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卡介苗分泌性蛋白对人单个核细胞体外刺激效应的探讨

Preliminary study on influence of Bacillus Calmette-Guerin secretory protein to human mononuclear cells
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摘要 目的初步探讨卡介苗(Bacillus Calmette-Guerin,BCG)分泌性蛋白在体外培养试验中对人单个核细胞的刺激效应。方法用淋巴细胞转化试验(MTT法)检测单个核细胞经卡介苗纯蛋白衍化物(BCG-PPD)刺激后的增殖程度和IL-2生成情况,同时设ConA对照组。结果BCG-PPD体外刺激人单个核细胞后,单个核细胞增殖程度和IL-2生成量均明显增加,且显著高于有丝分裂原Co-nA对照组(P均<0.001);单个核细胞增殖程度和IL-2生成量之间呈正相关关系(r=0.6 666,P<0.001)。结论BCG分泌性蛋白具有较强的免疫原性,可显著激活单个核细胞功能,提示卡介苗分泌性蛋白在抗结核免疫中起了积极作用。 Objective To observe the influence of Bacillus Calmette-Guerin (BCG)'s secretory protein to human mononuclear cells (MCs). Methods The proliferation and IL-2 production of human MCs stimulated with BCG's purified protein derivative (BCG-PPD) were detected by lymphocyte transformation test (LTT) and enzyme-linked immunosorbent assay (ELISA). Results After stimulated with BCG-PPD in vitro, the proliferation and IL-2 production of human MCs were remarkably higher than ConA control group (P〈0. 001). Significant correlation was showed between the proliferation degree and IL-2 production of human MCs (r=0. 6 666, P〈0. 001). Conclusion BCG's secretory protein has strong immunogenicity can activate human MCs.
作者 蒋红梅 王妤 王永霞
机构地区 贵阳医学院检验系
出处 《贵州医药》 CAS 2006年第9期777-779,共3页 Guizhou Medical Journal
基金 贵州省高层次人才科研条件特助经费(030516)资助
关键词 卡介苗 分泌性蛋白 单个核细胞 BCG Secretory protein Mononuclear cells
分类号 R329.28 [医药卫生—人体解剖和组织胚胎学] R392.13 [医药卫生—免疫学]
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  • 1张立兴,屠德华,阚冠卿.国际结核病流行出现的严重问题和我们的对策[J].中国防痨杂志,1996,18(3):97-100. 被引量:35
  • 2林学颜 张玲.T细胞-介导免疫应答的效应机制.现代细胞与分子免疫学[M].广州:中山医科大学出版社,1998.243.
  • 3薛彬 雷志明 等.免疫毒理学实验技术(第1版)[M].北京:北京医科大学、中国协和医科大学联合出版社,1995.19-20.
  • 4Pollock JM, Andersen P. Predominant recognition of the ESAT-6 protein in the first phase of interferon with mycobacterium bovis in cattle[J]. Infect Immun, 1997, 65:2587-2592.
  • 5Ulrichs T, Munk ME, Mollenkopf H, et al. Differential T cell responses to mycobacterium tuberculosis ESAT6 in tuberculosis patients and healthy donors[J]. Eur J Immun, 1998, 28:3949-3958.
  • 6Brandt L, Elhay M, Rosenkrands I, et al. ESAT-6 subunit vaccination against mycobacterium tuberculosis[J ]. Infect Immun, 2000, 68: 791-795.
  • 7Olsen AW, Van Pinxteren LA, Okkels LM, et al. Protection of mice with a tuberculosis subunit vaccine based on a fusion protein of antigen 85B and ESAT-6[J]. Infect Immun, 2001, 69:2773-2778.
  • 8Kamath AT, Feng CG, Macdonald M, et al. Differential protective efficacy of DNA vaccine expressing secreted proteins of mycobacterium tuberculosis[J]. Infect Immun, 1999, 67:1702-1707.
  • 9Mcshane H, Brookes R, Gilbert SC, et al. Enhanced immunogenicity of CD4 + T-cell responses and protective efficacy of a DNA-modified vaccinia virus ankara prime-boost vaccination regimen for murine tuberculosis[J]. Infect Immun, 2001, 69:681-686.
  • 10Malin AS, Huygen K, Content J, et al. Vaccinia expression of mycobacterium tuberculosis-secreted proteins: tissue plasminogen activator signal sequence enhances expression and immunogenicity of M. tuberculosid Ag85[J]. Microbes Infect, 2000, 2:1677-1685.

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贵州医药
2006年 第9期

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