cells to BCL-2 family inhibitors dependent on the EWS-FLI1 regulome including altered MCL-1 expression and subcellular localization. This study facilitates the selection of effective targeted approaches for future combinatorial therapies of patients suffering from Ewing sarcoma.
...
PMID:Identifying the druggable interactome of EWS-FLI1 reveals MCL-1 dependent differential sensitivities of Ewing sarcoma cells to apoptosis inducers. 3012 24
Ewing's sarcoma (EWS) is a
bone cancer
arising predominantly in young children.
EWSR1
(Ewing Sarcoma breakpoint region 1/EWS RNA binding protein 1) gene is ubiquitously expressed in most cell types, indicating it has diverse roles in various cellular processes and organ development. Recently, several studies have shown that missense mutations of
EWSR1
genes are known to be associated with central nervous system disorders such as amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). Otherwise,
EWSR1
plays epigenetic roles in gene expression, RNA processing, and cellular signal transduction. Interestingly,
EWSR1
controls micro RNA (miRNA) levels via Drosha, leading to autophagy dysfunction and impaired dermal development. Ewsr1 deficiency also leads to premature senescence of blood cells and gamete cells with a high rate of apoptosis due to the abnormal meiosis. Despite these roles of
EWSR1
in various cellular functions, the exact mechanisms are not yet understood. In this context, the current review overviews a large body of evidence and discusses on what
EWSR1
genetic mutations are associated with brain diseases and on how
EWSR1
modulates cellular function via the epigenetic pathway. This will provide a better understanding of bona fide roles of
EWSR1
in aging and its association with brain disorders.
...
PMID:EWSR1, a multifunctional protein, regulates cellular function and aging via genetic and epigenetic pathways. 3048 90
Ewing sarcoma is a pediatric
bone cancer
that expresses the chimeric protein
EWSR1
/FLI1. We previously demonstrated that
EWSR1
/FLI1 impairs the localization of Aurora B kinase to the midzone (the midline structure located between segregating chromosomes) during anaphase. While localization of Aurora B is essential for faithful cell division, it is unknown whether interference with midzone organization by
EWSR1
/FLI1 induces aneuploidy. To address this, we generated stable Tet-on inducible cell lines with
EWSR1
/FLI1, using CRISPR/Cas9 technology to integrate the transgene at the safe-harbor AAVS1 locus in DLD-1 cells. Induced cells expressing
EWSR1
/FLI1 displayed an increased incidence of aberrant localization of Aurora B, and greater levels of aneuploidy, compared to non-induced cells. Furthermore, the expression of
EWSR1
/FLI1-T79A, containing a threonine (Thr) to alanine (Ala) substitution at amino acid 79, failed to induce these phenotypes, indicating that Thr 79 is critical for
EWSR1
/FLI1 interference with mitosis. In contrast, the phosphomimetic mutant
EWSR1
/FLI1-T79D (Thr to aspartic acid (Asp)) retained the high activity as wildtype
EWSR1
/FLI1. Together, these findings suggest that phosphorylation of
EWSR1
/FLI1 at Thr 79 promotes the co-localization of
EWSR1
/FLI1 and Aurora B on the chromosomes during prophase and metaphase, and in addition, impairs the localization of Aurora B during anaphase, leading to induction of aneuploidy. This is the first demonstration of the mechanism for
EWSR1
/FLI1-dependent induction of aneuploidy associated with mitotic dysfunction, and the identification of the phosphorylation of the Thr 79 of
EWSR1
/FLI1 as a critical residue required for this induction.
...
PMID:Chromosomal localization of Ewing sarcoma EWSR1/FLI1 protein promotes the induction of aneuploidy. 3329 70
