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Identified OAS OAS 3 gene variants associated with coexistence of HB HB sAg and anti‐ HB HB s in chronic HBV HBV infection

机译:鉴定了与慢性HBV HBV感染的HB HB下垂和抗HB HB S相关联的OAS OAS 3基因变体

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Summary The underlying mechanism of coexistence of hepatitis B surface antigen ( HB sAg) and hepatitis B surface antigen antibody (anti‐ HB s) is still controversial. To identify the host genetic factors related to this unusual clinical phenomenon, a two‐stage study was conducted in the Chinese Han population. In the first stage, we performed a case‐control (1:1) age‐ and gender‐matched study of 101 cases with concurrent HB sAg and anti‐ HB s and 102 controls with negative HB sAg and positive anti‐ HB s using whole exome sequencing. In the second validation stage, we directly sequence the 16 exons on the OAS 3 gene in two dependent cohorts of 48 cases and 200 controls. Although, in the first stage, a genome‐wide association study of 58,563 polymorphism variants in 101 cases and 102 controls found no significant loci ( P ‐value?≤?.05/58563), and neither locus achieved a conservative genome‐wide significance threshold ( P ‐value?≤?5e‐08), gene‐based burden analysis showed that OAS 3 gene rare variants were associated with the coexistence of HB sAg and anti‐ HB s. ( P ‐value?=?4.127e‐06?≤?0.05/6994). A total of 16 rare variants were screened out from 21 cases and 3 controls. In the second validation stage, one case with a stop‐gained rare variant was identified. Fisher’s exact test of all 149 cases and 302 controls showed that the rare coding sequence mutations were more frequent in cases vs controls ( P ‐value?=?7.299e‐09, OR ?=?17.27, 95% CI [5.01‐58.72]). Protein‐coding rare variations on the OAS 3 gene are associated with the coexistence of HB sAg and anti‐ HB s in patients with chronic HBV infection in Chinese Han population.
机译:乙型肝炎表面抗原(HB-sAg)和乙型肝炎表面抗原抗体(抗-HB-s)共存的潜在机制仍有争议。为了确定与这种异常临床现象相关的宿主遗传因素,在中国汉族人群中进行了一项两阶段研究。在第一阶段,我们使用全外显子组测序对101例同时患有HB sAg和抗HB s的病例和102例HB sAg阴性和抗HB s阳性的对照进行了病例对照(1:1)年龄和性别匹配研究。在第二个验证阶段,我们在48例病例和200例对照的两个依赖队列中直接对OAS 3基因的16个外显子进行测序。尽管在第一阶段,对101个病例和102个对照组的58563个多态性变体进行了全基因组关联研究,但没有发现显著的位点(P值?≤?.05/58563),两个位点均未达到保守的全基因组显著性阈值(P值?≤?5e-08),基于基因的负荷分析表明OAS 3基因罕见变异与HB sAg和抗HB s共存相关(P值?=4.127e-06?≤?0.05/6994). 从21例病例和3例对照中筛选出16种罕见变异。在第二个验证阶段,发现了一例具有停止获得罕见变异的病例。Fisher对所有149个病例和302个对照组进行的精确测试表明,病例组与对照组相比,罕见的编码序列突变更频繁(P值?=7.299e-09,或?=17.27,95%可信区间[5.01-58.72])。在中国汉族慢性HBV感染患者中,OAS 3基因上编码蛋白质的罕见变异与HB sAg和抗HB s共存有关。

著录项

  • 来源
    《Journal of viral hepatitis.》 |2018年第8期|共7页
  • 作者单位

    Department of Infectious DiseasesPeking University First HospitalBeijing China;

    Department of Medical Genetics and Developmental BiologyCapital Medical UniversityBeijing China;

    Department of Infectious DiseasesPeking University First HospitalBeijing China;

    Center for GeneticsNational Research Institute for Family PlanningBeijing China;

    Center for GeneticsNational Research Institute for Family PlanningBeijing China;

    Center for GeneticsNational Research Institute for Family PlanningBeijing China;

    BGI‐ShenzhenShenzhen China;

    BGI‐ShenzhenShenzhen China;

    BGI‐ShenzhenShenzhen China;

    BGI‐ShenzhenShenzhen China;

    Theodosius Dobzhansky Center for Genome BioinformaticsSt. Petersburg State UniversitySt. Petersburg;

    Theodosius Dobzhansky Center for Genome BioinformaticsSt. Petersburg State UniversitySt. Petersburg;

    Department of Laboratory MedicinesPeking University First HospitalBeijing China;

    Department of Laboratory MedicinesPeking University First HospitalBeijing China;

    The Fifth Hospital of ShijiazhuangShijiazhuang China;

    The Fifth Hospital of ShijiazhuangShijiazhuang China;

    Department of Infectious DiseasesPeking University First HospitalBeijing China;

    Department of Infectious DiseasesPeking University First HospitalBeijing China;

    Department of Infectious DiseasesPeking University First HospitalBeijing China;

    Center for GeneticsNational Research Institute for Family PlanningBeijing China;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 传染病;
  • 关键词

    coexistence of HB sAg and anti‐ HB s; OAS 3; rare variants; whole exome sequencing;

    机译:HB-sAg和抗-HB-s共存;美洲国家组织3;罕见变种;全外显子组测序;

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