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Altered RECQL5 expression in urothelial bladder carcinoma increases cellular proliferation and makes RECQL5 helicase activity a novel target for chemotherapy

机译:尿路上皮膀胱癌中RECQL5表达的改变会增加细胞增殖并使RECQL5解旋酶活性成为化疗的新靶标

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摘要

RECQ helicases are a family of enzymes with both over lapping and unique functions. Functional autosomal recessive loss of three members of the family BLM, WRN and RECQL4, results in hereditary human syndromes characterized by cancer predisposition and premature aging, but despite the finding that RECQL5 deficient mice are cancer prone, no such link has been made to human RECQL5. Here we demonstrate that human urothelial carcinoma of the bladder (UCC) has increased expression of RECQL5 compared to normal bladder tissue and that increasing RECQL5 expression can drive proliferation of normal bladder cells and is associated with poor prognosis. Further, by expressing a helicase dead RECQL5 and by depleting bladder cancer cells of RECQL5 we show that inhibition of RECQL5 activity has potential as a new target for treatment of UCC.
机译:RECQ解旋酶是具有重叠作用和独特功能的酶家族。 BLM,WRN和RECQL4家族三个成员的功能性常染色体隐性遗传丧失导致遗传性人类综合征,其特征是癌症易感性和过早衰老,但是尽管发现RECQL5缺陷型小鼠易患癌症,但与人类RECQL5的联系尚未建立。在这里,我们证明,与正常膀胱组织相比,人膀胱尿路上皮癌(UCC)的RECQL5表达增加,并且增加的RECQL5表达可以驱动正常膀胱细胞增殖,并与不良预后相关。此外,通过表达解旋酶死亡的RECQL5并耗尽RECQL5的膀胱癌细胞,我们表明抑制RECQL5活性具有作为治疗UCC的新靶标的潜力。

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