次黄嘌呤在活的人类细胞中的诱变潜力。
Mutagenic potential of hypoxanthine in live human cells.
作者信息
DeVito Stephen, Woodrick Jordan, Song Linze, Roy Rabindra
机构信息
Department of Oncology, Georgetown Lombardi Comprehensive Cancer Center, Georgetown University, Washington, DC, United States.
Department of Oncology, Georgetown Lombardi Comprehensive Cancer Center, Georgetown University, Washington, DC, United States.
出版信息
Mutat Res. 2017 Oct;803-805:9-16. doi: 10.1016/j.mrfmmm.2017.06.005. Epub 2017 Jun 28.
Hypoxanthine (Hx) is a major DNA lesion generated by deamination of adenine during chronic inflammatory conditions, which is an underlying cause of various diseases including cancer of colon, liver, pancreas, bladder and stomach. There is evidence that deamination of DNA bases induces mutations, but no study has directly linked Hx accumulation to mutagenesis and strand-specific mutations yet in human cells. Using a site-specific mutagenesis approach, we report the first direct evidence of mutation potential and pattern of Hx in live human cells. We investigated Hx-induced mutations in human nonmalignant HEK293 and cancer HCT116 cell lines and found that Hx is mutagenic in both HEK293 and HCT116 cell lines. There is a strand bias for Hx-mediated mutations in both the cell lines; the Hx in lagging strand is more mutagenic than in leading strand. There is also some difference in cell types regarding the strand bias for mutation types; HEK293 cells showed largely deletion (>80%) mutations in both leading and lagging strand and the rest were insertions and A:T→G:C transition mutations in leading and lagging strands, respectively, whereas in HCT116 cells we observed 60% A:T→G:C transition mutations in the leading strand and 100% deletions in the lagging strand. Overall, Hx is a highly mutagenic lesion capable of generating A:T→G:C transitions and large deletions with a significant variation in leading and lagging strands in human cells. In recent meta-analysis study A→G (T→C) mutations were found to be a prominent signature in a variety of cancers, including a majority types that are induced by inflammation. The deletions are known to be a major cause of copy-number variations or CNVs, which is a major underlying cause of many human diseases including mental illness, developmental disorders and cancer. Thus, Hx, a major DNA lesion induced by different deamination mechanisms, has potential to initiate inflammation-driven carcinogenesis in addition to various human pathophysiological consequences.
次黄嘌呤(Hx)是慢性炎症条件下腺嘌呤脱氨基产生的一种主要DNA损伤,是包括结肠癌、肝癌、胰腺癌、膀胱癌和胃癌在内的各种疾病的潜在病因。有证据表明DNA碱基的脱氨基会诱导突变,但尚无研究直接将Hx积累与人类细胞中的诱变和链特异性突变联系起来。使用位点特异性诱变方法,我们报告了活的人类细胞中Hx诱变潜力和模式的首个直接证据。我们研究了Hx在人类非恶性HEK293和癌症HCT116细胞系中诱导的突变,发现Hx在HEK293和HCT116细胞系中均具有诱变作用。两种细胞系中Hx介导的突变都存在链偏向性;滞后链中的Hx比前导链更具诱变作用。在突变类型的链偏向性方面,细胞类型之间也存在一些差异;HEK293细胞在前导链和滞后链中主要表现为缺失(>80%)突变,其余分别为前导链和滞后链中的插入以及A:T→G:C转换突变,而在HCT116细胞中,我们观察到前导链中有60%的A:T→G:C转换突变,滞后链中有100%的缺失。总体而言,Hx是一种高度诱变的损伤,能够在人类细胞中产生A:T→G:C转换和大的缺失,在前导链和滞后链中存在显著差异。在最近的荟萃分析研究中,发现A→G(T→C)突变是多种癌症中的一个显著特征,包括大多数由炎症诱导的类型。已知缺失是拷贝数变异或CNV的主要原因,而CNV是包括精神疾病、发育障碍和癌症在内的许多人类疾病的主要潜在病因。因此,由不同脱氨基机制诱导的主要DNA损伤Hx,除了会导致各种人类病理生理后果外,还具有引发炎症驱动的致癌作用的潜力。
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