Peripheral CD4^(+)CD8^(+) double positive T cells:A potential marker to evaluate renal impairment susceptibility during systemic lupus erythematosus

Lupus nephritis(LN) has a high incidence in systemic lupus erythematosus(SLE) patients, but there is a lack of sensitive predictive markers. The purpose of the study was to investigate the association between the CD4^(+)CD8^(+)double positive T(DPT) lymphocytes and LN. The study included patients with SLE without renal impairment(SLE-NRI), LN, nephritic syndrome(NS), or nephritis. Peripheral blood lymphocyte subsets were analyzed by flow cytometry. Biochemical measurements were performed with peripheral blood in accordance with the recommendations proposed by the National Center for Clinical Laboratories. The proportions of DPT cells in the LN group were significantly higher than that in the SLE-NRI group(t=4.012, P<0.001), NS group(t=3.240,P=0.001), and nephritis group(t=2.57, P=0.011). In the LN group, the risk of renal impairment increased significantly in a DPT cells proportion-dependent manner. The risk of LN was 5.136 times(95% confidence interval, 2.115–12.473) higher in cases with a high proportion of DPT cells than those whose proportion of DPT cells within the normal range. These findings indicated that the proportion of DPT cells could be a potential marker to evaluate LN susceptibility, and the interference of NS and nephritis could be effectively excluded when assessing the risk of renal impairment during SLE with DPT cell proportion.

Glutamine deprivation impairs function of infiltrating CD8^(+)T cells in hepatocellular carcinoma by inducing mitochondrial damage and apoptosis

BACKGROUND The functions of infiltrating CD8^(+)T cells are often impaired due to tumor cells causing nutrient deprivation in the tumor microenvironment.Thus,the mechanisms of CD8^(+)T cell dysfunction have become a hot research topic,and there is increased interest on how changes in metabolomics correlate with CD8^(+)T cell dysfunction.AIM To investigate whether and how glutamine metabolism affects the function of infiltrating CD8^(+)T cells in hepatocellular carcinoma.METHODS Immunohistochemical staining and immunofluorescence were performed on surgically resected liver tissues from patients.Differentially expressed genes in infiltrating CD8^(+)T cells in hepatocellular carcinoma were detected using RNA sequencing.Activated CD8^(+)T cells were co-cultured with Huh-7 cells for 3 d.The function and mitochondrial status of CD8^(+)T cells were analyzed by flow cytometry,quantitative real-time polymerase chain reaction,and transmission electron microscopy.Next,CD8^(+)T cells were treated with the mitochondrial protective and damaging agents.Functional alterations in CD8^(+)T cells were detected by flow cytometry.Then,complete medium without glutamine was used to culture cells and their functional changes and mitochondrial status were detected.RESULTS There were a large number of infiltrating PD-1+CD8^(+)T cells in liver cancer tissues.Next,we cocultured CD8^(+)T cells and Huh-7 cells to explore the regulatory effect of hepatoma cells on CD8^(+)T cells.Flow cytometry results revealed increased PD-1 expression and decreased secretion of perforin(PRF1)and granzyme B(GZMB)by CD8^(+)T cells in the co-culture group.Meanwhile,JC-1 staining was decreased and the levels of reactive oxygen species and apoptosis were increased in CD8^(+)T cells of the co-culture group;additionally,the mitochondria of these cells were swollen.When CD8^(+)T cells were treated with the mitochondrial protective and damaging agents,their function was restored and inhibited,respectively,through the mitochondrial damage and apoptotic pathways.Subsequently,complete medium without glutamine was used to culture cells.As expected,CD8^(+)T cells showed functional downregulation,mitochondrial damage,and apoptosis.CONCLUSION Glutamine deprivation impairs the function of infiltrating CD8^(+)T cells in hepatocellular carcinoma through the mitochondrial damage and apoptotic pathways.

Correlation between CD4^＋CD25^＋Treg Cells and CCR4 in Nasopharyngeal Carcinoma

OBJECTIVE CD4^＋CD25^＋ T regulatory （Treg） cells are a population of T cells which suppress an overactive immune system. CCR4 is a chemokine receptor involved in the recruitment of lymphocytes. Nasopharyngeal carcinoma （NPC） is resistant to immunosurveillance, owing to the increased number of tumor-infiltrating Treg cells which are recruited to the tumor bv CCR4.

原发性肝癌患者外周血CD4^(+)T、CD8^(+)T、Tc17、Th17和Treg淋巴细胞的变化及其意义

目的了解原发性肝癌(PLC)患者外周血CD4^(+)T、CD8^(+)T、Tc17、Th17和Treg淋巴细胞的变化。方法2018年6月~2019年12月我院诊治的PLC患者83例(巴塞罗那临床肝癌分期A期25例,B期23例,C期18例,D期17例)和健康人35例,采用流式细胞技术检测外周血CD4^(+)T、CD8^(+)T及Tc17(CD8^(+)IL-17)、Th17(CD4^(+)IL-17)和CD4^(+)CD25^(+)CD45RA^(+)Treg淋巴细胞百分比。结果PLC患者外周血CD4^(+)T淋巴细胞百分比为(32.8±8.5)%,显著低于健康人[(43.3±7.4)%,P<0.05],CD4^(+)/CD8^(+)细胞比值为(0.9±0.3),显著低于健康人[(1.2±0.1),P<0.05];PLC患者外周血Treg细胞[(6.4±0.9)%对(3.0±0.1)%]、Th17细胞[(5.0±1.1)%对(3.1±1.5)%]及Tc17细胞[(2.3±0.4)%对(1.0±0.2)%],均较健康人显著升高(P<0.05);BCLC C/D期患者外周血CD4^(+)CD25^(+)CD45RA^(+)Treg细胞百分比较A/B期患者显著升高[(7.6±0.4)%对(5.3±0.5)%,P<0.001],Th17(CD4^(+)IL-17)和Tc17(CD8^(+)IL-17)细胞百分比较A/B期亦显著升高[分别为(6.9±1.1)%对(5.4±0.6)%,P<0.01和(2.8±0.6)%对(1.6±0.4)%,P<0.01]。结论PLC患者外周血淋巴细胞亚群出现异常改变,可能与肿瘤的分期密切相关,为从免疫学角度开展调节T淋巴细胞失衡的免疫治疗提供了理论依据。

Effect of Mg^(2+)level on the functions of CD8^(+)T lymphocytes and NK cells in patients with COVID-19

Objective:To investigate the changes of Mg^(2+) levels in serum and peripheral blood mononuclear cells(PBMCs)of patients with COVID-19 and its effects on the functions of CD8^(+)T lymphocytes and NK cells.Methods:A total of 165 COVID-19 patients hospitalized in Ezhou Central Hospital from January 20 to February 20,2020 were divided into mild/common group(98 cases)and severe/critical group(67 cases).At the same time,34 healthy persons were selected as the control group.Peripheral blood was collected and PBMCs were isolated,the level of Mg^(2+) in serum and PBMCs was detected.The subsets of CD8^(+)T lymphocytes and NK cell and the expression levels of their surface inhibitory molecular PD-1 and activator molecular NKG2D were detected by flow cytometry.The correlation between Mg^(2+) concentration and the expression levels of PD-1 and NKG2D was also analyzed.Results:Compared with the control group,the concentration of Mg^(2+) in serum and PBMCs,the counts of CD8^(+)T lymphocytes and NK cell in patients with mild/common and severe/critical groups were significantly reduced(P<0.05),while the expression level of surface inhibitory molecular PD-1 were significantly increased(P<0.05),while the expression level of the activation molecule NKG2D were significantly decreased(P<0.05).However,the changes of the above indicators in patients with severe/critical group were greater than those in the mild/common group(P<0.05).In addition,the Mg^(2+) concentration in COVID-19 patients was negatively correlated with the expression level of PD-1 on CD8^(+)T lymphocytes and NK cells(P<0.05),and positively correlated with the expression levels of NKG2D(P<0.05).Conclusion:The concentration of Mg^(2+) in the serum and PBMCs of COVID-19 patients is significantly reduced,which may cause the function of CD8^(+)T lymphocytes and NK cells to be inhibited.

Revolutionizing tumor immunotherapy:unleashing the power of progenitor exhausted T cells

In exploring persistent infections and malignancies, a distinctive subgroup of CD8^(+) T cells, progenitor exhausted CD8^(+) T(Tpex) cells, has been identified. These Tpex cells are notable for their remarkable self-renewal and rapid proliferation abilities. Recent strides in immunotherapy have demonstrated that Tpex cells expand and differentiate into responsive exhausted CD8^(+) T cells, thus underscoring their critical role in the immunotherapeutic retort. Clinical examinations have further clarified a robust positive correlation between the proportional abundance of Tpex cells and enhanced clinical prognosis. Tpex cells have found noteworthy applications in the formulation of inventive immunotherapeutic approaches against tumors. This review describes the functions of Tpex cells in the tumor milieu, particularly their potential utility in tumor immunotherapy. Precisely directing Tpex cells may be essential to achieving successful outcomes in immunotherapy against tumors.

胃癌患者血清IL-21与Treg细胞及CD4^+/CD8^+T细胞的相关性研究

目的探究胃癌患者血清IL-21与Treg细胞及CD4^+/CD8^+T细胞的关系。方法随机选取2014年12月—2016年12月100例血清样本,50例为胃癌患者,50例为健康人群。对所有待测患者外周血进行IL-21与Treg细胞及CD4^+/CD8^+T细胞的表达情况进行检测。结果研究表明,实验组与对照组在IL-21与Treg细胞及CD4^+/CD8^+T细胞的表达情况上差异有统计学意义(P<0.05)。结论 IL-21与Treg细胞及CD4^+/CD8^+T细胞的表达情况能检测出患者是否有胃癌,可以用于临床诊断,患者的表达值与患者的病理特征存在相关性。

HBV慢性感染者肝脏组织中CD4^+T、CD8^+T和FoxP3^+Tregs细胞的表达水平

目的:计数慢性乙型肝炎病毒(HBV)感染者肝脏组织中CD4^+T、CD8^+T和Fox P3^+Tregs细胞,观察不同免疫状态下的肝脏组织中CD4^+T和CD8^+T细胞表达水平之间的差异,探索其临床意义。方法:选取慢性HBV感染者68例,健康对照组(非HBV感染组)30例,运用免疫组织化学的方法进行检测。结果:慢性HBV感染组的CD4^+T、CD8^+T和Fox P3^+Tregs细胞表达水平明显升高,与非HBV感染组相比,P均<0.001;在HBV感染组中,CD4^+T和CD8^+T细胞在免疫耐受期患者肝脏组织中的表达水平最低,CD4^+T、CD8^+T细胞在免疫清除期、再活动期中的表达水平与二者在免疫耐受期相比,均有增高趋势,然而CD4^+T、CD8^+T细胞的表达水平在免疫耐受期、免疫清除期、低复制期及再活动期任意两期之间比较,P均>0.05。结论:CD4^+T和CD8^+T细胞在免疫耐受期、免疫清除期、低复制期及再活动期患者肝脏组织中表达水平的变化趋势在一定程度上反应了各期肝脏的免疫状态;Fox P3^+Tregs细胞可能与HBV感染慢性化有关。

乳腺癌患者手术前后外周血CD4^+和CD8^+及Treg细胞的表达及临床意义

目的观察手术前后乳腺癌患者体内血CD4+T细胞、CD8+T细胞和Treg细胞的表达及临床意义。方法选择2016年1月至2018年8月本院收治的原发性乳腺癌患者83例为病例组,检测其术前、术后外周血CD4^+T细胞、CD8^+T细胞和Treg细胞的变化,同时选取60例健康成年妇女作为对照组,检测其外周血中CD4+T细胞、CD8^+T细胞和Treg细胞的表达情况。分析CD4^+T细胞、CD8^+T细胞和Treg细胞的变化与临床病理参数的关系。结果与对照组相比,乳腺癌患者术前CD4^+T细胞、Treg细胞明显增加,差异有统计学意义(P<0.05);与Ⅰ期患者相比,Ⅱ~Ⅲ期患者术前CD4^+T细胞、Treg细胞增加更明显,差异有统计学意义(P<0.05);乳腺癌患者术后CD4^+T细胞含量降低、CD8^+T细胞含量增加,差异有统计学意义(P<0.05)。结论外周血Treg细胞、CD4+T细胞和CD8^+T细胞水平对于乳腺癌的诊断和预后有一定价值,值得进行深入探讨并将其应用于临床。手术切除肿瘤可在一定程度上改善机体免疫状态,对预后产生积极作用。

An Association between Immunosenescence and CD4^+CD25^+ Regulatory T Cells: A Systematic Review

Objective Age-related increment of the prevalence of CD4^＋CD25^＋ regulatory T （Treg） cells were described controversially, and whether such changes explain immune dysfunction in the elderly is still unclear. The aim of this systematic review is to evaluate the role of the Tregs in immunosenescence. Methods Medline and manual searches were performed to identify all published epidemiological and animal studies investigating the efficacy of the association between immunosenescence and Treg cells. Results It was founded that the frequency, phenotypic characteristics, and number/function of Tregs were altered significantly with aging. Medical conditions in individuals with advanced ageas well as apoptosis intensity of Treg cells had an impact on the accumulation of Tregs which in turn could deteriorate cytotoxic activity of CD8＋ T and NK cells and production of IL-2. The range of immune cells that could be suppressed by Treg cells was quite wide and covered CD4^＋CD25^＋ T cells, NK cells, dendritic cells and even monocytes. These changes were observed both in humans and experimental animals. Besides, it was believed that frequency of Tregs increased with age and was accompanied by intensified suppressive activity for Tregs in patients, for example, with Alzheimer disease （AD） and Parkinson disease （PD）. The impaired condition of CD4＋ T cells, so-called immunosenescence, rendered transplant recipients less responsive to an allogeneic kidney graft, an effect that was limited to transplant recipients who were aged over 60 years. Conclusions Treg cells are associated with immunosenescence. All these changes contribute to the aging-related decline of immune responses and lead to the higher risk of immune-mediated diseases, cancer or infections in aged individuals.

Expression of PD1 and BTLA on the CD8^+T Cell and γδT Cell Subsets in Peripheral Blood of Non-Small Cell Lung Cancer Patients

Objective To investigate the expression and regulation of programmed cell death protein 1(PD1),B lymphocyte and T lymphocyte attenuator(BTLA)in peripheral blood of patients with non-small cell lung cancer(NSCLC);to examine the correlation of the mRNA levels between PD and BTLA in NSCLC.Methods Flow cytometry was used to detect the expression of PD1 and BTLA on the surfaces of CD8^+T cells andγδ+T cells in the peripheral blood samples collected from 32 in-patients with stage IV NSCLC and 30 healthy individuals.We compared the expression of PD1 and BTLA on the surfaces ofγδ+T cells in the NSCLC patients with bone metastasis before and after the treatment of zoledronic acid.The correlations of PD1 and BTLA,as well as their ligands were analyzed using Pearson correlation analysis with the cBioPortal data platform.Results The frequency of PD1 on the surfaces of CD8^+T cells was significantly higher than that of theγδT cells in both healthy controls(t=2.324,P=0.024)and NSCLC patients(t=2.498,P=0.015).The frequency of PD1 on CD8^+T cells,rather than onγδ+T cells,was significantly upregulated in advanced NSCLC patients compared with that in healthy controls(t=4.829,P<0.001).The PD1+BTLA+γδT cells of the healthy controls were significantly lower than that of the NSCLC patients(t=2.422,P=0.0185).No differences in percentage of PD1+γδ+and BTLA+γδ+T cells were observed in 7 NSCLC patients with bone metastasis before and after zoledronic acid treatment.PD1 was positively correlated with BTLA in both lung adenocarcinoma(r=0.54;P<0.05)and lung squamous cell carcinoma(r=0.78;P<0.05).Conclusions The upregulation of co-inhibitory molecules occurs on the surfaces of both CD8^+T cells andγδT cells in advanced NSCLC,suggesting that these molecules were involved in regulating the inactivation of CD8^+T cells andγδ+T cells,immune escape and tumor invasion.

外周血CD4^(+)CD25^(+)Treg、CD3^(+)、NK+Caspase 8^(+)在免疫性血小板减少性紫癜患者中的检测意义

目的探究外周血CD4^(+)CD25^(+)Treg、CD3^(+)、NK+Caspase-8^(+)在免疫性血小板减少性紫癜(ITP)患者中的检测意义。方法选取2019年10月~2020年1月我院收治30例ITP患者设为观察组。同期纳入30例健康志愿者设为对照组,比较两组外周血CD4^(+)CD25^(+)Treg、CD3^(+)、NK+Caspase-8^(+)水平,并采用Pearson法分析上述指标与血小板计数相关性。结果观察组外周血CD4^(+)CD25^(+)Treg、CD3^(+)低于对照组,NK+Caspase-8^(+)水平高于对照组(P<0.05);经Pearson相关性分析提示,血小板计数与外周血CD4^(+)CD25^(+)Treg、CD3^(+)水平呈正相关,与NK+Caspase-8^(+)水平呈负相关(P<0.05)。结论ITP患者外周血CD4^(+)CD25^(+)Treg、CD3^(+)水平降低,NK+Caspase-8^(+)呈高表达状态,提示ITP的发生发展与细胞免疫调控异常、凋亡信号异常密切相关,为临床治疗提供有力依据。

子痫前期患者外周血CD8^+CD25^+FoxP3^+调节T细胞的变化及意义

目的:探讨外周血CD8^+CD25^+FoxP3^+调节T细胞(Treg)在子痫前期(PE)疾病过程中的作用。方法:研究对象包括子痫前期孕晚期患者46例,其中轻度子痫24例(MPE组),重度子痫22例(SPE组),并选择24例与患者孕龄匹配的健康孕妇作为对照组(HP组)。流式细胞仪检测分析外周血CD8^+CD25^+FoxP3^+Treg比例;Luminex200检测血清IL-6、IL-17A、IL-10、IL-1β、IL-33和TGF-β1浓度。分离10例健康对照者单个核细胞(PBMCs),IL-33刺激培养后检测CD8^+CD25^+ FoxP3^+ Treg比例的变化。结果:MPE和SPE组CD8^+CD25^+FoxP3^+Treg比例分别为[0.32(0.19-0.63)%]、[0.13(0.02-0.41)%],两组均低于HP组[0.48(0.21-0.96)%],三组差异有统计学意义(P<0.05)。与HP组相比,MPE组和SPE组血清IL-6、IL-17A浓度均升高,且SPE组患者血清IL-6、IL-17A浓度升高更明显,差异有统计学意义(P<0.05);IL-10、IL-1β和IL-33浓度在HP、MPE及SPE三组间差异无统计学意义(P>0.05);与HP对照者相比,MPE和SPE组血清TGF-β浓度均升高,差异有统计学意义(P<0.05);但MPE和SPE组之间差异无统计学意义(P>0.05)。PE患者CD8^+CD25^+FoxP3^+Treg比例与血清IL-17A负相关(r=-0.338,P=0.021),与IL-33正相关(r=0.548,P=0.001)。PBMCs用IL-33刺激5 d后,与空白对照组相比,CD8^+CD25^+ FoxP3^+Treg比例显著增高(P<0.05)。结论:子痫前期患者外周血CD8^+CD25^+FoxP3^+Treg细胞比例降低可能在其疾病过程中发挥重要作用。

CD4^+CD25^+和CD8^+调节性T细胞的作用机制

调节性T细胞(Treg)主要在机体免疫系统中发挥负向调节作用,既能抑制不恰当的免疫反应,又能限定免疫应答的范围、程度及作用时间,对CD4+和CD8+效应性T淋巴细胞的增殖起抑制作用,因此在移植物抗宿主病、自身免疫病、过敏性疾病等的发病机制和临床治疗中有潜在的应用价值。本文重点介绍CD4+CD25+Treg和CD8+Treg的作用机制,并简述调节性T细胞研究面临的挑战与展望。

NOD小鼠人源化后CD4~＋ Tregs和CD8~＋ Tregs频率和功能变化及意义

目的观察NOD小鼠人源化后,CD4^+和CD8^+调节性T细胞(regulatory T cells,Tregs)频率和功能的变化,揭示Tregs在人源化NOD小鼠1型糖尿病中的作用及免疫学机制可能的变化。方法流式细胞术分别分析12周龄未发病的人源化NOD小鼠和NOD小鼠脾淋巴细胞和胰腺淋巴结细胞中CD8^+CD122^+T、CD8^+CD28-T、CD8^+CD25^+Foxp3^+T和CD4^+CD25^+Foxp3^+T细胞的频率,并采用3H-Td R掺入法检测脾CD4^+CD25^+T和CD8^+CD25^+T细胞的免疫抑制功能。结果人源化NOD小鼠和NOD小鼠的脾淋巴细胞和胰腺淋巴结细胞中CD4^+CD25^+Foxp3^+T细胞频率无显著性差异(P>0.05),而人源化NOD小鼠脾淋巴细胞和胰腺淋巴结细胞中CD8^+CD122^+T、CD8^+CD28-T、CD8^+CD25^+Foxp3^+T细胞等CD8^+Tregs亚群的频率较NOD小鼠都显著降低,但NOD小鼠人源化后,CD4^+CD25^+T和CD8^+CD25^+T细胞的免疫抑制功能并没有显著性差异;同时与人源化NOD小鼠相比,NOD小鼠的胰腺淋巴结细胞中CD8^+T细胞频率更低。结论人源化NOD小鼠脾脏和胰腺淋巴结中CD8^+Tregs亚群频率的降低,引起其胰腺淋巴结中CD8^+T细胞频率的升高,导致胰岛β细胞破坏更严重,可能是引起人源化NOD小鼠自发1型糖尿病较NOD小鼠明显提前且加重的因素之一。

CD8^+调节性T细胞与器官移植

调节性T细胞（regulatory T cells，Treg）在维持机体免疫平衡方面发挥关键作用，对于器官移植术后诱导治疗和维持免疫耐受具有重要意义。

CD8^+T细胞依赖的急性移植物抗宿主病小鼠模型的建立

目的建立CD8^+T细胞依赖的急性移植物抗宿主病(GVHD)小鼠模型。方法分别以主要组织相容性抗原(MHC)相同,而次要组织相容性抗原(miHAs)不同的8～12周龄C3H．SW(H-2D^b,CD45．2^+)和B6/SJL(H-2D^b,CD45．1^+)雌性小鼠为供受体,从供体骨髓分离去除T细胞的骨髓细胞(T BM),与其脾脏和淋巴结来源的CD8^+T细胞混合,经尾静脉输注给受致死剂量^(137)γ照射的受体鼠。观察移植后受体的体重、毛色、皮肤和生存率的变化,并用流式细胞术(FACS)和组织病理学进一步分析受鼠靶器官细胞浸润和损伤状况。结果移植后受体鼠出现体重明显减轻、毛发脱落、皮肤溃疡等表现,并在28d后出现死亡；FACS证实浸润受鼠骨髓、脾脏和肝脏的细胞主要为CD45．2^+的供鼠细胞,实验组中还有大量CD45．2^+CD8^+T细胞浸润；组织病理学发现肝脏中大量淋巴细胞浸润,皮肤结构破坏,组织坏死。结论成功建立了miHAs不匹配的异基因骨髓移植诱导的CD8^+ T细胞依赖的GVHD动物模型,该模型模拟了目前临床病人采用的同种异基因骨髓移植配型方式,可为异基因骨髓移植GVHD发病机理及该病的防治研究提供良好的实验平台和工具。

CD4^(+)CD45RC^(low)Treg在大鼠肝移植免疫耐受中的调节作用研究

目的探讨CD4^(+)CD45RC^(low)调节性T细胞(Treg)在肝移植免疫耐受诱导中的作用。方法建立急性排斥反应(AR)[Lewis→Brown Norway(BN),AR组]与自发耐受(BN→Lewis,耐受组)大鼠肝移植模型,每组6只。并设立假手术组(对照组),Lewis大鼠和BN大鼠各3只。对各组大鼠肝组织进行病理学检查;检测各组大鼠外周血、移植肝、脾脏T细胞亚群和浆细胞样树突状细胞(pDC)的表达情况,分析pDC与CD4^(+)CD45RC^(low)Treg的相关性;检测各组大鼠移植肝和脾脏CD4、CD45RC、CD103的表达情况。结果AR组大鼠病理学主要表现为移植肝炎症细胞浸润和组织结构紊乱。与AR组大鼠比较,耐受组大鼠外周血CD4^(+)CD25^(+)Treg、CD8^(+)Treg表达水平均升高(均为P<0.05)。外周血CD4^(+)CD25^(+)Treg与CD8^(+)Treg表达水平呈正相关(r=0.742,P=0.022)。AR组大鼠外周血CD4+CD45RChighT细胞水平高于耐受组和对照组大鼠(均为P<0.05)。与AR组大鼠比较,耐受组大鼠脾脏CD4+CD45RClowTreg表达水平升高,外周血、移植肝、脾脏CD8^(+)CD45RC^(low)Treg表达水平均升高(均为P<0.05)。与对照组和AR组大鼠比较,耐受组大鼠外周血CD8^(+)CD45RC^(low)Treg/CD8+T比值升高,外周血、移植肝、脾脏中pDC的表达水平均升高(均为P<0.05);且CD4^(+)CD45RC^(low)Treg与pDC表达水平的变化呈正相关(r=0.506,P=0.016)。耐受组大鼠移植肝和脾脏CD4、CD45RC、CD103的表达均增多;而AR组大鼠移植肝CD4、CD45RC的表达增多,CD103表达降低。结论CD4+CD45RClowTreg是具有负向免疫调控作用的细胞亚群,与CD8^(+)CD45RC^(low)Treg及pDC等构成免疫耐受诱导的调节性细胞网络。

肿瘤相关巨噬细胞及CD8^(+)/CD68^(+)细胞比值是影响肺腺癌患者预后的独立危险因素

目的:探讨CD68^(+)肿瘤相关巨噬细胞(TAM)、CD8^(+)T细胞、Foxp3^(+)Treg细胞等在肺腺癌(LUAD)组织中浸润分布及其与患者预后的关系。方法:收集2004年9月至2009年4月间在苏州大学附属第三医院手术切除的93例LUAD组织及78例癌旁组织,采用组织芯片(TMA)及多重免疫荧光(mIF)技术检测其中的免疫细胞浸润与分布,Wilcoxon秩和检验比较癌与癌旁组织、癌巢与间质中浸润水平的差异,χ^(2)检验分析其浸润水平及CD8^(+)/CD68^(+)细胞比值与临床病理特征的关系,Kaplan-Meier法和COX模型分析影响患者OS的潜在危险因素。结果:与癌旁组织比较,癌组织中CD68^(+)TAM、CD8^(+)T细胞、Foxp3^(+)Treg细胞浸润水平均显著增加(均P<0.01),间质CD68^(+)TAM、CD8^(+)T细胞的浸润水平均显著高于癌巢(均P<0.01)。总CD68^(+)TAM、癌巢及间质CD68^(+)TAM浸润水平与淋巴结转移呈正向关联(均P<0.05),癌巢CD68^(+)TAM浸润水平与T分期呈正向关联(P<0.05),间质CD68^(+)TAM浸润水平与病理分级呈正向关联(P<0.05);癌组织中CD8^(+)/CD68^(+)细胞比值与病理分级、淋巴结转移均呈负向关联(均P<0.05)。Kaplan-Meier生存分析显示,LUAD组织中总CD68^(+)TAM、癌巢及间质CD68^(+)TAM高浸润患者OS均短于低浸润患者(P<0.05或P<0.01)、癌组织中CD8^(+)/CD68^(+)细胞比值高患者OS显著长于低比值患者(P<0.05)。多因素COX模型分析示,LUAD患者年龄、TNM分期及癌组织中CD8^(+)/CD68^(+)细胞比值是影响患者预后的独立风险因素(P<0.05或P<0.01)。结论:高度浸润的CD68^(+)TAM与LUAD的进展、侵袭、转移和不良预后显著关联,而高CD8^(+)/CD68^(+)细胞比值是影响LUAD患者OS的独立保护因素。

CD8^(+)CD25^(+)调节性T细胞在疾病中的研究进展

CD8^(+)CD25^(+)Treg具有抑制免疫反应和诱导免疫耐受作用。本文综述了CD8^(+)CD25^(+)Treg在恶性肿瘤、自身免疫性疾病及其他常见病如哮喘、过敏性疾病、2型糖尿病、子痫前期中的变化及相应的作用机制,CD8^(+)CD25^(+)Treg在不同疾病中的变化不一致,在恶性疾病中升高,而在自身免疫性疾病中降低。进一步加深对CD8^(+)CD25^(+)Treg的认识将为疾病的防治及预后提供依据。