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Supplementary Material for: Identification of a splicing variant c.3813-3A>G in NPHP3 by reanalysis of whole exome sequencing in a Chinese boy with nephronophthisis|遗传疾病数据集|基因测序数据集

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Mendeley Data2024-06-25 更新2024-06-27 收录
遗传疾病
基因测序
下载链接:
https://karger.figshare.com/articles/dataset/Supplementary_Material_for_Identification_of_a_splicing_variant_c_3813-3A_G_in_NPHP3_by_reanalysis_of_whole_exome_sequencing_in_a_Chinese_boy_with_nephronophthisis/22220179/1
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资源简介:
Nephronophthisis is an autosomal recessive cystic kidney disease characterized by tubular injury and commonly results in kidney failure. We reported a case of 4-year-old Chinese boy presented with severe anemia, kidney and liver dysfunction. Whole exome sequencing (WES) was performed to identify the candidate variant with a negative result initially. After complete collection of clinical information, reanalysis of WES identified a homozygous NPHP3 variant c.3813-3A>G (NM_153240.4). The effect on mRNA splicing of the intronic variant was predicted through software (three in silico splice tools). Furthermore, in vitro minigene assay was conducted to validate the predicted deleterious effects of the intronic variant. All of the splice prediction programs and minigene assay indicated that the variant had an impact on the normal splicing pattern of NPHP3. Our study confirmed the effect of the c.3813-3A>G variant on NPHP3 splicing in vitro, which gives additional evidence for the clinical significance of the variant and provides a basis for genetic diagnosis of nephronophthisis 3. In addition, we think that it is essential to reanalyze WES data after the complete clinical information collection to avoid missing some important candidate variants.
创建时间:
2023-06-28
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