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Non-Bloom syndrome-associated partial and total loss-of-function variants of BLM helicase

机译:非布鲁姆综合征相关的BLM解旋酶的部分和全部功能丧失变异

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摘要

Bloom syndrome (BS) is an autosomal recessive disorder caused by mutations in the RecQ-like DNA helicase BLM, which functions in the maintenance of genome stability. Using a humanized model of Saccharomyces cerevisiae that expresses a chimera of the N terminus of yeast Sgs1 and the C terminus of human BLM from the chromosomal SGS1 locus, we have functionally evaluated 27 BLM alleles that are not currently known to be associated with BS. We identified nine alleles with impaired function when assessed for hypersensitivity to the DNA-damaging agent hydroxyurea (HU). Six of these alleles (P690L, R717T, W803R, Y811C, F857L, G972V) caused sensitivity to HU that was comparable to known BS-associated or helicase-dead alleles, suggesting that they may cause BS and, in the heterozygous state, act as risk factors for cancerogenesis. We also identified three alleles (R791C, P868L, G1120R) that caused intermediate sensitivity to HU; although unlikely to cause BS, these partial loss-of-function alleles may increase risk for cancers or other BS-associated complications if a person is homozygous or compound heterozygous for these alleles or if they carry a known BS-associated allele.
机译:Bloom综合征(BS)是常染色体隐性遗传疾病,由RecQ样DNA解旋酶BLM中的突变引起,该突变在维持基因组稳定性中起作用。使用从酵母Sgs1基因座表达酵母Sgs1的N末端和人BLM的C末端的嵌合体的酿酒酵母的人源化模型,我们已经在功能上评估了27种BLM等位基因,这些等位基因目前尚不与BS相关。当评估对DNA损伤剂羟基脲(HU)的超敏性时,我们鉴定了9个功能受损的等位基因。这些等位基因中的六个(P690L,R717T,W803R,Y811C,F857L,G972V)对HU的敏感性与已知的BS相关或解旋酶死亡的等位基因相当,表明它们可能导致BS,并且在杂合状态下充当致癌的危险因素。我们还鉴定了三个对HU引起中等敏感性的等位基因(R791C,P868L,G1120R)。尽管一个人不太可能引起BS,但是如果一个人对这些等位基因纯合或复合杂合,或者携带已知的BS相关等位基因,则这些部分功能丧失的等位基因可能会增加罹患癌症或其他BS相关并发症的风险。

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