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Time to Bloom

机译:开花时间

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摘要

Bloom Syndrome (BS) is an autosomal recessive disorder due to mutation in Bloom helicase (referred in literature either as BLM helicase or BLM). Patients with BS are predisposed to almost all forms of cancer. BS patients are even today diagnosed in the clinics by hyper-recombination phenotype that is manifested by high rates of Sister Chromatid Exchange. The function of BLM as a helicase and its role during the regulation of homologous recombination (HR) is well characterized. However in the last few years the role of BLM as a DNA damage sensor has been revealed. For example, it has been demonstrated that BLM can stimulate the ATPase and chromatin remodeling activities of RAD54 in vitro. This indicates that BLM may increase the accessibility of the sensor proteins that recognize the lesion. Over the years evidence has accumulated that BLM is one of the earliest proteins that accumulates at the site of the lesion. Finally BLM also acts like a "molecular node" by integrating the upstream signals and acting as a bridge between the transducer and effector proteins (which again includes BLM itself), which in turn repair the DNA damage. Hence BLM seems to be a protein involved in multiple functions - all of which may together contribute to its reported role as a "caretaker tumor suppressor". In this review the recent literature documenting the upstream BLM functions has been elucidated and future directions indicated.
机译:Bloom综合症(BS)是由于Bloom解旋酶(在文献中称为BLM解旋酶或BLM)中的突变引起的常染色体隐性遗传疾病。 BS患者易患几乎所有形式的癌症。如今,甚至在临床上也通过高重组表型诊断出BS患者,这种表型表现出较高的姊妹染色单体交换率。 BLM作为解旋酶的功能及其在同源重组(HR)调节中的作用已得到很好的表征。然而,在最近几年中,已经揭示出BLM作为DNA损伤传感器的作用。例如,已经证明BLM可以在体外刺激RAD54的ATP酶和染色质重塑活性。这表明BLM可能会增加识别病变的传感器蛋白的可及性。多年以来,已有证据表明BLM是最早聚集在病变部位的蛋白质之一。最后,BLM还通过整合上游信号并充当换能器和效应蛋白(又包括BLM本身)之间的桥梁,像“分子节点”一样发挥作用,从而修复DNA损伤。因此,BLM似乎是一种涉及多种功能的蛋白质-所有这些都可能共同促进了其作为“看护肿瘤抑制剂”的作用。在这篇综述中,阐明了上游BLM功能的最新文献,并指出了未来的发展方向。

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