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SARS患者康复期T细胞亚群、活化状态及TCRVβ表达格局的分析 被引量:1
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作者 曾星 蔡萃 +2 位作者 黄羽 欧爱华 张娴 《细胞与分子免疫学杂志》 CAS CSCD 北大核心 2005年第1期114-117,共4页
目的: 研究中西医结合治疗后, SARS患者康复期淋巴细胞功能状态和T细胞受体(TCR)Vβ24个亚家族表达的格局。方法: 应用流式细胞分析技术, 观察我院 76例康复期患者T细胞亚群, T、B细胞的活化状态及CD3+和TCRVβ1、2、3、4、5. 1、5. 2、... 目的: 研究中西医结合治疗后, SARS患者康复期淋巴细胞功能状态和T细胞受体(TCR)Vβ24个亚家族表达的格局。方法: 应用流式细胞分析技术, 观察我院 76例康复期患者T细胞亚群, T、B细胞的活化状态及CD3+和TCRVβ1、2、3、4、5. 1、5. 2、5. 3、7. 1、7. 2、8、9、11、12、13. 1、13. 2、13. 6、14、16、17、18、20、21. 3、22及 23等 24个亚家族的表达。结果: T细胞亚群中, CD3+和CD4+ T细胞的百分率均数低于参考值; CD8+ T细胞的百分率高于参考值。CD8+ /CD28- T细胞(Ts)的百分率较参考值增高; 而CD8+ /CD28+ T细胞(Tc)的百分率较参考值降低, 其中有 39例Tc细胞的百分率降低, 有 48例Ts细胞的百分率升高。CD3+HLA DR+和CD3- /HLA DR+细胞的百分率高于正常参考值,增加的例数分别是 36例和 30例。TCRVβ24个亚家族中,TCRVβ14的表达最高, TCRVβ5. 3和 23的表达次之, 表现出TCRVβ呈优势表达。正常对照组TCRVβ24个亚家族中,只TCRVβ14的表达最高, 与SARS患者的结果相一致; 但TCRVβ24个亚家族的分布格局不一样。两组比较, Vβ1、Vβ5. 2、Vβ5. 3、Vβ7. 2、Vβ9、Vβ11、Vβ13. 1、Vβ13. 2、Vβ17、Vβ18、Vβ22和Vβ23表达有显著性差异, 康复期SARS患者组均高于正常对照组。同时, SARS患者激素用? 展开更多
关键词 SARS 康复期 T细胞亚群 tcr 24亚家族
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Characterization of human αβTCR repertoire and discovery of D-D fusion in TCRβ chains 被引量:1
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作者 Peipei Liu Di Liu +11 位作者 Xi Yang Jing Gaoai Ma3, Fangqing Zhaos, Xuyu Zhou~'2~, George F. Gao1'2'4'5~, Baoli Zhu~'2~ Yan Chen Xue Xiao Fei Liu Jing Zou Jun Wu Juncai Ma Fangqing Zhao Xuyu Zhou George F. Gao Baoli Zhu 《Protein & Cell》 SCIE CAS CSCD 2014年第8期603-615,共13页
The characterization of the human T-cell receptor (TCR) repertoire has made remarkable progress, with most of the work focusing on the TCRβ chains. Here, we ana- lyzed the diversity and complexity of both the TCRa ... The characterization of the human T-cell receptor (TCR) repertoire has made remarkable progress, with most of the work focusing on the TCRβ chains. Here, we ana- lyzed the diversity and complexity of both the TCRa and TCRβ repertoires of three healthy donors. We found that the diversity of the TCRα repertoire is higher than that of the TCRβ repertoire, whereas the usages of the V and J genes tended to be preferential with similar TRAV and TRAJ patterns in all three donors. The V-J pairings, like the V and J gene usages, were slightly preferential. We also found that the TRDV1 gene rearranges with the majority of TRAJ genes, suggesting that TRDV1 is a shared TRAV/DV gene (TRAV42/DV1). Moreover, we uncovered the presence of tandem TRBD (TRB D gene) usage in -2% of the productive human TCRβ CDR3 sequences. 展开更多
关键词 tcr repertoire next-generationsequencing v/J usage v-J pairing CDR3 D-D fusion
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Changes in the T-cell receptor Vβ gene repertoire after allogeneic hematopoietic stem cell transplantation 被引量:6
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作者 刘启发 李扬秋 +6 位作者 杨冬 张钰 杨力建 陈少华 孙竞 刘晓力 周淑芸 《Chinese Medical Journal》 SCIE CAS CSCD 2004年第3期413-418,共6页
Background We distinguished graft-versus-host disease (GVHD) from graft-versus-leukemia (GVL) effects and to investigate the distribution of T-cell receptor (TCR) Vβ gene repertoire in individuals with leukemia befor... Background We distinguished graft-versus-host disease (GVHD) from graft-versus-leukemia (GVL) effects and to investigate the distribution of T-cell receptor (TCR) Vβ gene repertoire in individuals with leukemia before and after allogeneic hematopoietic stem cell transplantation (allo-HSCT).Methods Peripheral blood mononuclear cells (PBMC) were obtained from 10 normal individuals, 8 donors and 11 patients with leukemia before and after transplantation. Polymerase chain reaction (PCR) amplification of complementarity-determining region 3 (CDR3) of 24 TCR Vβ genes was used to examine serial samples of PBMC. The PCR products were further analyzed by genescan to evaluate clonality of T cells.Results The 24 TCR Vβ gene repertoire displayed highly diverse and polyclonal spectratypes in all normal individuals and 4 of 8 donors. Anoth er 4 donors expressed part of the 24 TCR Vβ subfamily and 1 donor had oligoclonality. The expressions of the 24 TCR Vβ subfamilies were skewed and restric ted in 11 leukemia patients before and after transplantation. Some absences of 24 TCR Vβ subfamily expression were quite similar between the recipients pro-transplantation and related donors. The number of subfamilies expressed increased over time post-transplantation, but the restricted expressions of the subfamily could last 6-30 months after transplantation. All patients with GVHD and some without GVHD exhibited T cell clonal expansion. The expansive T cell clone was distributed in Vβ 2-3, 16-17, 18-19, 21 and Vβ 23 in patients with GVHD and in Vβ 7, 9, 16 and 19 in patients without GVHD. One patient with syngeneic-HSCT (syn-HSCT) had Vβ 15 and 16 T cell expansion after transplantation. One patient displayed Vβ 18 T cell expansion after donor lymphocyte infusion (DLI).Conclusions Normal individuals express the entire 24 TCR Vβ ge ne repertoire and have polyclonal distribution. However, the TCR Vβ gene repertoire is only partially expressed in some donors. The TCR Vβ gene repertoire is restrictedly expressed in a skew fashion in patients with leukemia before and after transplantation. The number of TCR Vβ gene subfamilies increases over time post- transplantation. GVHD and GVL effects may induce the proliferation of T cell clones.Clinical GVL response may be distinguished from GVHD alloreactivity through the host MHC antigen. 展开更多
关键词 tcr gene repertoire · T cell clonality · hem atopoietic stem cell transplantation · graft-versus-host disease · graft-versus-leukemia
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