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HIV-1感染者CD4+T细胞受体基因多样性特点及其与病毒载量的相关性
引用本文:高占,任国良,宋玉国,贾明明,郑扬,赵全壁,邵一鸣,毕胜利,洪坤学. HIV-1感染者CD4+T细胞受体基因多样性特点及其与病毒载量的相关性[J]. 中华微生物学和免疫学杂志, 2011, 31(5). DOI: 10.3760/cma.j.issn.0254-5101.2011.05.001
作者姓名:高占  任国良  宋玉国  贾明明  郑扬  赵全壁  邵一鸣  毕胜利  洪坤学
作者单位:1. 102206,北京,中国疾病预防控制中心性病艾滋病预防控制中心,传染病预防控制国家重点实验室;132011,北华大学医学部
2. 中国疾病预防控制中心性病艾滋病预防控制中心,传染病预防控制国家重点实验室,北京,102206
3. 北华大学医学部,132011
基金项目:"十一五"重大传染病防治研究项目,973项目
摘    要:目的 分析HIV-1感染者CD4+T细胞受体(TCR)基因的多样性特征及其与病毒载量的相关性.方法 应用抗CD4单克隆抗体从25份HIV-1感染者和10份HIV-1阴性对照样本外周血单个核细胞(PBMC)中分离CD4+T细胞,提取细胞总RNA,然后通过逆转录及巢式多聚酶链反应(nestedPCR)对TCR 22个Vβ基因家族的互补决定区3(CDR3)进行扩增,利用ABI3700测序仪对扩增的PCR产物进行扫描,定最分析HIV-1感染者TCRCDR3区多样性变化特征及其与病毒载量的相关性.结果 HIV-1感染者CD4+T细胞TCR CDR3区平均D(distance)值显著高于正常对照组(P<0 05),TCR Vβ基因各家族CDR3长度谱型成寡克隆分布,TCR CDR3区的紊乱与病毒载量呈正相关(r=0 494,P<0 05);HIV-1感染引起TCR多样性的改变不仅表现在不同Vβ基因家族上,而且也表现在CDR3长度上,其中感染者Vβ8、Vβ22、Vβ23基因家族的变化与正常人差异有统计学意义.结论 HIV-1感染能引起CD4+T细胞TCR基因多样性的减少及高斯(Gaussian)分布的破坏,TCR CDR3区的紊乱与病毒载量呈正相关.
Abstract:
Objective To assess the impact of the virus on the complementary determining region 3 (CDR3) length diversity of T cell receptor(TCR) Vβ repertoires of CD4+ T lymphocytes and to explore its association with viral load in individuals with HIV-1 infection. Methods The TCR repertoire was examined using spectratyping of CDR3 length diversity within CD4+ T cells in HIV infected and healthy adults. Separation of CD4+ T cells from peripheral blood mononuclear cells ( PBMCs) was carried out by using immunomagnetic beads coated with anti-CD4 antibody. Total RNAs from the purified CD4 + T lymphocytes were isolated and used to perform nested-PCR amplifications in CDR3 of 22 TCR gene families. CDR3 diversity and its association with viral load in individuals with HIV-1 infection were analyzed. Results An average diversity for all CDR3 profiles in CD4+ T cells from 25 HIV-infected individuals was significantly different as compared to 10 age-matched healthy donors (P<0.05) with the HIV-infected individuals losing diversity in the CDR3 profiles. There was positive correlation between changes in TCR CDR3 diversity and viral load (r = 0. 494, P < 0. 05). The changes in CDR3 length diversity of Vβ families in HIV-infected individuals, particular in Vβ8, Vβ22, Vβ23 were statistically different from the healthy controls. Conclusion HIV-1 infection might induce the loss of TCR Vp repertoire diversity and disrupt the CDR3 Gaussian distributions within CD4 + T cells. There should be positive correlation between changes in TCR CDR3 diversity and the viral load in HIV-1 infected patients.

关 键 词:CD4+T淋巴细胞  T细胞受体  互补决定区3

Association of T cell receptor diversity of CD4+ T lymphocytes with viral load in individuals with HIV-1 infection
GAO Zhan,REN Guo-liang,SONG Yu-guo,JIA Ming-ming,ZHENG Yang,ZHAO Quan-bi,SHAO Yi-ming,BI Sheng-li,HONG Kun-xue. Association of T cell receptor diversity of CD4+ T lymphocytes with viral load in individuals with HIV-1 infection[J]. Chinese Journal of Microbiology and Immunology, 2011, 31(5). DOI: 10.3760/cma.j.issn.0254-5101.2011.05.001
Authors:GAO Zhan  REN Guo-liang  SONG Yu-guo  JIA Ming-ming  ZHENG Yang  ZHAO Quan-bi  SHAO Yi-ming  BI Sheng-li  HONG Kun-xue
Abstract:Objective To assess the impact of the virus on the complementary determining region 3 (CDR3) length diversity of T cell receptor(TCR) Vβ repertoires of CD4+ T lymphocytes and to explore its association with viral load in individuals with HIV-1 infection. Methods The TCR repertoire was examined using spectratyping of CDR3 length diversity within CD4+ T cells in HIV infected and healthy adults. Separation of CD4+ T cells from peripheral blood mononuclear cells ( PBMCs) was carried out by using immunomagnetic beads coated with anti-CD4 antibody. Total RNAs from the purified CD4 + T lymphocytes were isolated and used to perform nested-PCR amplifications in CDR3 of 22 TCR gene families. CDR3 diversity and its association with viral load in individuals with HIV-1 infection were analyzed. Results An average diversity for all CDR3 profiles in CD4+ T cells from 25 HIV-infected individuals was significantly different as compared to 10 age-matched healthy donors (P<0.05) with the HIV-infected individuals losing diversity in the CDR3 profiles. There was positive correlation between changes in TCR CDR3 diversity and viral load (r = 0. 494, P < 0. 05). The changes in CDR3 length diversity of Vβ families in HIV-infected individuals, particular in Vβ8, Vβ22, Vβ23 were statistically different from the healthy controls. Conclusion HIV-1 infection might induce the loss of TCR Vp repertoire diversity and disrupt the CDR3 Gaussian distributions within CD4 + T cells. There should be positive correlation between changes in TCR CDR3 diversity and the viral load in HIV-1 infected patients.
Keywords:HIV-1
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