Abdelrahman Ibrahim, Edwin Lin, Mack Hinckley, Mazdak Khalighi, Zena Altawallbeh, Daher Al-Rabadi, Zakariya Al-Hassanat, Marcus G Pezzolesi, Martin C Gregory, Laith Al-Rabadi
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引用次数: 0
摘要
背景:Alport综合征(AS)是一种以进行性肾脏疾病、听力缺陷和眼部异常为特征的遗传性疾病。本研究调查了具有相同常染色体基因突变的COL4A3个体的表型变异性,并探讨了修饰基因的潜在影响。该研究的重点是三个携带相同COL4A3突变(c.2083G>A, p.Gly695Arg)但表现出表型差异的家族。目的是阐明家族间和家族内的变异,并确定导致这些差异的潜在遗传修饰因子。方法:对犹他大学一个队列中的三个家庭进行研究。在知情同意的情况下收集临床资料、血液、尿液和组织样本。使用SureSelect Human All Exon Target Enrichment System进行全外显子测序(WES)以鉴定遗传变异。用GATK、VEP和PEDDY进行变异调用和标注。使用变异注释、分析和搜索工具(VAAST)、pVAAST和表型驱动变异本体重新排序工具(PHEVOR)实现疾病基因优先级。利用公共数据库进行共分离分析和功能标注,鉴定出修饰基因。结果:该研究突出了具有相同COL4A3突变的家族内部和家族之间显著的表型变异性。单个突变的个体通常表现为轻微的表型,如孤立性血尿,而复合杂合子和基因病例表现为严重的表型,包括蛋白尿、听力损失和慢性肾病(CKD)。修饰基因如GRIP1、CCND1和CYP3A7被鉴定并与表型变异性相关联,表明它们在疾病进展中的潜在作用。结论:研究结果强调了遗传修饰因子在影响AS表型变异性中的作用。了解这些修饰因子对于个性化治疗策略和遗传咨询至关重要。未来的研究应该通过功能研究和更大的队列来验证这些候选基因,以加强临床护理和改善对AS患者的预后预测。
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