Analysis of CD4^+CD25^+ Regulatory T Cells and Foxp3 mRNA in the Peripheral Blood of Patients with Asthma

The changes of CD4^＋CD25^＋ regulatory T cells （CD4^＋CD25^＋ Treg） and Foxp3 mRNA in peripheral blood mononuclear cells （PBMCs） from patients with asthma were investigated in order to elucidate the possible roles of CD4^＋CD25^＋ Treg in the development of asthma. The peripheral blood samples were collected from 29 healthy controls （normal control group） and 78 patients with asthma which included 30 patients in exacerbation group, 25 patients in persistent group, and 23 patients in remission group. By using flow cytometry and RT-PCR, the CD4^＋CD25^＋ Treg ratio and Foxp3 mRNA in PBMCs were detected. The CD4^＋CD25^＋ Treg ratio and Foxp3 mRNA in PBMCs of exacerbation and persistent groups were lower than that of remission and normal control groups （P〈0.05）. Although the CD4^＋CD25^＋ Treg ratio and Foxp3 mRNA of remission group were also lower than that of normal control group, there was no significant difference between them （P〉0.05）. As compared with persistent group, exacerbation group had lower CD4^＋CD25^＋ Treg ratio and Foxp3 mRNA （P〈0.05）. It was indicated that the decrease of CD4^＋CD25^＋ Treg ratio and its function in PBMCs may be responsible for pathogenesis of asthma.

Immunotherapy of rat glioma without accumulation of CD4^+CD25^+FOXP3^+ regulatory T cells

Immunotherapy may be used for the treatment of glioblastoma multiforme; however, the induced immune response is inadequate when either T cells or dendritic cells are used alone. In this study we established a novel vaccine procedure in rats, using dendritic cells pulsed with C6 tumor cell lysates in combination with adoptive transfer of T lymphocytes from syngenic donors. On day 21 after tumor inoculation, all the rats were sacrificed, the brains were harvested for calculation of glioma volume, cytolytic T lymphocyte responses were measured by cytotoxic assay, and the frequency of regulatory T lymphocytes （CD4＋CD25~FOXP3~） in the peripheral blood was investigated by flow cytometric analysis. The survival rate of rats bearing C6 glioma was observed. Results showed that the co-immunization strategy had significant anti-tumor potential against the pre-established C6 glioma, and induced a strong cytolytic T lymphocyte response in rats. The frequency of peripheral blood CD4＊CD25＊FOXP3＊ regulatory T lymphocytes was significantly decreased following the combination therapy, and the rats survived for a longer period. Experimental findings indicate that the combined immunotherapy of glioma cell lysate-pulsed dendritic cell vaccination following adoptive transfer of T cells can effectively inhibit the growth of gliomas in rats, boost anti-tumor immunity and produce a sustained immune response while avoiding the accumulation of CD4＋CD25＋FOXP3＋ regulatory r lymphocytes.

急性非ST抬高心肌梗死患者外周血CD4^(+)CD25^(+)Foxp3^(+)Treg和IL-27变化的临床意义

目的观察急性非ST抬高心肌梗死患者(Non-STMI)治疗过程中外周血CD4^(+)CD25^(+)T/CD4^(+)T、CD4^(+)CD25highFoxp3^(+)Treg/CD4^(+)CD25high T比例及细胞因子TGF-β1、IL-10、INF-γ、IL-27的浓度变化,阐明Non-STMI患者是否存在调节性T细胞比例及功能异常。方法选取2012年8月至2016年4月入住中山大学附属第一医院急诊病房和CCU的Non-STMI40名,不稳定性心绞痛(UA)患者19名和同龄健康志愿者20名作为对照组(HC)。患者诊断明确后次日清晨和经规范治疗后5~7天,留取空腹外周血标本。流式细胞术检测CD4^(+)CD25^(+)T/CD4^(+)T、CD4^(+)CD25high Foxp3^(+)Treg/CD4^(+)CD25high T细胞。ELISA法检测细胞因子TGF-β1、IL-10、INF-γ和IL-27浓度。结果UA、Non-STMI组CD4^(+)CD25highFoxp3^(+)Treg/CD4^(+)CD25highT比例较HC组减低(P<0.01);Non-STMI明显低于UA组(P<0.05),而治疗后Non-STMI组Foxp3^(+)Treg细胞比例显著升高(P<0.05)。入院时Non-STMI和UA组TGF-β1、IL-10浓度较HC组明显降低(P<0.05),而INF-γ和IL-27浓度明显升高(P<0.05)。治疗后Non-STMI组IL-27迅速下降,而UA组变化不明显。治疗前IL-27浓度与CD4^(+)CD25highFoxp3^(+)Treg/CD4^(+)CD25highT呈线性负相关、与INF-γ浓度呈线性正相关。治疗后只有IL-27和CD4^(+)CD25high Foxp3^(+)Treg/CD4^(+)CD25highT呈线性负相关。结论Non-STMI患者CD4^(+)CD25highFoxp3^(+)Treg比例及功能异常,细胞因子IL-27有助于判断患者的临床疗效。

冷冻消融联合养肺方治疗对Lewis肺癌CD4^(+)CD25^(+)Foxp3^(+)Treg的影响及机制

目的 探讨冷冻消融联合养肺方治疗对Lewis肺癌CD4^(+)CD25^(+)Foxp3^(+)Treg细胞影响及机制。方法 构建C57BL/6小鼠肺癌皮下移植瘤模型,随机分为模型组、冷冻消融组、冷冻消融联合养肺方低、中、高剂量组,每组5只。模型组行假手术,在小鼠移植瘤部位切开缝合,其余各组均行双循环冷冻消融术。术后冷冻消融联合养肺方低、中、高剂量组分别给予1.64、3.28、6.56 g/kg养肺方灌胃,模型组、冷冻消融组分别给予等体积的生理盐水灌胃,均1次/d,连续给药14 d。给药期间观察并记录各组小鼠肿瘤体积,末次给药后剥离脾脏和移植瘤,称取瘤体质量并计算抑瘤率;流式细胞术检测脾脏CD4^(+)T、CD4^(+)CD25^(+)Foxp3^(+)T细胞比例;qRT-PCR和Western blot法检测瘤组织中Foxp3表达。结果 各组小鼠肿瘤体积均逐渐增长,增长速度为模型组>冷冻消融组>冷冻消融联合养肺方低剂量组>冷冻消融联合养肺方中剂量组>冷冻消融联合养肺方高剂量组。手术联合药物干预14 d后,与模型组比较,各治疗组肿瘤体积小(P<0.05);与冷冻消融组比较,冷冻消融联合养肺方低、中、高剂量组肿瘤体积小(P<0.01);冷冻消融联合养肺方高剂量组肿瘤体积小于低剂量组(P<0.01)。与模型组比较,冷冻消融联合养肺方低、中、高剂量组瘤体质量小(P<0.05);与冷冻消融组比较,冷冻消融联合养肺方低、中、高剂量组瘤体质量小(P<0.05)。冷冻消融组、冷冻消融联合养肺方低、中、高剂量组抑瘤率逐渐升高。与模型组比较,各治疗组CD4^(+)T细胞比例低(P<0.05),冷冻消融联合养肺方低、中、高剂量组的CD4^(+)CD25^(+)Foxp3^(+)T%细胞比例低(P<0.05);与冷冻消融组比较,冷冻消融联合养肺方高剂量组CD4^(+)T、CD4^(+)CD25^(+)Foxp3^(+)T细胞比例低(P<0.05);冷冻消融联合养肺方低、中、高剂量组CD4^(+)T、CD4^(+)CD25^(+)Foxp3^(+)T细胞比例逐渐降低。与模型组比较,冷冻消融联合养肺方低、中、高剂量组肿瘤组织中Foxp3 mRNA相对表达量和Foxp3蛋白表达均降低(P<0.01);冷冻消融联合养肺方中、高剂量组Foxp3 mRNA相对表达量和Foxp3蛋白表达均低于冷冻消融组(P<0.01)和冷冻消融联合养肺方低剂量组(P<0.05)。结论冷冻消融联合养肺方通过减少Lewis肺癌小鼠脾脏CD4^(+)CD25^(+)Foxp3^(+)Treg细胞比例,下调肿瘤组织中Foxp3表达,发挥抑制Lewis肺癌增殖作用,其机制可能与增强机体抗肿瘤免疫应答,改善肿瘤免疫抑制有关。

Combined TIM-3 and PD-1 blockade restrains hepatocellular carcinoma development by facilitating CD4+ and CD8+T cellmediated antitumor immune responses

BACKGROUND Immune checkpoint inhibitors(ICIs)targeting programmed cell death protein 1(PD-1)and T cell immunoglobulin and mucin domain-containing protein 3(TIM-3)are beneficial to the resumption of anti-tumor immunity response and hold extreme potential as efficient therapies for certain malignancies.However,ICIs with a single target exhibit poor overall response rate in hepatocellular carcinoma(HCC)patients due to the complex pathological mechanisms of HCC.AIM To investigate the effects of combined TIM-3 and PD-1 blockade on tumor development in an HCC mouse model,aiming to identify more effective immunotherapies and provide more treatment options for HCC patients.METHODS The levels of PD-1 and TIM-3 on CD4+and CD8+T cells from tumor tissues,ascites,and matched adjacent tissues from HCC patients were determined with flow cytometry.An HCC xenograft mouse model was established and treated with anti-TIM-3 monoclonal antibody(mAb)and/or anti-PD-1 mAb.Tumor growth in each group was measured.Hematoxylin and eosin staining and immunohistochemical staining were used to evaluate T cell infiltration in tumors.The percentage of CD4+and CD8+T cells in tissue samples from mice was tested with flow cytometry.The percentages of PD-1+CD8+,TIM-3+CD8+,and PD-1+TIM-3+CD8+T cells was accessed by flow cytometry.The levels of the cytokines including tumor necrosis factor alpha(TNF-α),interferon-γ(IFN-γ),interleukin(IL)-6,and IL-10 in tumor tissues were gauged with enzyme-linked immunosorbent assay kits.RESULTS We confirmed that PD-1 and TIM-3 expression was substantially upregulated in CD4+and CD8+T cells isolated from tumor tissues and ascites of HCC patients.TIM-3 mAb and PD-1 mAb treatment both reduced tumor volume and weight,while combined blockade had more substantial anti-tumor effects than individual treatment.Then we showed that combined therapy increased T cell infiltration into tumor tissues,and downregulated PD-1 and TIM-3 expression on CD8+T cells in tumor tissues.Moreover,combined treatment facilitated the production of T cell effector cytokines TNF-α and IFN-γ,and reduced the production of immunosuppressive cytokines IL-10 and IL-6 in tumor tissues.Thus,we implicated that combined blockade could ameliorate T cell exhaustion in HCC mouse model.CONCLUSION Combined TIM-3 and PD-1 blockade restrains HCC development by facilitating CD4+ and CD8+T cell-mediated antitumor immune responses.

Rapamycin increased development of CD4^+ CD25~h ighFoxp3^+ T cells of peripheral blood in liver transplant recipients

Objective To investigate the possible influence of immunosuppressive therapy,including sirolimus ( SRL) and calcineurin inhibitors ( CNI,tacrolimus) ,on level of Treg in liver allo - graft recipients. Methods Forty - seven liver transplant recipients with stable liver function were assessed for at least 2 years,and divided into

All-transRetinoic Acid Regulates Th1/Th2 Balance in CD4+T cells When GATA-3 is Deficient

The essential effect of vitamin A on immune function occurs through various mechanisms including direct effect on ThloTh2 balance modulation. However, it is unclear whether or not vitamin A can regulate Thl-Th2 balance under a strong Thl-polarizing condition. Therefore, the purpose of our study was to examine the effect of vitamin A metabolite allotrans retinoic acid （ATRA） on ThloTh2 differentiation in CD4~ T cells under GATA-3 deficiency, which can induce Thl-polarizing condition. In the present study, GATA-3 deficiency T cells were induced by siRNA and checked by real-time quantitative PCR and western blot. GATA-3 deficiency CD4＋ T cells and normal CD4＋ T were treated for 48 h with or without ATRA.

Influence of Danshen Injection on airway inflammation and CD4^+ CD25^+ regulatory T cells of asthmatic rats

Objective： To investigate the influence of Danshen Injection on airway inflammation and CD4^＋CD25^＋ regulatory T cells（CD4^＋CD25^＋ Tr） of asthmatic rats, and elucidate the possible mechanism of Danshen Injection in treatment of asthma. Methods： 30 Wister rats were randomly divided into control group, asthma group and Danshen Injection treated group. Bronchoalveolar lavage fluids （BALF） were collected, and cytology studies were conducted. Lung tissues were obtained and pathologic analyses were done with hematoxylin and eosin stain （HE）. Flow cytometry was used to detect the CD4^＋CD25^＋ Tr ratio in peripheral blood mononuclear cells （PBMCs）. Results： Total cell, the percentage of lymphocytes, neutrophils and eosinophils （Eos） in BALF of Danshen Injection-treated group were lower than that in asthma group （P〈0.05, P〈0.01）. Compared with asthma group, less infiltration of inflammatory cells in lung tissues was observed in Danshen Injection-treated group. CD4^＋CD25^＋ Tr of asthma group was lower than that of control and Danshen Injection treated group （P〈0.05）. Conclusion： Danshen Injection can suppress airway inflammation of asthmatic rats, probably by increasing the number of CD4^＋CD25^＋ Tr.

肺癌患者CD4^+ CD25^(high) Foxp3^+调节性T细胞的格局变化及意义

目的:研究肺癌患者外周血(PBMC)及肿瘤浸润淋巴细胞(TIL)中CD4+CD25h ighFoxp3+调节性T细胞(Treg)的比例改变,探讨其在抗肿瘤免疫中的调节作用。方法:分离肺癌患者PBMC及TIL,FACS分析CD4+/CD8+T细胞的比值及CD4+CD25h ighT细胞占CD4+T细胞的比例。Real-tim e PCR检测Treg特异性转录因子Foxp3基因在PBMC及TIL中的表达。结果:肺癌患者PBMC及TIL中CD4+/CD8+比值降低;而CD4+CD25h ighT细胞在CD4+T细胞中所占比例升高;Foxp3基因仅在TIL中高表达,而在PBMC中低或不表达,表明肿瘤局部的CD4+CD25h ighT细胞主要是CD4+CD25h ighFoxp3+Treg。结合临床资料分析显示Treg在肺腺癌比例较高。结论:CD4+CD25h ighFoxp3+Treg在肺癌患者肿瘤浸润淋巴细胞中明显升高,可能与其通过细胞与细胞间接触抑制CD8+T细胞的杀伤效应,最终发挥免疫抑制效应相关。

不同分期老年COPD患者外周血中CD4^＋Foxp3^＋调节性T细胞变化及其与肺功能改变的相关性

目的观察急性期、稳定期老年慢性阻塞性肺病(COPD)患者和健康人外周血中的CD 4+Foxp3+调节性T细胞(Treg细胞)比例变化,分析Treg细胞与各期老年COPD患者肺功能改变的相关性,探讨Treg细胞在老年COPD发生发展中的作用。方法①随机选取2010年2～12月就诊我院呼吸内科的急性期老年COPD患者30例、稳定期老年COPD患者35例,分别设为实验1组和实验2组,选取同期进行社区流行病学调查的健康人25例设为对照组。所有受试者均填写统一的调查问卷,了解他们的一般情况、吸烟史等99个变量,并完善肺功能检查;②各组受试者空腹6 h后于清晨8时肘正中静脉抽取静脉血2 ml,应用细胞内染色的流式细胞术检测各组受试者外周血中Treg细胞;③多组间比较采用单因素方差分析,多组内两两比较采用SNK检验(方差齐)和Games-Howell法(方差不齐),Treg细胞的比例与肺功能关系用Spearman相关分析进行相关性检验。结果①实验1组、实验2组和对照组外周血Treg细胞比例分别为(2.62±0.68)%、(0.86±0.46)%和(1.45±0.70)%,三组结果两两比较差异显著(P<0.05);②实验1组、实验2组和对照组外周血CD4和CD25双阳性细胞比例为(3.90±1.64)%、(3.01±1.40)%和(3.78±1.83)%,三组比较无统计学意义(P>0.05);③外周血Treg细胞比例与第1秒用力呼气容积实测值与预计值比(FEV1%prep)和第1秒用力呼气容积/用力肺活量比(FEV1/FVC)均无相关性(r=-0.158、-0.188,P值分别为0.136、0.076);外周血Treg细胞比例与年龄之间无相关性(r值为0.014,P>0.05)。结论老年COPD患者体内存在免疫功能失调,Treg细胞可能参与了老年COPD的发病和急性加重过程;外周血中的CD 4+Foxp3+Treg细胞的比例与老年COPD患者肺功能无相关性。

肺结核患者外周血中CD4^+CD25^+FoxP3^+调节T细胞增多并抑制抗结核免疫

目的研究肺结核患者外周血中CD4+CD25+FoxP3+调节T细胞是否增多,这些调节T细胞是否抑制结核的特异细胞免疫反应。方法使用细胞分离、流式细胞分析及细胞增殖及增殖抑制等实验方法,对20例肺结核患者及17例健康人群外周血中CD4+CD25+FoxP3+调节T细胞的数量及免疫学特征作研究。结果肺结核患者外周血中CD4+CD25+FoxP3+调节T细胞数占CD4+细胞总数的比例显著高于健康人群(P<0.01)。在体外,肺结核患者外周血单个核细胞在BCG及ESAT-6的刺激下增殖能力比健康对照人群明显增强(P<0.01),产生的γ-干扰素比健康人群也明显增强(P<0.05);清除调节T细胞后的肺结核患者外周血单个核细胞对BCG刺激下产生γ-干扰素及白介素-10比没有清除时显著增强(P<0.05);从肺结核患者外周血分离CD4+CD25+调节T细胞和CD4+CD25-细胞,CD4+CD25-细胞对BCG及ESAT-6刺激产生γ-干扰素和白介素-10的能力因CD4+CD25+调节T细胞加入后而显著减弱(P<0.05)。结论肺结核患者CD4+CD25+FoxP3+调节T细胞增多,通过抑制结核患者细胞免疫反应,参与肺结核的发病。

Graves病患者^(131)I治疗前后CD4^+CD25^+ Foxp3^+调节性T细胞的变化

目的:通过对Graves病患者131I治疗前后外周血各淋巴细胞亚群和CD4+CD25+ Foxp3+调节性T细胞含量以及相关基因Foxp3mRNA表达水平的测定,探讨131I治疗方法是否可以通过改变调节性T细胞的含量从而改善Graves病患者的免疫功能异常。方法:采集30例Graves病患者131I治疗前及治疗后1个月的外周血,流式细胞仪检测外周血CD3+、CD3+CD4+、CD3+CD8+、CD3-CD19+、CD3-CD16+CD56+淋巴细胞亚群及CD4+CD25+ Foxp3+调节性T细胞的百分率,Real-TimePCR检测外周血单个核细胞Foxp3mRNA的表达水平。结果:和治疗前相比,Graves病患者131I治疗1个月后外周血CD3+CD4+T细胞和CD3-CD19+B细胞百分率都明显减少(P<0.05),CD3-CD16+CD56+NK细胞百分率明显增加(P<0.05),CD3-CD8+T细胞、CD4+CD25+ Foxp3+调节性T细胞百分率和Foxp3mRNA的表达水平无明显变化。结论:131I不能通过增加调节性T细胞的含量而改善Graves病患者的免疫耐受障碍,但可以通过减少CD4+T和B淋巴细胞的含量和增加NK细胞的含量来控制过度的免疫应答。

大鼠急性脑缺血后CD4^+CD25^+调节性T细胞、Foxp3表达及其意义

目的动态观察大鼠急性脑缺血后不同时期外周血中CD4+CD25+调节性T细胞和脑组织中Foxp3的表达,探讨其在急性缺血性卒中病理生理演变过程中的作用。方法 48只Wistar大鼠按随机数字表法分为缺血组和假手术组。参考改良的Zea-Longer插线方法将缺血组大鼠制作成右侧大脑中动脉线栓脑缺血动物模型。采用流式细胞术和免疫组化染色检测造模后1、3、7、14 d时大鼠外周血中CD4+CD25+调节性T细胞表达和脑组织中Foxp3表达,同时采用改良NSS神经功能评分观察大鼠行为学变化。结果缺血组和假手术组大鼠神经功能缺损评分在模型制备后逐渐下降(P<0.01)。流式细胞术显示脑缺血后1、3 d时缺血组大鼠外周血中CD4+CD25+调节性T细胞的表达与假手术组比较差异无统计学意义(P>0.05),7、14 d时表达明显高于假手术组(P<0.05),且与大鼠的神经功能评分呈负相关(r=-0.68,P=0.01)。免疫组化显示脑缺血后1 d时缺血组大鼠脑组织中即可观察到Foxp3表达,且主要集中在缺血灶区域,在未缺血侧也可观察到Foxp3表达,但表达量较少,而假手术组脑组织中未见Foxp3表达。结论 CD4+CD25+调节性T细胞参与了大鼠急性脑缺血后炎症免疫反应的发生发展过程,且在脑缺血后1 d时便开始参与脑缺血性损伤的免疫调节,这种免疫调节对脑细胞有着保护作用。

雷帕霉素诱导Balb/c小鼠CD4^+ CD25^+ foxp3^+调节性T细胞增殖

目的探讨雷帕霉素对Balb/c小鼠CD4+ CD25+ foxp3+调节性T细胞的作用。方法取8wk龄的SPF级Balb/c小鼠30只,随机分为两组,实验组每只灌胃雷帕霉素0.4mg.d-1,对照组灌胃每天予等体积无菌水,共3wk。无菌条件下肝素抗凝心脏采血,分离脾脏,制备单细胞悬液。采用流式细胞仪检测小鼠外周血和脾细胞CD4+CD25+T细胞,实时定量PCR检测小鼠脾细胞foxp3 mRNA的表达。结果实验组小鼠外周血和脾细胞中CD4+CD25+T细胞的比例分别为(9.95±4.65)%和(24.13±10.06)%,对照组小鼠外周血和脾细胞中CD4+CD25+T细胞的比例分别为(5.01±1.49)%和(8.48±3.19)%,差异均有显著性(P<0.01)。实验组小鼠脾细胞foxp3 mRNA的表达水平明显高于对照组,是对照组的6.029倍,差异有显著性(P<0.01)。结论雷帕霉素能够明显诱导Balb/c小鼠体内CD4+CD25+T细胞的增殖,并能提高foxp3+ mRNA的表达。

T-bet、GATA-3、FoxP3及CD_4^+CD_(25)^+调节性T细胞在AA发病机制中的作用

目的探讨转录因子T-bet、GATA-3和CD+4CD+25调节性T细胞及其转录因子FoxP3在再生障碍性贫血(AA)发病机制中的作用。方法选择AA患者27例(AA组)、体检健康者25例(对照组),采用RT-PCR技术检测两组外周血单个核细胞(PBMCs)中Th1、Th2细胞及CD4+CD2+5调节性T细胞特异性转录因子T-bet、GATA-3、FoxP3 mR-NA的表达,运用流式细胞术检测外周血中T淋巴细胞亚群,ELISA法检测血浆中Th1和Th2类细胞因子IFN-γ、IL-4水平。结果与对照组相比,AA组的血浆T-bet mRNA相对表达量升高(P<0.01),GATA-3与FoxP3 mRNA相对表达量降低(P<0.05,P<0.01);AA组外周血中CD+3、CD+3CD+8T细胞占淋巴细胞的百分比较对照组升高(P均<0.05),CD+3CD+4、CD+4CD+25T细胞占淋巴细胞的百分比和CD+4/CD+8值较对照组降低(P<0.05或P<0.01);AA组血浆中IFN-γ水平及IFN-γ/IL-4高于对照组(P均<0.01)。结论 AA患者存在CD+4CD+25调节性T细胞及其特异性转录因子FoxP3 mRNA表达下调,调节性T细胞的减少及由此引起免疫抑制效应不足可能是AA发生的重要原因之一。

不明原因复发性流产小鼠模型CD4^+CD25^+ Treg的比例及Foxp3表达的变化

目的分析比较小鼠正常妊娠模型和流产模型中CD4+CD25+调节性T细胞CD4+CD25+Treg的比例、Foxp3蛋白表达水平及胎盘吸收率,探讨CD4+CD25+Treg与不明原因复发性流产的关系。方法以雌性CBA/J×雄性Balb/c为对照组,以雌性CBA/J×雄性DBA/2J为流产组,各10对,于妊娠第14天采用流式细胞术(flow cytometry,FCM)分析CD4+CD25+Treg在CD4+细胞中所占比例,Western blot检测并比较2组CD4+T细胞中Foxp3的表达,并观察2组小鼠的胎盘吸收情况。结果流产组CD4+CD25+Treg所占比例为(10.1±0.59)%低于对照组(15.5±0.78)%(P<0.05)。流产组胚胎吸收率为(25.6±3.5)%,明显高于对照组(2.4±1.6)%(P<0.01)。流产组Foxp3谱带密度相对值为0.30±0.018,低于正常组的0.68±0.025(P<0.05)。结论小鼠的自然流产模型建立成功,流产组孕鼠CD4+CD25+Treg的比例和Foxp3蛋白表达水平明显低于正常妊娠组,提示流产组高流产率可能与CD4+CD25+Treg数量和Foxp3的表达减少有关,CD4+CD25+Treg细胞的数量减少和功能缺陷可能是不明原因复发性流产的发生机制之一。

慢性乙型肝炎患者抗病毒治疗前后CD4^+CD25^+Foxp3^+调节性T细胞的变化

目的研究慢性乙型肝炎(以下简称乙肝)患者干扰素抗病毒治疗前后外周血CD4+CD25+Foxp3+调节性T细胞(Treg)频率的变化情况。方法慢性乙肝患者30例(干扰素组),经干扰素α1b(50μg)治疗6个月;肝炎病毒标志物阴性,肝功能正常的健康志愿者10例(正常对照组);尸检正常肝组织10例(尸检组)。采集干扰素组和正常对照组6个月前后的抗凝外周血,收集干扰素组抗病毒前和尸检组的肝组织。流式细胞术检测外周血Treg的频率(Treg/淋巴细胞的百分比);免疫组化检测肝组织中Foxp3的表达;逆转录-聚合酶链反应(RT-PCR)检测外周血Foxp3 mRNA的表达;并分析其与血清谷丙转氨酶(ALT)、谷草转氨酶(AST)、HBV DNA的相关性。结果干扰素组治疗前Treg的频率为(1.18±0.45)%,明显高于正常对照组的(0.55±0.13)%(P<0.01),Treg的频率与ALT、AST的变化均呈正相关(r=0.69、0.72,均P<0.01),而与HBV DNA无明显的相关性(r=-0.06,P>0.05);干扰素组治疗6个月后Treg的频率为(0.74±0.19)%,明显低于治疗前。免疫组化和RT-PCR可以对该结果鉴定和印证。结论慢性乙肝患者外周血中Treg的频率升高,干扰素α1b治疗能改善患者的免疫功能,降低Treg的频率。

胃癌患者外周血及癌组织中CD4^+ CD25^+调节性T细胞、转录因子Foxp3的表达及临床意义

目的探讨胃癌患者外周血及胃癌组织中CD4+CD25+调节性T细胞(Tregs)和转录因子Foxp3表达及临床意义。方法收集38例胃癌患者术前血液样本和20例健康体检者血液样本进行流式细胞仪检测,同时胃癌组中留取胃癌组织和癌旁组织(距肿瘤边缘>5 cm)进行免疫组化染色,检测CD4+CD25+Foxp3+Tregs表达,并与胃癌的TNM分期、肿瘤分化程度、淋巴转移、肿瘤所在部位、肿瘤直径等相关参数进行分析。结果胃癌组外周血中CD4+CD25+Foxp3+Tregs的表达水平与对照组相比差异有统计学意义(P<0.01),且在胃癌TNM分期、淋巴转移组内比较差异有统计学意义(P<0.01)。胃癌组织中Foxp3+Tregs的表达水平与癌旁组织相比,差异有统计学意义(P<0.01),且在胃癌TNM分期、分化程度、淋巴转移组内比较差异有统计学意义(P<0.01,P<0.05)。外周血中CD4+CD25+Foxp3+Tregs与胃癌组织中Foxp3+Tregs的表达水平呈显著正相关(r=0.786,P<0.01)。结论外周血中CD4+CD25+Foxp3+Tregs和组织中Foxp3+Tregs在胃癌患者中明显增加,且与胃癌发生、发展关系密切,可为胃癌的早期诊断和免疫治疗提供理论基础。

胃癌患者不同区域淋巴结和外周血CD4^+CD25^+Foxp3^+调节性T细胞的表达和临床意义

目的探讨胃癌患者不同区域淋巴结及外周血中CD4+CD25+Foxp3+调节性T细胞(Tregs)频数变化和临床意义。方法收集45例胃癌患者不同区域淋巴结及外周血标本,采用流式细胞仪检测各标本中Tregs占CD4+T细胞比例,并与胃癌TNM分期、分化程度等参数进行相关性分析。结果 Tregs在引流区阳性淋巴结、引流区阴性淋巴结、非引流区淋巴结、外周血中比例分别为(20.71±2.72)%、(14.43±2.62)%、(10.09±2.27)%、(9.72±2.13)%,前3组中两两相比均差异显著(P<0.05),后2组相比无显著差异(P>0.05)。引流区阳性淋巴结中Tregs细胞比例与肿瘤分期无显著相关(P>0.05);引流区阴性淋巴结、非引流区淋巴结、外周血中Tregs细胞比例与肿瘤分期相关(r=0.429、0.453、0.367;P<0.05),且Ⅲ+Ⅳ期Tregs比例显著高于Ⅰ+Ⅱ期比例。不同区域淋巴结Tregs分布与年龄、性别、肿瘤部位、病理分化间差异无相关性。结论 Tregs在不同区域淋巴结及外周血中分布表达呈递减趋势,可能是导致胃癌淋巴结微环境内出现局部免疫抑制,导致肿瘤细胞发生免疫逃逸的重要因素。

高表达Foxp3的肺癌细胞抑制人CD4＋T细胞免疫活性

目的:研究高表达转录因子Foxp3的肺癌细胞对CD4^+T淋巴细胞的作用。方法:利用脂质体转染法建立稳定高表达Foxp3的NCIH-h Foxp3肺癌细胞株,荧光定量PCR和Western blot检测细胞Foxp3的表达;ELISA法检测NCIHh Foxp3培养上清中IL-8、IL-10表达量的变化;分离并活化CD4^+T淋巴细胞,用含20%NCIH-h Foxp3肿瘤上清的培养基培养,检测CD4^+T淋巴细胞IL-2表达量的变化;将NCIH-h Foxp3与活化的CD4^+T淋巴细胞共培养,MTT评价免疫效应细胞增殖情况;免疫细胞化学法观察NCIH-h Foxp3细胞对活化CD4^+T淋巴细胞黏附作用的抑制。结果:建立高表达Foxp3的NCIHh Foxp3肺癌细胞株,与阴性对照相比,NCIH-h Foxp3细胞培养上清IL-8表达量降低,IL-10表达量升高,NCIH-h Foxp3肿瘤细胞能抑制活化的CD4^+T淋巴细胞IL-2的表达、增殖及浸润。结论:肺癌细胞Foxp3的表达对活化的CD4^+T淋巴细胞有免疫抑制作用,这可能与NCIH-h Foxp3分泌细胞因子IL-8表达量降低,IL-10表达量升高有关。