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PiggyBac transposon tools for recessive screening identify B-cell lymphoma drivers in mice

机译:用于隐性筛选的Piggybac转座子工具鉴定小鼠中的B细胞淋巴瘤司机

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B-cell lymphoma (BCL) is the most common hematologic malignancy. While sequencing studies gave insights into BCL genetics, identification of non-mutated cancer genes remains challenging. Here, we describe PiggyBac transposon tools and mouse models for recessive screening and show their application to study clonal B-cell lymphomagenesis. In a genome-wide screen, we discover BCL genes related to diverse molecular processes, including signaling, transcriptional regulation, chromatin regulation, or RNA metabolism. Cross-species analyses show the efficiency of the screen to pinpoint human cancer drivers altered by non-genetic mechanisms, including clinically relevant genes dysregulated epigenetically, transcriptionally, or post-transcriptionally in human BCL. We also describe a CRISPR/Cas9-based in vivo platform for BCL functional genomics, and validate discovered genes, such as Rfx7, a transcription factor, and Phip, a chromatin regulator, which suppress lymphomagenesis in mice. Our study gives comprehensive insights into the molecular landscapes of BCL and underlines the power of genome-scale screening to inform biology.
机译:B细胞淋巴瘤(BCL)是最常见的血液学恶性肿瘤。虽然测序研究对BCL遗传学的洞察进行了深度,但鉴定不突变的癌症基因仍然具有挑战性。在这里,我们描述了Piggybac转座子工具和小鼠模型,用于隐性筛选,并展示其应用于研究克隆B细胞淋巴瘤的应用。在全基因组屏幕中,我们发现与不同分子过程相关的BCL基因,包括信号传导,转录调节,染色质调控或RNA代谢。交叉物种分析显示屏幕的效率,以确定非遗传机制改变的人类癌症司机,包括在表述,转录或在人BCl中转录的临床相关基因。我们还描述了基于CLC / CAS9的体内平台,用于BCL功能基因组学,并验证发现的基因,例如RFX7,转录因子和PHIP,染色质调节剂,其抑制小鼠中的淋巴瘤。我们的研究为BCL的分子景观提供了全面的见解,并强调了基因组措施筛选的力量来告知生物学。

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