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Small-molecule screen identifies modulators of EWS/FLI1 target gene expression and cell survival in Ewing's sarcoma

机译:小分子筛查可识别Ewing / FLI1靶基因表达调节剂和尤因肉瘤中的细胞存活率

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摘要

Ewing's sarcoma family of tumors (EFT) is characterized by the presence of chromosomal translocations leading to the expression of oncogenic transcription factors such as, in the majority of cases, EWS/FLI1. Because of its key role in Ewing's sarcoma development and maintenance, EWS/FLI1 represents an attractive therapeutic target. Here, we characterize PHLDA1 as a novel direct target gene whose expression is repressed by EWS/FLI1. Using this gene and additional specific well-characterized target genes such as NROB1, NKX2.2 and CAV1, all activated by EWS/FLI1, as a read-out system, we screened a small-molecule compound library enriched for FDA-approved drugs that modulated the expression of EWS/FLI1 target genes. Among a hit-list of nine well-known drugs such as camptothecin, fenretinide, etoposide and doxorubicin, we also identified the kinase inhibitor midostaurin (PKC412). Subsequent experiments demonstrated that midostaurin is able to induce apoptosis in a panel of six Ewing's sarcoma cell lines in vitro and can significantly suppress xenograft tumor growth in vivo. These results suggest that midostaurin might be a novel drug that is active against Ewing's cells, which might act by modulating the expression of EWS/FLI1 target genes.
机译:尤因氏肉瘤家族(EFT)的特征是存在染色体易位,导致致癌转录因子(在大多数情况下为EWS / FLI1)表达。由于EWS / FLI1在尤因氏肉瘤的发展和维持中起着关键作用,因此它是一个有吸引力的治疗靶标。在这里,我们将PHLDA1表征为一种新型的直接靶基因,其表达被EWS / FLI1抑制。使用该基因以及其他均被EWS / FLI1激活的,特征明确的靶基因(如NROB1,NKX2.2和CAV1)作为读出系统,我们筛选了一个富含FDA批准药物的小分子化合物文库调节EWS / FLI1靶基因的表达。在喜树碱,fenretinide,依托泊苷和阿霉素等9种知名药物的畅销书中,我们还鉴定了激酶抑制剂Midostaurin(PKC412)。随后的实验表明米多骨蛋白能够在体外诱导一组六个尤因氏肉瘤细胞系中的凋亡,并可以在体内显着抑制异种移植肿瘤的生长。这些结果表明,米ostaurin可能是一种对Ewing细胞具有活性的新型药物,它可能通过调节EWS / FLI1靶基因的表达起作用。

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