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生成并鉴定 ABCB4 基因敲除斑马鱼模型,该基因编码人类多药外排转运蛋白 P-糖蛋白的同源物。

Generation and characterization of a zebrafish knockout model of abcb4, a homolog of the human multidrug efflux transporter P-glycoprotein.

机构信息

Department of Molecular Physiology and Biophysics, Vanderbilt University, 2215 Garland Ave, Nashville, TN, 37240, USA.

Department of Chemical and Biomolecular Engineering, Vanderbilt University, Nashville, TN, USA.

出版信息

Hum Genomics. 2023 Sep 6;17(1):84. doi: 10.1186/s40246-023-00530-3.

Abstract

The ATP-binding cassette subfamily B member 1 (ABCB1), encoding a multidrug transporter referred to as P-glycoprotein (Pgp), plays a critical role in the efflux of xenobiotics in humans and is implicated in cancer resistance to chemotherapy. Therefore, developing high-throughput animal models to screen for Pgp function and bioavailability of substrates and inhibitors is paramount. Here, we generated and validated a zebrafish knockout line of abcb4, a human Pgp transporter homolog. CRISPR/Cas9 genome editing technology was deployed to generate a frameshift mutation in exon 4 of zebrafish abcb4. The zebrafish abcb4 homozygous mutant exhibited elevated accumulation of fluorescent rhodamine 123, a substrate of human Pgp, in the intestine and brain area of embryos. Moreover, abcb4 knockout embryos were sensitized toward toxic compounds such as doxorubicin and vinblastine compared to the WT zebrafish. Immunostaining for zebrafish Abcb4 colocalized in the endothelial brain cells of adult zebrafish. Transcriptome profiling using Gene Set Enrichment Analysis uncovered that the 'cell cycle process,' 'mitotic cell cycles,' and 'microtubule-based process' were significantly downregulated in the abcb4 knockout brain with age. This study establishes and validates the abcb4 knockout zebrafish as an animal model to study Pgp function in vivo. Unexpectedly it reveals a potentially novel role for zebrafish abcb4 in age-related changes in the brain. The zebrafish lines generated here will provide a platform to aid in the discovery of modulators of Pgp function as well as the characterization of human mutants thereof.

摘要

ATP 结合盒亚家族 B 成员 1(ABCB1),编码一种称为 P-糖蛋白(Pgp)的多药转运蛋白,在人类中外源物质的外排中发挥关键作用,并且与癌症对化疗的耐药性有关。因此,开发高通量动物模型以筛选 Pgp 功能以及底物和抑制剂的生物利用度至关重要。在这里,我们生成并验证了一种斑马鱼 abcb4 的敲除系,abcb4 是人类 Pgp 转运蛋白同源物。CRISPR/Cas9 基因组编辑技术被用于在斑马鱼 abcb4 的外显子 4 中产生移码突变。斑马鱼 abcb4 纯合突变体在胚胎的肠道和大脑区域中表现出荧光罗丹明 123(人 Pgp 的底物)的积累增加。此外,与 WT 斑马鱼相比,abcb4 敲除胚胎对多柔比星和长春新碱等有毒化合物更加敏感。斑马鱼 Abcb4 的免疫染色在成年斑马鱼的内皮脑细胞中发生共定位。使用基因集富集分析进行转录组谱分析发现,abcb4 敲除脑的“细胞周期过程”、“有丝分裂细胞周期”和“基于微管的过程”随年龄显著下调。这项研究建立并验证了 abcb4 敲除斑马鱼作为体内研究 Pgp 功能的动物模型。出乎意料的是,它揭示了斑马鱼 abcb4 在与年龄相关的大脑变化中可能具有新的作用。这里生成的斑马鱼系将为发现 Pgp 功能调节剂以及表征人类突变体提供一个平台。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7da0/10481557/09e3a94cb68c/40246_2023_530_Fig1_HTML.jpg

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