CD80、CD86表达与ITP患者免疫紊乱的相关性研究

doi:10.3969/j.issn.1671-2587.2019.01.027

临床输血与检验 ›› 2019, Vol. 21 ›› Issue (1): 81-84.DOI: 10.3969/j.issn.1671-2587.2019.01.027

CD80、CD86表达与ITP患者免疫紊乱的相关性研究

潘珂

621000 四川省绵阳市妇幼保健院检验科

收稿日期:2018-07-16 出版日期:2019-02-20 发布日期:2019-01-28
作者简介:潘珂（1976-）,男,四川绵阳人,学士,主管检验师,主要从事检验工作,（E-mail）ganxue189@126.com。

The Study of the Relationship between CD80/CD86 Expression in B Cells and Immune Disorders in Patients with Immune Thrombocytopenia

PAN Ke

Mianyang Maternal and Child Health Hospital,Mianyang 621000

Received:2018-07-16 Online:2019-02-20 Published:2019-01-28

摘要/Abstract

摘要： 目的研究CD80、CD86表达与免疫性血小板减少症（ITP）患者免疫紊乱的相关性。方法纳入90例ITP患者作为研究对象,采用流式细胞术检测所有患者外周血中CD19⁺CD80⁺、CD19⁺CD86⁺及CD19⁺B细胞内抗体IgG、IgM的表达水平。所有患者均接受重组人血小板生成素（rhTPO）+泼尼松治疗,随访记录完全缓解率,采用Logistic多因素分析探讨ITP预后高危因素,采用偏相关分析CD19⁺CD80⁺、CD19⁺CD86⁺与IgG、IgM表达水平的相关性。结果随访3~11个月,平均随访时间（7.95±2.74）月,ITP完全缓解率为46.67%,多因素分析结果显示CD19⁺CD80⁺、CD19⁺CD86⁺、IgG及IgM是影响预后的高危因素（P<0.05）。CD19⁺CD80⁺与IgG、IgM呈线性分布,经偏相关分析发现均具有正相关性（r=0.229,0.592;P=0.031,P<0.001）。CD19⁺86⁺与IgG、IgM呈线性分布,经偏相关分析发现均具有正相关性（r=0.415,0.292, P<0.001,0.005）。结论 CD80和CD86与免疫紊乱密切相关,是影响ITP患者预后的高危因素,CD80和CD86的过度表达可能是CD19⁺B细胞过度活化,并介导免疫功能紊乱的重要机制。

关键词: 免疫性血小板减少症, CD80, CD86, 免疫紊乱

Abstract: Objective To study the relationship between CD80/CD86 expression in B cells and immune disorders in patients with immune thrombocytopenia（ITP）. Methods 90 patients with ITP were enrolled in the study,the flow cytometry was used to detect the expression CD80⁺/CD86⁺in CD19⁺B cells,the IgG/IgM level in peripheral blood. All patients were treated with recombinant human thrombopoietin （rhTPO） and prednisone,the complete remission rate was recorded by followed up,Logistic analysis was used to test the risk factors of the prognosis of ITP the partial correlation analysis was used to test relationship between CD19⁺CD80⁺,CD19⁺CD86⁺ and IgG,IgM expression. Results The patients were followed up for 3-11 months with an average follow-up time of （7.95±2.74） months,the complete remission rate of ITP was 46.67%. The multivariate analysis showed that CD19⁺CD80⁺,CD19⁺CD86⁺,IgG and IgM level were the high risk factors of prognosis （P<0.05）.The CD19⁺CD80⁺ and IgG,IgM had linear distribution,the partial correlation analysis showed significant positive correlation（r=0.229,0.592;P=0.031,P<0.001）.The CD19⁺CD86⁺and IgG,IgM had linear distribution,the partial correlation analysis showed significant positive correlation（r=0.415,0.292,P<0.001,0.005）. Conclusion The CD80 and CD86 are closely related to immune disturbances,and they are the high risk factors for the prognosis of patients with ITP,the over expression of CD80 and CD86 in B cells may be the important mechanism for over activation of CD19⁺B cells and mediated immune dysfunction.

Key words: ITP, CD80, CD86, Immune disorder

中图分类号:

R555⁺.1

潘珂. CD80、CD86表达与ITP患者免疫紊乱的相关性研究[J]. 临床输血与检验, 2019, 21(1): 81-84.

PAN Ke. The Study of the Relationship between CD80/CD86 Expression in B Cells and Immune Disorders in Patients with Immune Thrombocytopenia[J]. JOURNAL OF CLINICAL TRANSFUSION AND LABORATORY MEDICINE, 2019, 21(1): 81-84.

参考文献

1 骆林胜,冯爱梅,薛阿利,等. 小剂量美罗华治疗难治性原发免疫性血小板减少症疗效以及对细胞免疫功能的影响[J]. 中国医师杂志,2016,18(6):890-891.
2 胡成琳.对免疫性血小板减少症发病机制及治疗的研究进展[J].重庆医学,2012,41(24):2541-2544.
3 陈燕文,王超,王旭光,等.系统性红斑狼疮患者外周血T、B细胞自噬水平及其临床意义[J].中国免疫学杂志,2015,15(10):1380-1384,1388.
4 牛延良,姜炎,孙乐羽,等.重症肌无力患者B细胞激活及其与激素治疗相关性研究[J].重庆医学,2014,7(30):4075-4077.
5 张琰,房光萃,张丽华,等.共刺激分子CTLA-4与B7在自身免疫性心肌炎中的作用[J].中国免疫学杂志,2013,29(3):283-287.
6 中华医学会血液学分会血栓与止血学组.成人原发免疫性血小板减少症诊断与治疗中国专家共识[J].中华血液学杂志,2012,33(11):975-977.
7 杨敏,刘文君.免疫性血小板减少症发病机制研究最新进展[J].中国实验血液学杂志,2016,24(3):958-962.
8 Zhang X M.,Shan N N,Sun M,et al.Imbalanced expression of human Tim-1 and Tim-3 in peripheral blood mononuclear cells from immune thrombocytopenia patients[J]. Int Immunopharmacol,2014,19(1):1-4.
9 孙明玲,王新有,江明,等.重组人血小板生成素联合大剂量地塞米松治疗初治原发性免疫性血小板减少症的临床分析[J].中华内科杂志,2016,55(3):202-205.
10 隋涛,马立,李新,等.免疫性血小板减少症患者血浆微小RNA差异表达谱的筛选与验证[J].中华医学杂志,2014,19(14):1083-1086.
11 曾艳,韩红,陈慧,等.免疫性血小板减少症患者外周血Treg细胞microRNA分析[J].中国免疫学杂志,2016,32(9):1350-1353.
12 旷文勇,顾艳艳,郑敏翠,等.糖皮质激素对慢性免疫性血小板减少症患儿树突状细胞的影响[J].中国当代儿科杂志,2013,15(2):91-94.
13 陈永玲,袁琳,邓明凤,等.原发性血小板减少性紫癜患者血小板相关抗体的检测[J].微循环学杂志,2005,15(2):83-84.
14 周振海,李小银,潘倩影,等.免疫性血小板减少症患者树突状细胞的分布特点及其活化状态的研究[J].中国实验血液学杂志,2013,21(6):1513-1516.
15 郭莹,瞿文,王一浩,等.共刺激信号分子对免疫性血小板减少症患者B淋巴细胞免疫功能的影响[J].中国实验血液学杂志,2016,24(4):1110-1115.
16 任敏,单哲,许联红.免疫性血小板减少症患者协同刺激分子的表达及意义[J].中国医学创新,2014,13(34):29-31.
17 张娜,蒋慧,邵静波,等.405例儿童原发免疫性血小板减少症的分层治疗[J].中华血液学杂志,2015,36(12):1031-1034.

[1]	郑静娴, 李晓辉, 孙洪强. 儿童免疫性血小板减少症的临床观察及抗核抗体在其中作用的研究[J]. 临床输血与检验, 2021, 23(2): 231-235.
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[4]	刘正婷, 黄佳丽, 陈尚良. 二孩时代,我们能为FNAIT做些什么[J]. 临床输血与检验, 2019, 21(5): 552-557.
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[6]	张笑盼, 宋继军, 马曙轩. 血栓弹力图在儿童免疫性血小板减少症治疗中的应用[J]. 临床输血与检验, 2017, 19(3): 240-242.

CD80、CD86表达与ITP患者免疫紊乱的相关性研究

The Study of the Relationship between CD80/CD86 Expression in B Cells and Immune Disorders in Patients with Immune Thrombocytopenia

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