CD4+T细胞与肿瘤免疫

在肿瘤免疫中细胞免疫发挥着重要作用,其中T细胞介导的特异性免疫应答反应更为重要.近年来CD4+T细胞在抗肿瘤免疫中的作用越来越受到重视.在肿瘤免疫中CD4+T细胞启动后可以通过多种机制启动细胞毒性T淋巴细胞(CTL),维持和加强CTL的抗肿瘤反应,并且可以作为效应细胞发挥抗肿瘤作用,CD4+T细胞中的一个亚群细胞CD4+ CD25+T调节细胞对肿瘤免疫有抑制作用.     

CD4~+T 细胞与肿瘤免疫

CD4~+T细胞不仅辅助激活CD8~+T细胞,而且对记忆性细胞毒性T淋巴细胞(CTL)应答的产生和维持起重要作用,并具有直接的抗肿瘤功能.另外,CD4~+CD25~+ 调节性T细胞(Tregs)具有免疫负调控功能,在肿瘤免疫抑制及免疫逃逸中发挥重要作用,是肿瘤免疫治疗失败的重要原因.近年肿瘤免疫治疗已获得很大进步,相关肿瘤疫苗的研究也备受关注.     

CD4+T细胞在肝细胞癌中的作用

CD4+T细胞为一系列多功能细胞,研究发现肝细胞癌(HCC)中大部分CD4+T细胞亚群可通过活化或抑制机体固有免疫细胞、适应性免疫细胞及非免疫细胞等,参与肿瘤血管生成及浸润、肿瘤细胞凋亡、急性期蛋白及促癌基因的表达,进而发挥肿瘤促进或抑制作用.     

CD4+/CD8+ T淋巴细胞在肝细胞癌组织中的浸润及与预后的相关性研究

目的 检测CD4⁺/CD8⁺ T淋巴细胞在肝细胞癌（hepatocellular carcinoma,HCC）组织中的浸润程度,并分析其与预后的相关性。方法 收集行肝切除术的HCC患者215例,采用免疫组化技术检测CD4⁺/CD8⁺ T淋巴细胞在HCC癌组织中的浸润程度,根据浸润情况比较患者肝切除术后无瘤生存率和总生存率。结果 CD4⁺ T淋巴细胞高浸润和低浸润比例分别为60.9%和39.1%。CD4⁺ T淋巴细胞高浸润组患者总生存率和无瘤生存率均显著高于低浸润组（P=0.015,P=0.038）。CD8⁺ T淋巴细胞高浸润和低浸润比例分别为34.9%和65.1%。CD8⁺ T淋巴细胞高浸润组患者的总生存率和无瘤生存率亦显著高于低浸润组患者（P=0.033,P=0.047）。结论 CD4⁺或CD8⁺ T淋巴细胞低浸润可能与HCC患者术后不良预后相关。     

Identification of new NY-ESO-1 epitopes recognized by CD4+ T cells and presented by HLA-DQ B1 03011

NY-ESO-1 is one of the most immunogenic cancer antigens eliciting strong humoral and cellular immune responses in patients with NY-ESO-1-expressing malignancies. Since CD4+ T cells play a critical role in generating and maintaining antigen-specific cellular and humoral immune responses, we searched for new NY-ESO-1 epitopes presented by MHC class II molecules. CD4+ T cells of patients with NY-ESO-1-expressing cancer were presensitized with 18-mer overlapping synthetic peptides spanning the entire sequence of NY-ESO-1. Two partly overlapping NY-ESO-1 epitopes p49-66 and p55-72 were identified as targets for NY-ESO-1-specific CD4+ T cells. Peptide-specific CD4+ T-cell clones were generated by repetitive stimulation with NY-ESO-1 p49-66 and p55-72. Further experiments confirmed distinct specificities for the CD4+ T-cell clones indicating that at least 2 different CD4+ T-cell epitopes are located in the region p49-72 of the NY-ESO-1 sequence. Using a set of partially histocompatible EBV-B cell lines and MHC class II-specific antibodies, we found that both CD4+ T-cell epitopes were presented in the context of HLA-DQ B1 03011(DQ7). Natural processing and presentation of these epitopes was demonstrated by recognition of an HLA-DQ B1 03011- and NY-ESO-1-expressing lymphoma cell line and by recognition of dendritic cells (DC) exogenously loaded with NY-ESO-1 protein or infected with recombinant NY-ESO-1 adenoviral constructs. The specific production of IFN-gamma and TNF-alpha suggests that the NY-ESO-1-specific CD4+ T-cell clones belong to the Th1 subtype. The characterization of the new HLA-DQ B1 03011-restricted NY-ESO-1 peptides broadens the repertoire of epitopes that can be used to monitor NY-ESO-1-specific spontaneous and vaccine-induced T-cell responses in cancer patients.     

原发性肝细胞癌微环境中CD4^＋CD25^＋调节性T细胞分布与局部免疫的关系

目的通过检测原发性肝细胞癌（hepatocellular carcinoma,HCC）局部肝癌组织和癌旁组织中T细胞亚群的分布情况,探讨在肝癌发生、发展过程中CD4^＋CD25^＋调节性T细胞与局部免疫状态的关系。方法54例肝癌组织和癌旁组织及10例正常肝组织用免疫组织化学S—P法标记CD4^＋T细胞、CD8^＋T细胞及CD4^＋CD25^＋调节性T细胞（CD4^＋CD25^＋Tr细胞）,并对组织中CD4^＋CD25^＋Tr细胞与CD4^＋T、CD8^＋T及CD4^＋T／CD8^＋T值进行相关性分析。结果54例肝癌、癌旁组织中CD4^＋CD25^＋Tr细胞单个高倍视野平均数分别为5．6208±2．7235和3．8554±1．6018（P=0．001）;肝癌中CD4^＋CD25^＋Tr细胞数目与肿瘤大小、有无子灶有关,组间差异有显著性（P〈0．01）;肝癌中CD4^＋CD25^＋Tr数量与CD4^＋T细胞的数量以及CD4^＋T／CD8^＋T值呈显著负相关（r=-0．459,P=0．015;r=-0．563,P=0．011）,而与浸润性CD8^＋T细胞的数量分布无关（r=-0．485,P=0．072）。结论在肝癌微环境中CD4^＋T淋巴细胞表达降低,CD4^＋CD25^＋Tr细胞表达增高,后者可能通过抑制CD4^＋T淋巴细胞的增殖来抑制肝癌局部免疫,从而促进肿瘤的进展以及侵袭或转移。     

CIITA‐driven MHC‐II positive tumor cells: Preventive vaccines and superior generators of antitumor CD4+ T lymphocytes for immunotherapy

In our study, we have investigated whether tumors of distinct histological origin can be rejected if expressing CIITA‐driven MHC class II molecules. Moreover, we assessed whether antitumor lymphocytes generated by this approach could be used as an immunotherapeutic tool for established cancers. Stable CIITA‐transfectants of C51colon adenocarcinoma, RENCA renal adenocarcinoma, WEHI‐164 sarcoma as well as TS/A mammary adenocarcinoma were generated. Tumor cells transfectants were injected in vivo, and their growth kinetics and recipient's immune response were analyzed. Tumor rejection and/or retardation of growth was found for the first 3 CIITA‐transfected tumor cell lines and confirmed for TS/A‐CIITA. Animals rejecting CIITA‐transfected tumors acquired specific immunological memory as demonstrated by resistance to challenge with parental tumors. Adoptive cell transfer experiments demonstrated that tumor immunity correlates with the efficient priming of CD4⁺ T helper cells and the consequent activation of CD8⁺ T lymphocytes. T cells from TS/A‐vaccinated mice were used in an adoptive immunotherapy model of established tumors. The results showed the cure at early stages and significantly prolonged survival at later stages of tumor progression. Importantly, CD4⁺ T cells were clearly superior to CD8⁺ T cells in antitumor protective function. Interestingly, the protective phenotype was associated to both a Th1 and Th2 polarization of the immune effectors. These results establish the general application of our tumor vaccine model and disclose the additional application of this strategy for producing better lymphocyte effectors for adoptive antitumor immunotherapy.     

非霍奇金淋巴瘤患者血中CD+4 CD+25 T细胞/CD+4 T细胞比率意义初探

  目的 探讨非霍奇金淋巴瘤（NHL）患者外周血中CD+4 CD+25 T细胞／CD+4 T细胞比率的意义。方法 应用流式细胞技术检测15例健康人、41例初诊NHL患者、16例CTOP方案化疗后完全缓解后的NHL患者及25例化疗后未达到完全缓解的患者单位体积内外周血中CD+4 CD+25 T细胞数量和CD+4 T细胞,计算CD+4 CD+25 T细胞占CD+4 T细胞的比率。结果 初诊NHL患者CD+4 CD+25 T细胞／CD+4 T细胞的比率为（7.54±2.31）％,高于健康者的（4.13±1.25）％（P＜0.05）;化疗完全缓解后NHL患者外周血CD+4 CD+25 T细胞／CD+4 T细胞的比率为（6.26±2.28）％,低于初诊化疗前患者的（7.54±2.31％）（P＜0.05）。化疗后未达到完全缓解患者CD+4 CD+25 T细胞／CD+4 T细胞的比率为（7.85±2.12）％,高于化疗后完全缓解的患者的比率（6.26±2.28）％（P＜0.05）。结论 化疗缓解后的NHL患者外周血中CD+4 CD+25 T细胞／CD+4 T细胞的比率较化疗前及化疗未缓解的患者降低,提示CD+4 CD+25 T细胞／CD+4 T细胞的比率可能与NHL患者免疫功能及治疗效果有关。     

CD4+T细胞与肿瘤免疫

在肿瘤免疫中细胞免疫发挥着重要作用,其中T细胞介导的特异性免疫应答反应更为重要.近年来CD4+T细胞在抗肿瘤免疫中的作用越来越受到重视.在肿瘤免疫中CD4+T细胞启动后可以通过多种机制启动细胞毒性T淋巴细胞(CTL),维持和加强CTL的抗肿瘤反应,并且可以作为效应细胞发挥抗肿瘤作用,CD4+T细胞中的一个亚群细胞CD4+ CD25+T调节细胞对肿瘤免疫有抑制作用.     

CD4+CD25+调节性T细胞与CD4+T、CD8+T细胞在结直肠癌组织中的分布

 目的 分析CD4+CD25+ FOXP3+调节性T细胞（Treg）与CD4+T、CD8+T在结直肠癌（colorectal carcinoma, CRC）组织中的分布及其与临床病理特征之间的关系。方法 收集42例CRC新鲜手术标本,应用冰冻切片、免疫组织化学SP法检测肿瘤组织和癌旁组织中FOXP3+、CD4+T和CD8+T阳性细胞数。结果 CRC患者肿瘤组织中FOXP3表达水平显著升高,与癌旁组织相比差异有统计学意义（P<0.01）;中低分化组Treg细胞数明显高于高分化组（P<0.01）;淋巴结转移组Treg细胞数明显高于无淋巴结转移组（P<0.05）;癌巢内CD4+、CD8+T细胞数及CD4+/CD8+值显著低于间质（P<0.01）;Ⅲ+Ⅳ期、淋巴结转移组癌巢内CD4+/CD8+比值显著低于Ⅰ+Ⅱ期及无淋巴结转移组（P<0.05）;CRC中Treg数量与癌巢内CD4+/CD8+比值显著负相关（r=-0.605, P<0.01）。结论 CRC的发生发展可能与其癌组织局部微环境中Treg数量变化相关,肿瘤局部Treg数量的增多与T淋巴细胞亚群比例失调可能成为肿瘤免疫逃逸的机制之一。     

Induction of potent CD4+ T cell-mediated antitumor responses by a helper HER-2/neu peptide linked to the Ii-Key moiety of the invariant chain

The Ii-Key fragment from the MHC class II-associated invariant chain (or Ii protein) has been shown to facilitate direct charging of MHC class II epitopes to the peptide binding groove. The purpose of the present study was to test the potential of a series of Ii-Key/HER-2/neu776-790 hybrid peptides to generate increased frequencies of peptide-specific CD4+ T cells over the native peptide in mice transgenic (Tg) for a chimeric human mouse class II molecule (DR4-IE) (H-2b) as well as their antitumor potency. Following in vivo priming, such hybrid peptides induced increased proliferation and frequencies of IFN-gamma producing CD4+ T cells in response to either syngeneic dendritic cells pulsed with native peptide, or HLA-DR4+ human tumor cell lines expressing HER-2/neu. Hybrid peptides were more stable in an off-rate kinetics assay compared to the native peptide. In addition, antigen-specific CD4+ T cells from hybrid peptide immunized DR4-IE Tg mice synergized with HER-2/neu(435-443)-specific CD8+ T cells from HLA-A2.1 Tg HHD (H-2b) mice in producing antitumor immunity into SCID mice xenografted with the HER-2/neu+, HLA-A2.1+ and HLA-DR4+ FM3 human melanoma cell line. High proportions of these adoptively transferred HER-2/neu peptide-specific CD4+ and CD8+ T cells infiltrated FM3-induced tumors (tumor infiltrating lymphocytes; TIL) in SCID mice. CD8+ TIL exhibited long-lasting antitumor activity when cotransferred with CD4+ TIL, inducing regression of FM3 tumors in a group of untreated, tumor-bearing SCID mice, following adoptive transfer. Our data show that Ii-Key modified HER-2/neu776-790 hybrid peptides are sufficiently potent to provide antigen-specific CD4+ TH cells with therapeutic antitumor activity.     

Tumor-specific CD4+ T cells from a patient with renal cell carcinoma recognize diverse shared antigens

Murine models for immune-mediated tumor regression have defined an essential role for CD4+ T helper (Th) cells, but the contribution of these cells to antitumoral immune responses in humans remains poorly defined. Here, we investigated the Th cell response against the autologous tumor in a patient with metastasized renal cell carcinoma (RCC) exhibiting objective clinical response to immunotherapy. Peripheral blood T cells of the patient were repeatedly stimulated in vitro using either autologous IFNgamma-treated whole tumor cells or Epstein-Barr virus-immortalized B cells (EBV-B) pulsed with tumor cell lysate. CD4+ T-cell clones recognizing autologous tumor cells but not EBV-B cells were efficiently reactivated and expanded with both types of stimulator cells, establishing the latter as potentially useful for isolating CD4+ T cells reactive against MHC class II-negative tumors. Two T-cell clones from both stimulation protocol were further characterized. The restricting MHC class II molecules were defined by using allogeneic EBV-B cells pulsed with tumor lysate, and the expression pattern of the antigens was examined by analyzing lysates from normal kidney cells, allogeneic RCCs as well as tumors of different histologic origin. Furthermore, the subcellular localization of the antigens recognized by the T-cell clones was examined by fractionating the tumor lysate, and the Th phenotype was determined by assessing the cytokines released after T cell activation. These experiments show that a dual Th1/Th2, MHC class II-restricted T-helper-cell response against diverse shared tumor antigens has been elicited in this patient.     

117例肝癌患者外周血调节T细胞水平及其临床意义

背景与目的:CD4 CD25 T细胞又称为调节性T细胞(Treg),是一群具有免疫抑制功能的T细胞亚群.近来的研究表明Treg能够显著地抑制免疫反应,导致肿瘤细胞的免疫耐受.然而,Treg在肝癌临床中的意义目前尚未阐明.本研究旨在探讨Treg水平与肝癌临床病理特征及预后的关系.方法:采用前瞻性研究设计,117例原发性肝癌患者于1999年1月至2000年12月住院且首次行肝癌根治性手术切除,术前用流式细胞仪检测其外周血Treg水平.术后随访至2005年12月30日.分析外周血Treg水平与肝癌临床病理特征及生存率的关系.40例正常对照来自健康献血者.结果:肝癌患者外周血中Treg的水平为(12.54±4.69)%,正常对照组为(8.81±1.98)%,两者比较差异有显著统计学意义(P＜0.01).全组1、3、5年生存率分别为83.8%、49.6%、35.9%.在单个病灶的患者中,Treg水平与肿瘤的边界有关,肿瘤边界不清楚者Treg水平显著增高;外周血Treg水平与其它临床病理特征无关.外周血Treg水平增高的患者预后差.结论:肝癌患者外周血Treg比例升高是影响预后的独立危险因素.     

肿瘤患者CD4+CD25+调节性T细胞流式细胞术分析

目的:分析比较肿瘤患者和健康人外周血CD4+CD25+调节性T细胞的特点,为肿瘤免疫学研究及治疗探索新方法.方法:收集并分离30例肿瘤患者和32例健康人的外周血单个核细胞(PBMCs),用荧光标记的抗人CD4及抗人CD25单抗标记肿瘤患者和健康人PBMCs细胞,FCM检测CD4+CD25+Treg细胞,分析CD4+CD25+Treg细胞在肿瘤患者和健康人中的差别.结果:肿瘤患者的CD4+CD25+Treg细胞百分数明显高于健康人(年龄<55者62.4 vs 40.4;年龄≥55者53.1 vs 31.0,P<0.05).结论:肿瘤患者的CD4+CD25+Treg细胞高于健康对照,为肿瘤免疫治疗提供新策略,通过删除CD4+CD25+Treg细胞,有可能增强抗瘤免疫反应.     

CIK细胞中CD4+T细胞亚群抗肿瘤免疫活性

目的：观察CIK细胞中CD4+T细胞亚群抗肿瘤免疫活性。方法：体外大规模扩增CIK细胞，利用磁珠分离系统富集纯化CIK细胞中的CD4+T细胞亚群。采用胞内染色法分析其中Th1/Th2的比例变化； LDH法和荧光染色法比较4 h和20 h其对raji细胞的杀伤率和raji凋亡。结果：经磁珠分离法富集的CD4+CIK细胞纯度高达96%， 其中Th1/Th2的分布较PBMC有显著的改变：Th1亚群、Th0亚群明显升高，Th2亚群无显著变化。CD4+CIK细胞虽然不能在4 h之内溶解raji细胞，但可在20 h时产生同CD4-CIK细胞同样强大的杀伤活性，荧光染色可见其在4 h之内诱导raji出现早期凋亡的迹象。结论：本研究提示CD4+CIK细胞具有明显的“Th1优势”可以调节宿主免疫细胞活性；同时CD4+CIK细胞可通过诱导肿瘤细胞凋亡实现对肿瘤的抑制和杀伤。     

CD4+CD25+调节性T细胞与大肠癌的关系

近来CD4 CD25 调节性T细胞对肿瘤免疫调节的抑制作用正受到越来越多的重视,许多恶性肿瘤患者外周血都存在CD4 CD25 调节性T细胞比例上调,机体抗肿瘤免疫力下降.大肠癌的发病率正逐年上升,其发病分子机制已为熟知,免疫机制研究不多,国内尚未见大肠癌与该类细胞关系的报道,现对CD4 CD25 调节性T细胞在大肠癌的发生、发展、治疗中的研究综述如下.     

CD4^＋CD25^＋调节性T细胞与肿瘤的相关性研究

通过了解CD4^＋CD25^＋调节性T细胞（CD4^＋CD25^＋Treg）表面分子的特性和CD4^＋CD25^＋Treg在外周血和组织中的表达,认识CD4^＋CD25^＋Treg在肿瘤免疫调节中的作用,探索其作用的分子机制。     

Proportion of CD4+CD25+ regulatory T cell is increased in the patients with ovarian carcinoma

Objective: To study the frequency of the CD4⁺CD25⁺ regulatory T cells (Tregs) in the patients with ovarian carcinoma and its possible mechanism. Methods: The percentages of CD4⁺CD25⁺ Tregs in the peripheral blood lymphocytes (PBLs), tumor infiltrating lymphocytes (TILs) and tumor associated lymphocytes (TALs) from 13 patients with ovarian carcinoma and in the PBLs from 14 healthy women were determined by flow cytometry. The expression of CD69 on CD4⁺PBLs from the patients was detected. PBLs from healthy women were cultured in complete RPMI 1640 containing the supernatant from SKOV3 cell line with or without PHA (phytohemagglutinin) stimulation for 72 hours, then the percentage of CD4⁺CD25⁺ T cells was detected. Results: CD4⁺CD25⁺ Tregs in the PBLs from patients with ovarian carcinoma were significantly increased compared with those from the control. The percentage of CD4⁺CD25⁺ Tregs in TILs was higher than that in PBLs and TALs from the patients, but not significantly. The expression of CD69 on CD4⁺PBLs from the patients was negative. The percentages of CD4⁺CD25⁺ T cells in PBLs cultured with SKOV3 supernatant elevated significantly compared with those without supernatant whether PHA was added or not (P = 0.001 and 0.001, respectively). Conclusion: There is an increasing of the proportion of CD4⁺CD25⁺ Tregs in PBLs, TILs and TALs of the patients with ovarian carcinoma, which probably results from up-regulation of soluble factor secreted by ovarian carcinoma cells.     

CD3+CD56+NKT细胞及CD3-CD56+NK细胞在恶性肿瘤患者的临床意义研究

背景与目的细胞毒性淋巴细胞在抗肿瘤免疫效应中发挥着重要作用,CD3 CD56 NKT细胞作为一类新的具有细胞毒性的效应细胞,目前关于其抗肿瘤意义的探讨主要集中于血液系统恶性疾病,而在实体肿瘤中的应用和临床价值研究尚少。本研究旨在初步探讨抗肿瘤细胞CD3 CD56 NKT细胞及CD3-CD56 NK细胞在恶性肿瘤患者外周血的表达状态及其临床意义。方法采用流式细胞术分析118例恶性肿瘤患者(55例肺癌患者和63例乳腺癌患者)及46例健康对照组外周血中的T细胞亚群及CD3 CD56 NKT细胞、CD3-CD56 NK细胞表达。结果恶性肿瘤患者组CD3 CD8 T细胞、CD3 CD56 NKT细胞以及CD3-CD56 NK细胞表达率均明显高于健康对照组(P<0.01)。肺癌患者中以CD3 CD8 T细胞和CD3 CD56 NKT细胞明显增加为主;乳腺癌患者中以CD3 CD56 NKT细胞和CD3-CD56 NK细胞明显增加为主。结论CD3 CD56 NKT细胞在肺癌和乳腺癌患者的抗肿瘤效应中占据重要地位,而CD3 CD8 CTL和CD3-CD56 NK细胞在不同类型肿瘤患者中具有不同的重要性。