Therapeutic vulnerabilities in the DNA damage response for the treatment of ATRX mutant neuroblastoma

DNA 损伤反应在 ATRX 突变型神经母细胞瘤治疗中的治疗脆弱性

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作者：Sally L George, Federica Lorenzi, David King, Sabine Hartlieb, James Campbell, Helen Pemberton, Umut H Toprak, Karen Barker, Jennifer Tall, Barbara Martins da Costa, Marlinde L van den Boogaard, M Emmy M Dolman, Jan J Molenaar, Helen E Bryant, Frank Westermann, Christopher J Lord, Louis Chesler

期刊：

EBioMedicine

影响因子：

9.700

时间：

2020

起止号：

2020 Sep:59:102971.

doi：

10.1016/j.ebiom.2020.102971

研究方向：

神经

细胞类型：

其它细胞

Background

In neuroblastoma, genetic alterations in ATRX, define a distinct poor outcome patient subgroup. Despite the need for new therapies, there is a lack of available models and a dearth of pre-clinical research.

Methods

To evaluate the impact of ATRX loss of function (LoF) in neuroblastoma, we utilized CRISPR-Cas9 gene editing to generate neuroblastoma cell lines isogenic for ATRX. We used these and other models to identify therapeutically exploitable synthetic lethal vulnerabilities associated with ATRX LoF. Findings: In isogenic cell lines, we found that ATRX inactivation

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