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Selective HDAC1/HDAC2 inhibitors induce neuroblastoma differentiation

机译:选择性HDAC1 / HDAC2抑制剂诱导神经母细胞瘤分化

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While cytotoxic chemotherapy remains the hallmark of cancer treatment, intensive regimens fall short in many malignancies, including high-risk neuroblastoma. One alternative strategy is to therapeutically promote tumor differentiation. We created a gene expression signature to measure neuroblast maturation, adapted it to a high-throughput platform, and screened a diversity oriented synthesis-generated small-molecule library for differentiation inducers. We identified BRD8430, containing a nine-membered lactam, an ortho-amino anilide functionality, and three chiral centers, as a selective class I histone deacetylase (HDAC) inhibitor (HDAC1 > 2 > 3). Further investigation demonstrated that selective HDAC1/HDAC2 inhibition using compounds or RNA interference induced differentiation and decreased viability in neuroblastoma cell lines. Combined treatment with 13-cis retinoic acid augmented these effects and enhanced activation of retinoic acid signaling. Therefore, by applying a chemical genomic screening approach, we identified selective HDAC1/HDAC2 inhibition as a strategy to induce neuroblastoma differentiation.
机译:尽管细胞毒性化学疗法仍然是癌症治疗的标志,但在许多恶性肿瘤(包括高危神经母细胞瘤)中,强化治疗仍未达标。一种替代策略是治疗上促进肿瘤分化。我们创建了一个基因表达特征来测量神经母细胞的成熟度,使其适应于高通量平台,并筛选了用于合成分化诱导剂的,面向多样性的合成小分子文库。我们鉴定出含有九元内酰胺,邻氨基苯胺官能团和三个手性中心的BRD8430作为选择性的I类组蛋白脱乙酰基酶(HDAC)抑制剂(HDAC1> 2> 3)。进一步的研究表明,使用化合物或RNA干扰对HDAC1 / HDAC2进行选择性抑制可诱导神经母细胞瘤细胞系分化并降低活力。 13-顺式视黄酸的联合治疗增强了这些作用,并增强了视黄酸信号的激活。因此,通过应用化学基因组筛选方法,我们确定了选择性HDAC1 / HDAC2抑制作为诱导神经母细胞瘤分化的策略。

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