Department of Genetics, Yale University School of Medicine, New Haven, CT 06510, USA.
Systems Biology Institute, Yale University School of Medicine, 850 West Campus Drive, West Haven, CT 06516, USA.
Sci Adv. 2018 Feb 28;4(2):eaao5508. doi: 10.1126/sciadv.aao5508. eCollection 2018 Feb.
Cancer genomics consortia have charted the landscapes of numerous human cancers. Whereas some mutations were found in classical oncogenes and tumor suppressors, others have not yet been functionally studied in vivo. To date, a comprehensive assessment of how these genes influence oncogenesis is lacking. We performed direct high-throughput in vivo mapping of functional variants in an autochthonous mouse model of cancer. Using adeno-associated viruses (AAVs) carrying a single-guide RNA (sgRNA) library targeting putative tumor suppressor genes significantly mutated in human cancers, we directly pool-mutagenized the livers of Cre-inducible CRISPR (clustered regularly interspaced short palindromic repeats)-associated protein 9 (Cas9) mice. All mice that received the AAV-mTSG library developed liver cancer and died within 4 months. We used molecular inversion probe sequencing of the sgRNA target sites to chart the mutational landscape of these tumors, revealing the functional consequence of multiple variants in driving liver tumorigenesis in immunocompetent mice. AAV-mediated autochthonous CRISPR screens provide a powerful means for mapping a provisional functional cancer genome atlas of tumor suppressors in vivo.
癌症基因组学联盟已经绘制了许多人类癌症的图谱。虽然一些突变发生在经典的癌基因和肿瘤抑制基因中,但其他突变尚未在体内进行功能研究。迄今为止,缺乏对这些基因如何影响肿瘤发生的全面评估。我们在癌症的同源小鼠模型中进行了功能变异的直接高通量体内作图。使用携带靶向人类癌症中显著突变的假定肿瘤抑制基因的单指导 RNA(sgRNA)文库的腺相关病毒(AAV),我们直接对 Cre 诱导的 CRISPR(成簇的、规则间隔的短回文重复)相关蛋白 9(Cas9)小鼠的肝脏进行了池诱变。所有接受 AAV-mTSG 文库的小鼠都患上了肝癌,并在 4 个月内死亡。我们使用 sgRNA 靶位点的分子倒置探针测序来绘制这些肿瘤的突变图谱,揭示了多种变体在驱动免疫活性小鼠肝肿瘤发生中的功能后果。AAV 介导的同源 CRISPR 筛选为在体内绘制暂定的肿瘤抑制因子功能性癌症基因组图谱提供了一种强大的手段。
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