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首页> 外文期刊>Human Genetics >IFT88 mutations identified in individuals with non-syndromic recessive retinal degeneration result in abnormal ciliogenesis
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IFT88 mutations identified in individuals with non-syndromic recessive retinal degeneration result in abnormal ciliogenesis

机译:IFT88在具有非综合症隐性视网膜变性的个体中鉴定的突变导致纤毛发生异常

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摘要

Whole genome sequencing (WGS) was performed to identify the variants responsible for inherited retinal degeneration (IRD) in a Caucasian family. Segregation analysis of selected rare variants with pathogenic potential identified a set of compound heterozygous changes p.Arg266*:c.796C T and p.Ala568Thr:c.1702G A in the intraflagellar transport protein-88 (IFT88) gene segregating with IRD. Expression of IFT88 with the p.Arg266* and p.Ala568Thr mutations in mIMDC3 cells by transient transfection and in HeLa cells by introducing the mutations using CRISPR-cas9 system suggested that both mutations result in the formation of abnormal ciliary structures. The introduction of the IFT88 p.Arg266* variant in the homozygous state in HeLa cells by CRISPR-Cas9 genome-editing revealed that the mutant transcript undergoes nonsense-mediated decay leading to a significant depletion of IFT88 transcript. Additionally, abnormal ciliogenesis was observed in these cells. These observations suggest that the rare and unique combination of IFT88 alleles observed in this study provide insight into the physiological role of IFT88 in humans and the likely mechanism underlying retinal pathology in the pedigree with IRD.
机译:进行全基因组测序(WGS)以确定一个高加索家族中与遗传性视网膜变性(IRD)有关的变异体。对选定的具有致病潜力的罕见变异进行分离分析,确定了一组复合杂合子变化p.Arg266*:c.796C;T和p.Ala568Thr:c.1702G;在与IRD分离的鞭毛内运输蛋白-88(IFT88)基因中。通过瞬时转染在mIMDC3细胞中表达带有p.Arg266*和p.Ala568Thr突变的IFT88,通过使用CRISPR-cas9系统引入突变在HeLa细胞中表达表明,这两种突变都会导致异常睫状体结构的形成。通过CRISPR-Cas9基因组编辑在HeLa细胞中以纯合状态引入IFT88 p.Arg266*变体表明,突变转录本经历无义介导的衰变,导致IFT88转录本显著缺失。此外,在这些细胞中观察到异常纤毛形成。这些观察结果表明,本研究中观察到的罕见且独特的IFT88等位基因组合为深入了解IFT88在人类中的生理作用以及IRD家系视网膜病理学的可能机制提供了依据。

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  • 来源
    《Human Genetics》 |2018年第7期|共12页
  • 作者

    Chekuri Anil; Guru Aditya A.; Biswas Pooja; Branham Kari; Borooah Shyamanga; Soto-Hermida Angel; Hicks Michael; Khan Naheed W.; Matsui Hiroko; Alapati Akhila; Raghavendra Pongali B.; Roosing Susanne; Sarangapani Sripriya; Mathavan Sinnakaruppan; Telenti Amalio; Heckenlively John R.; Riazuddin S. Amer; Frazer Kelly A.; Sieving Paul A.; Ayyagari Radha;

  • 作者单位

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

    Univ Michigan Kellogg Eye Ctr Ophthalmol &

    Visual Sci Ann Arbor MI 48109 USA;

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

    Human Longev Inc San Diego CA USA;

    Univ Michigan Kellogg Eye Ctr Ophthalmol &

    Visual Sci Ann Arbor MI 48109 USA;

    Univ Calif San Diego Inst Genom Med La Jolla CA 92093 USA;

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

    REVA Univ Sch Biotechnol Bengaluru Karnataka India;

    Radboud Univ Nijmegen Med Ctr Dept Human Genet POB 9101 NL-6500 HB Nijmegen Netherlands;

    Sankara Nethralaya Vis Res Fdn 41 Coll Rd Madras Tamil Nadu India;

    Sankara Nethralaya Vis Res Fdn 41 Coll Rd Madras Tamil Nadu India;

    Human Longev Inc San Diego CA USA;

    Univ Michigan Kellogg Eye Ctr Ophthalmol &

    Visual Sci Ann Arbor MI 48109 USA;

    Johns Hopkins Univ Sch Med Wilmer Eye Inst Baltimore MD 21205 USA;

    Univ Calif San Diego Inst Genom Med La Jolla CA 92093 USA;

    NEI NIH Bethesda MD 20892 USA;

    Univ Calif San Diego Shiley Eye Inst 9415 Campus Point Dr JRC 206 La Jolla CA 92093 USA;

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  • 正文语种 eng
  • 中图分类 医学遗传学;
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