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马兜铃酸的全基因组突变特征及其作为筛选工具的应用。

Genome-wide mutational signatures of aristolochic acid and its application as a screening tool.

机构信息

NCCS-VARI Translational Research Laboratory, Division of Medical Sciences, National Cancer Centre Singapore, 11 Hospital Drive, Singapore 169610, Singapore.

出版信息

Sci Transl Med. 2013 Aug 7;5(197):197ra101. doi: 10.1126/scitranslmed.3006086.

Abstract

Aristolochic acid (AA), a natural product of Aristolochia plants found in herbal remedies and health supplements, is a group 1 carcinogen that can cause nephrotoxicity and upper urinary tract urothelial cell carcinoma (UTUC). Whole-genome and exome analysis of nine AA-associated UTUCs revealed a strikingly high somatic mutation rate (150 mutations/Mb), exceeding smoking-associated lung cancer (8 mutations/Mb) and ultraviolet radiation-associated melanoma (111 mutations/Mb). The AA-UTUC mutational signature was characterized by A:T to T:A transversions at the sequence motif A[C|T]AGG, located primarily on nontranscribed strands. AA-induced mutations were also significantly enriched at splice sites, suggesting a role for splice-site mutations in UTUC pathogenesis. RNA sequencing of AA-UTUC confirmed a general up-regulation of nonsense-mediated decay machinery components and aberrant splicing events associated with splice-site mutations. We observed a high frequency of somatic mutations in chromatin modifiers, particularly KDM6A, in AA-UTUC, demonstrated the sufficiency of AA to induce renal dysplasia in mice, and reproduced the AA mutational signature in experimentally treated human renal tubular cells. Finally, exploring other malignancies that were not known to be associated with AA, we screened 93 hepatocellular carcinoma genomes/exomes and identified AA-like mutational signatures in 11. Our study highlights an unusual genome-wide AA mutational signature and the potential use of mutation signatures as "molecular fingerprints" for interrogating high-throughput cancer genome data to infer previous carcinogen exposures.

摘要

马兜铃酸(Aristolochic acid,AA)是一种天然产物,存在于草药疗法和保健品中的马兜铃属植物中,属于 1 类致癌物质,可导致肾毒性和上尿路尿路上皮细胞癌(UTUC)。对 9 例 AA 相关 UTUC 的全基因组和外显子组分析显示,体细胞突变率极高(150 个突变/Mb),超过与吸烟相关的肺癌(8 个突变/Mb)和与紫外线辐射相关的黑色素瘤(111 个突变/Mb)。AA-UTUC 的突变特征是序列基序 A[C|T]AGG 处的 A:T 到 T:A 颠换,主要位于非转录链上。AA 诱导的突变在剪接位点也明显富集,提示剪接位点突变在 UTUC 发病机制中起作用。AA-UTUC 的 RNA 测序证实了无意义介导的衰变机制成分和与剪接位点突变相关的异常剪接事件的普遍上调。我们观察到染色质修饰物中的体细胞突变频率很高,特别是 AA-UTUC 中的 KDM6A,并证明 AA 足以在小鼠中诱导肾发育不良,并在实验处理的人肾小管细胞中重现 AA 突变特征。最后,我们探索了其他尚未被认为与 AA 相关的恶性肿瘤,筛选了 93 例肝细胞癌基因组/外显子组,并在 11 例中鉴定出 AA 样突变特征。我们的研究强调了一种不寻常的全基因组 AA 突变特征,以及突变特征作为“分子指纹”用于研究高通量癌症基因组数据以推断以前的致癌物暴露的潜在用途。

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