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Werner Syndrome Helicase is Required for the Survival of Cancer Cells with Microsatellite Instability.

iScience(2019)SCI 2区

IDEAYA Biosci

Cited 59|Views29
Abstract
Werner syndrome protein (WRN) is a RecQ enzyme involved in the maintenance of genome integrity. Germline loss-of-function mutations in WRN led to premature aging and predisposition to cancer. We evaluated synthetic lethal (SL) interactions between WRN and another human RecQ helicase, BLM, with DNA damage response genes in cancer cell lines. We found that WRN was SL with a DNA mismatch repair protein MutL homolog 1, loss of which is associated with high microsatellite instability (MSI-H). MSI-H cells exhibited increased double-stranded DNA breaks, altered cell cycles, and decreased viability in response to WRN knockdown, in contrast to microsatellite stable (MSS) lines, which tolerated depletion of WRN. Although WRN is the only human RecQ enzyme with a distinct exonuclease domain, only loss of helicase activity drives the MSI SL interaction. This SL interaction in MSI cancer cells positions WRN as a relevant therapeutic target in patients with MSI-H tumors.
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要点】:研究揭示了Werner综合征蛋白(WRN)与DNA错配修复蛋白MutL同源1(MLH1)之间存在合成致死性交互作用,该交互作用在微卫星不稳定性高(MSI-H)的癌细胞中至关重要,为MSI-H肿瘤患者提供了新的治疗靶点。

方法】:通过评估WRN与其他人类RecQ解旋酶BLM以及DNA损伤响应基因在癌细胞系中的合成致死性交互作用。

实验】:在MSI-H和微卫星稳定(MSS)细胞系中对WRN进行敲除,观察细胞的双链DNA断裂增加、细胞周期改变和存活率下降情况,使用的数据集名称未在文中提及。研究发现,仅失去解旋酶活性即可驱动MSI中的合成致死性交互作用。