Association of Graves’ disease and Graves’ ophthalmopathy with the polymorphisms in promoter and exon 1 of cytotoxic T lymphocyte associated antigen-4 gene

Objective: To investigate the association of Graves’ disease and Graves’ ophthalmopathy with the C/T transition polymorphism at position –318 of promoter and the A/G transition polymorphism at position 49 of exon 1 within cytotoxic T lymphocyte associated antigen-4 (CTLA-4) gene. Methods: Thirty-three patients with ophthalmopathy of Graves’ disease, fifty-six Graves’ patients without ophthalmopathy and sixty normal subjects as control were involved in the present case-control study. The polymorphisms were evaluated by polymerase chain reaction fragment length polymorphism (PCR-RFLP). Com-parisons were made of gene frequencies and allele frequencies between the groups. Results: The gene frequencies of CT and allele frequencies of T were much higher in Graves’ patients with ophthalmopathy than that in the group without ophthalmopathy (P=0.020, P=0.019). The gene frequencies of GG and allele frequencies of G in patients with Graves’ disease were significantly increased as compared with control group (P=0.008, P=0.007). The data suggest that smokers with Graves’ disease seemed to be more predisposed to ophthalmopathy than non-smokers (P=0.018). Conclusion: Our results suggest that an allele of T at position –318 of promoter is associated with genetic susceptibility to Graves’ ophthalmopathy while an allele of G at position 49 of exon 1 is associated with genetic susceptibility to Graves’ disease instead. Smoking is believed to be a major risk factor for ophthalmo-pathy.

Reconceptualization of immune checkpoint inhibitor-associated gastritis

In recent years,with the extensive application of immunotherapy in clinical practice,it has achieved encouraging therapeutic effects.While enhancing clinical efficacy,however,it can also cause autoimmune damage,triggering immunerelated adverse events(irAEs).Reports of immunotherapy-induced gastritis have been increasing annually,but due to its atypical clinical symptoms,early diagnosis poses a certain challenge.Furthermore,it can lead to severe complications such as gastric bleeding,elevating the risk of adverse outcomes for solid tumor patients if immunotherapy is interrupted.Therefore,gaining a thorough understanding of the pathogenesis,clinical manifestations,diagnostic criteria,and treatment of immune-related gastritis is of utmost importance for early identification,diagnosis,and treatment.Additionally,the treatment of immune-related gastritis should be personalized according to the specific condition of each patient.For patients with grade 2-3 irAEs,restarting immune checkpoint inhibitors(ICIs)therapy may be considered when symptoms subside to grade 0-1.When restarting ICIs therapy,it is often recommended to use different types of ICIs.For grade 4 irAEs,permanent discontinuation of the medication is necessary.

外周血sCTLA-4作为晚期非小细胞肺癌患者的预后因子

目的：通过检测晚期非小细胞肺癌（non-small-cell lung cancer，NSCLC）患者外周血可溶性细胞毒性T淋巴细胞相关抗原4（soluble cytotoxic T lymphocyte associated antigen- 4，sCTLA-4）的表达，探讨其与晚期NSCLC患者生存期的关系。方法：采集2010年8月至2013年6月上海中医药大学附属龙华医院肿瘤科经病理证实的58例晚期NSCLC患者和30例正常人的外周血，运用ELISA法检测血中sCTLA-4含量，通过电话随访或上海市疾控中心获得患者生存期数据，分析sCTLA-4表达与NSCLC生存期的关系。结果：NSCLC患者外周血sCTLA-4表达率高于正常人（70.7% vs 6.7%， χ2=32.44，P〈0.01）,外周血sCTLA-4增高的患者中位生存期（MST）较短（41.63个月vs 31.57个月， χ2=7.765，P〈0.01），死亡风险高于其他患者（RR=305， χ2=8.01, P〈0.01）。结论：NSCLC患者外周血中sCTLA-4高表达，sCTLA-4可能成为晚期NSCLC患者的预后因子之一。

突眼性甲状腺疾病病人外周血T淋巴细胞IL-2s、CTLA-4表达的研究

[目的]探讨抗甲状腺药物（ATD）治疗前后白细胞介素2（IL-2）调节突眼性甲状腺疾病（GD）病人外周血可溶性细胞毒性T淋巴细胞相关抗原4（sCTLA-4）表达的变化，为进一步研究GD病人的治疗对机体免疫功能的影响提供依据。[方法]2006年9月，对2000-2005年在山东省千佛山医院门诊及住院的72例GD患者和健康对照20人进行外周血淋巴细胞IL-2、sCTLA-4、FT3、FT4、TSH的检测。[结果]GD患者中经过药物治疗的甲状腺功能缓解组外周血FT3、FT4、sCTLA-4水平均低于未治疗的甲亢组，TSH、IL-2平均水平高于甲亢组（P〈0．05）；缓解组FT3、FT4、TSH、IL-2、sCTLA-4水平均接近对照组（P〉0．05）；甲亢组FT3、FT4、sCTLA-4水平均高于对照组，TSH、IL-2水平均低于对照组（P〈0．01）。[结论]抗甲状腺药物治疗可调节机体细胞因子的分泌水平，改善机体的免疫功能。

CD28/CTLA-4/B7 and CD40/CD40L costimulation and activation of regulatory T cells

Costimulatory signals are crucial for T cell activation. Attempts to block costimulatory pathways have been effective in preventing unwanted immune reactions. In particular, blocking the CD28/cytotoxic T lymphocyte antigen(CTLA)-4/B7 interaction(using CTLA-4Ig) and the CD40/CD40 L interaction(using anti-CD40 L antibodies) prevents T cell mediated autoimmune diseases, transplant rejection and graft vs host disease in experimental models. Moreover, CTLA-4Ig is in clinical use to treat rheumatoid arthritis(abatacept) and to prevent rejection of renal transplants(belatacept). Under certain experimental conditions, this treatment can even result in tolerance. Surprisingly, the underlying mechanisms of immune modulation are still not completely understood. We here discuss the evidence that costimulation blockade differentially affects effector T cells(Teff) and regulatory T cells(Treg). The latter are required to control inappropriate and unwanted immune responses, and their activity often contributes to tolerance induction and maintenance. Unfortunately, our knowledge on the costimulatory requirements of Treg cells is very limited. We therefore summarize the current understanding ofthe costimulatory requirements of Treg cells, and elaborate on the effect of anti-CD40 L antibody and CTLA-4Ig treatment on Treg cell activity. In this context, we point out that the outcome of a treatment aiming at blocking the CD28/CTLA-4/B7 costimulatory interaction can vary with dosing, timing and underlying immunopathology.

晚期卵巢癌患者外周血sPD-L1、sCTLA-4表达水平及临床意义

目的探讨晚期卵巢癌患者外周血可溶性程序性死亡配体-1(sPD-L1)、可溶性细胞毒T淋巴细胞相关抗原4(sCTLA-4)的表达水平及其临床意义。方法选取2017年1月至2018年12月我院收治的102例晚期卵巢癌患者作为观察组,100例卵巢良性肿瘤患者作为对照组。检测两组外周血sPD-L1、sCTLA-4的表达水平并比较其差异;分析sPD-L1与sCTLA-4水平的相关性;分析晚期卵巢癌患者外周血sPD-L1、sCTLA-4的表达水平与临床病理特征及预后的关系;以晚期卵巢癌患者的sPD-L1、sCTLA-4水平均数为临界值划分高、低表达亚组,比较其预后差异。结果观察组患者的外周血sPD-L1、sCTLA-4表达水平分别为(14.82±4.74)ng/ml、(17.95±5.68)ng/ml,高于对照组的(7.78±2.26)ng/ml、(9.13±2.96)ng/ml,差异均有统计学意义(P<0.05)。晚期卵巢癌患者的外周血sPD-L1与sCTLA-4水平呈正相关(r=0.634,P<0.001)。sPD-L1、sCTLA-4表达水平与晚期卵巢癌的组织分化程度、临床分期及腹水量有关(P均<0.05)。2年随访期内,共有31例患者死亡。其中sPD-L1高表达组的2年生存率为59.18%,明显低于sPD-L1低表达组的79.25%(P=0.028);sCTLA-4高表达组的2年生存率为55.56%,明显低于sCTLA-4低表达组的85.42%(P=0.001)。结论晚期卵巢癌患者外周血sPD-L1和sCTLA-4均呈高表达,且与患者预后密切相关。

系统性红斑狼疮患儿血清sCTLA4、TNF-α水平表达及其临床意义

目的探讨系统性红斑狼疮(SLE)患儿血清可溶性细胞毒性T淋巴细胞相关抗原-4(sCTLA4)、肿瘤坏死因子-α(TNF-α)水平表达及其临床意义。方法我院就诊的40例SLE患儿(SLE组),根据SLE疾病活动指数(SLEDAI)评分分为活动期组(SLEDAI评分≥10分,22例)和静止期组(SLEDAI评分<10分,18例),另选择同期同年龄组40例健康儿童(对照组),检测各组血清sCTLA4、TNF-α水平。结果 SLE组血清sCTLA4、TNF-α水平高于对照组(P<0. 05);活动期组血清sCTLA4、TNF-α水平高于静止期组(P<0. 05);SLE患儿血清sCTLA4、TNF-α水平与SLEDAI评分显著正相关(P<0. 05)。结论SLE患儿血清sCTLA4、TNF-α水平异常升高,且随病情严重程度加重而持续升高,共同参与了SLE的发病过程。

外周血sCTLA-4、sPD-L1及Ki-67在晚期卵巢癌中表达水平及与预后的相关性分析

目的探讨晚期卵巢癌(Ⅲc期和Ⅳ期)患者外周血可溶性细胞毒性T淋巴细胞相关抗原4(sCTLA-4)、可溶性程序性死亡配体-1(sPD-L1)、Ki-67的表达水平以及与其预后的相关性分析。方法采用前瞻性研究,选取2019年1月至2020年1月于空军军医大学第一附属医院就诊的88例晚期卵巢癌患者纳入观察组,92例卵巢良性肿瘤患者纳入对照组。检测并比较两组患者外周血sCTLA-4、sPD-L1、Ki-67的表达水平,分析外周血sCTLA-4、sPD-L1、Ki-67表达水平与晚期卵巢癌临床病理特征及患者预后的关系;根据外周血sCTLA-4、sPD-L1水平均数高低及Ki-67阳性细胞率大小将观察组分为高表达组与低表达组,随访2年时间,比较两组患者的预后质量。结果观察组患者外周血sCTLA-4、sPD-L1表达水平为(17.64±5.28)、(14.79±4.36)ng/mL,均明显高于对照组[(9.84±2.68)、(8.16±2.26)ng/mL],差异均有统计学意义(P<0.05)。观察组患者Ki-67表达水平为76.14%,明显高于对照组(30.43%),差异有统计学意义(P<0.05)。外周血sCTLA-4、sPD-L1及Ki-67表达水平与观察组卵巢癌患者的分化程度、临床分期、腹水量有关联(P<0.05),与患者的年龄、卵巢癌病理类型、糖链多肽抗原125(CA125)水平无关联(P>0.05)。对观察组患者进行1~2年的随访,共有死亡病例28例。其中sCTLA-4、sPD-L1及Ki-67表达水平的各低表达组的生存率均显著明显高于其高表达组,差异均有统计学意义(P<0.05)。结论外周血sCTLA-4、sPD-L1及Ki-67在晚期卵巢癌中呈高表达水平,与晚期卵巢癌患者的预后生存质量有密切联系。

可溶性细胞毒性T细胞相关抗原-4在川崎病中的表达及意义

目的:研究川崎病(KD)患儿血浆可溶性细胞毒性T细胞相关抗原-4(sCTLA-4)的表达及其与冠状动脉损害的相关性。方法:KD患儿40例,按病程分为急性期组(KDA组)40例和亚急性期组(KDS组)22例;KDA组按有无冠状动脉损害分为冠状动脉损害组(CAL组)11例和非冠状动脉损害组(NCAL组)29例;KDA组按治疗效果分为静脉注射用免疫球蛋白(IVIG)敏感组33例及IVIG不敏感组7例。呼吸道感染所致发热患儿18例作为发热对照组(F组)。同期健康体检儿童及斜疝、隐睾择期手术患儿18例为对照组(C组)。记录相关临床资料、临床实验室检验结果,采用酶联免疫吸附试验(ELISA)检测血浆sCTLA-4浓度。结果:(1)KDA组血浆sCTLA-4水平6.50(3.44)ng/mL,分别高于KDS组4.44(3.71)ng/mL、F组5.19(2.30)ng/mL及C组2.76(2.13)ng/mL,差异均具有统计学意义(H=34.231,P<0.05)。(2)CAL组血浆sCTLA-4水平9.04(3.70)ng/mL,高于NCAL组5.99(1.75)ng/mL,差异有统计学意义(Z=2.881,P<0.01)。(3)IVIG敏感组与不敏感组血浆sCTLA-4水平的差异无统计学意义(Z=0.445,P>0.05)。(4)血浆sCTLA-4与CAL呈正相关(r=0.461,P<0.01)。(5)受试者工作特征曲线(ROC曲线)分析显示,sCTLA-4预测KD冠脉损害的曲线下面积(AUC)为0.798(P<0.05),取临界值6.75 ng/mL,其预测KD冠脉损害的灵敏度为0.909,特异度为0.759。结论:在KD急性期血浆sCTLA-4水平升高,存在冠脉损害患儿sCTLA-4水平高于无冠脉损害患儿,提示sCTLA-4可能参与KD以及KD冠脉损害的发生发展。

可溶性细胞毒T淋巴细胞相关抗原-4联合癌胚抗原、糖类抗原19-9检测在诊断结直肠癌中的意义

目的探讨可溶性细胞毒T淋巴细胞相关抗原-4(s CTLA-4)、癌胚抗原(CEA)及糖类抗原19-9(CA19-9)联合诊断法对结直肠癌患者的临床诊断意义。方法选取80例结直肠癌患者作为实验组,选取40例健康人作为对照组,抽取其静脉血,测量s CTLA-4、CEA及CA19-9值。对比观察3种诊断方法和联合诊断法在敏感性、特异性、准确性、阳性预测值及阴性预测值方面的差异。结果联合诊断法的敏感性、准确性和阴性预测值明显高于单独任何一种诊断方法(P<0.05)。在特异性和阳性预测值方面与其他诊断方法差异无统计学意义(P>0.05)。结论 s CTLA-4、CEA及CA19-9联合诊断法在敏感性、准确性和阴性预测值方面有明显的优势,有很好的临床应用价值。

Emergence of immunotherapy as a novel way to treat hepatocellular carcinoma

Tumor immunity proceeds through multiple processes, which consist of antigen presentation by antigen presenting cells(APCs) to educate effector cells and destruction by the effector cytotoxic cells. However, tumor immunity is frequently repressed at tumor sites. Malignantly transformed cells rarely survive the attack by the immune system, but cells that do survive change their phenotypes to reduce their immunogenicity. The resultant cells evade the attack by the immune system and form clinically discernible tumors. Tumor microenvironments simultaneously contain a wide variety of immune suppressive molecules and cells to dampen tumor immunity. Moreover, the liver microenvironment exhibits immune tolerance to reduce aberrant immune responses to massively-exposed antigens via the portal vein, and immune dysfunction is frequently associated with liver cirrhosis, which is widespread in hepatocellular carcinoma(HCC) patients. Immune therapy aims to reduce tumor burden, but it is also expected to prevent non-cancerous liver lesions from progressing to HCC, because HCC develops or recurs from noncancerous liver lesions with chronic inflammatory states and/or cirrhosis and these lesions cannot be cured and/or eradicated by local and/or systemic therapies. Nevertheless, cancer immune therapy should augment specific tumor immunity by using two distinct measures: enhancing the effector cell functions such as antigen presentation capacity of APCs and tumor cell killing capacity of cytotoxic cells, and reactivating the immune system in immune-suppressive tumor microenvironments. Here, we will summarize the current status and discuss the future perspective on immune therapy for HCC.

Specific CD8^+ T cell response immunotherapy for hepatocellular carcinoma and viral hepatitis

Hepatocellular carcinoma (HCC), chronic hepatitis B (CHB) and chronic hepatitis C (CHC) are characterized by exhaustion of the specific CD8+ T cell response. This process involves enhancement of negative co-stimulatory molecules, such as programmed cell death protein-1 (PD-1), cytotoxic T-lymphocyte antigen-4 (CTLA-4), 2B4, Tim-3, CD160 and LAG-3, which is linked to intrahepatic overexpression of some of the cognate ligands, such as PD-L1, on antigen presenting cells and thereby favouring a tolerogenic environment. Therapies that disrupt these negative signalling mechanisms represent promising therapeutic tools with the potential to restore reactivity of the specific CD8+ T cell response. In this review we discuss the impressive in vitro and in vivo results that have been recently achieved in HCC, CHB and CHC by blocking these negative receptors with monoclonal antibodies against these immune checkpoint modulators. The article mainly focuses on the role of CTLA-4 and PD-1 blocking monoclonal antibodies, the first ones to have reached clinical practice. The humanized monoclonal antibodies against CTLA-4 (tremelimumab and ipilimumab) and PD-1 (nivolumab and pembrolizumab) have yielded good results in testing of HCC and chronic viral hepatitis patients. Trelimumab, in particular, has shown a significant increase in the time to progression in HCC, while nivolumab has shown a remarkable effect on hepatitis C viral load reduction. The research on the role of ipilimumab, nivolumab and pembrolizumab on HCC is currently underway.

Progress in immunotherapy for small cell lung cancer

Small-cell lung cancer(SCLC)is a special type of lung cancer that belongs to highly aggressive neuroendocrine tumors.At present,radiotherapy and chemotherapy remain the mainstay of treatment for SCLC.Progress in targeted therapies for SCLC with driver mutations has been slow,and these therapies are still under investigation in preclinical or early-phase clinical trials,and research on antiangiogenic tyrosine kinase inhibitors(e.g.,anlotinib)has achieved some success.Immunotherapy is becoming an important treatment strategy for SCLC after radiotherapy and chemotherapy.In this article we review the recent advances in immunotherapy for SCLC.

Extremely high frequency of autoimmune-predisposing alleles in medieval specimens

The precise etiology and reasons for the increase in incidence of autoimmune disorders still remain unclear, and although both genetic and environmental factors have been proven to shape individual predisposition, it is not known which of the factors, if not both, is responsible for the boom observed during the last decades. In order to establish whether a higher frequency of autoimmune-predisposing alleles may explain this increase we took advantage of ancient DNA methodology to establish the genetic predisposition, conferred by cytotoxic T lymphocyte associated antigen-4 （CTLA4） ＋49A/G and human leukocyte antigens （HLA） DQBI^57, in population inhabiting Poland in the Middle Ages. After successful typing of 42 individuals from a 12th-14th＇s century archeological burial site, we found that frequencies of the predisposing alleles in the medieval population were higher than they are at present, suggesting thus that the recently observed incidence increase results most probably from factors of other than genetic nature.

Present and future of immune checkpoint blockade: Monotherapy to adjuvant approaches

Immune regulation of aggressive tumor growth is often outpaced by tumor up-regulation of ligands that inhibit effector immune responses through the activation of immune checkpoints. A few of such checkpoints include programmed death-1(PD-1), cytotoxic T lymphocyte associated antigen-4(CTLA-4), lymphocyte activation gene-3, T-cell immunoglobulin and mucin protein-3, Glucocorticoid-induced TNFR family-related receptor(GITR), and killer cell immunoglobulin like receptor. With the exception of GITR, after binding to their respective ligands these checkpoints induce down-modulation of immune responses to prevent autoimmunity. However, such immune mechanisms are co-opted by tumors to allow rapid tumor cell proliferation. Pre-clinical studies in antibody blockade of PD-1 and CTLA-4 have led to promising augmentation of effector immune responses in murine tumor models, and human antibodies against PD-1 and CTLA-4 alone or in combination have demonstrated tumor regression in clinical trials. The development of immune checkpoint blockade as a potential future immunotherapy has led to increasing interest in combining treatment modalities. Combination checkpoint blockade with chemotherapy and radiation therapy has shown synergistic effects in pre-clinical and clinical studies, and combination checkpoint blockade with bacterial vaccine vectors have produced increased effector immune responses in pre-clinical models. The future of immune checkpoint blockade may be as a powerful adjuvant alongside the current standard of care.

sCTLA-4、RAD51C蛋白对宫颈癌患者介入治疗术后复发的预测价值

目的分析可溶性细胞毒T淋巴细胞相关抗原4(sCTLA-4)、RAD51旁系同源基因C(RAD51C)蛋白对宫颈癌患者介入治疗术后复发的预测价值。方法选取2015年5月至2019年4月河南省人民医院宫颈癌患者107例为观察组,均经介入手术治疗,统计术后复发情况,另选取同期良性宫颈疾病患者107例为对照组。比较观察组、对照组及是否复发患者sCTLA-4、RAD51C蛋白表达,采用Logistic回归分析宫颈癌患者术后复发的影响因素,构建宫颈癌患者术后复发的列线图模型并采用校准曲线验证,绘制决策曲线分析sCTLA-4、RAD51C蛋白预测宫颈癌患者术后复发的价值,并统计不同sCTLA-4、RAD51C蛋白表达患者的复发率。结果观察组sCTLA-4水平、RAD51C蛋白高表达率高于对照组(P<0.05);高危型人乳头瘤病毒阳性、脉管浸润、间质浸润≥1/2、宫旁浸润、RAD51C蛋白高表达及sCTLA-4高水平是宫颈癌患者术后复发的独立危险因素(P<0.05);高危型人乳头瘤病毒、脉管浸润、间质浸润、宫旁浸润、RAD51C蛋白及sCTLA-4水平构建宫颈癌患者术后复发的列线图预测模型,一致性指数分别为0.610(95%CI为0.511~0.702)、0.616(95%CI为0.517~0.708)、0.640(95%CI为0.541~0.730)、0.609(95%CI为0.510~0.702)、0.728(95%CI为0.633~0.809)、0.817(95%CI为0.731~0.885),且校准曲线验证显示具有较高一致性,sCTLA-4、RAD51C蛋白联合检测的净受益率大于单独检测。结论宫颈癌患者sCTLA-4、RAD51C蛋白均呈高表达,且二者同时高表达表明宫颈癌患者术后复发风险较高,临床可通过检测sCTLA-4、RAD51C蛋白表达情况筛选高复发风险患者并及早进行干预,以降低复发率。

布鲁氏菌病患者外周血CTLA-4和CD14表达及其相关性分析

目的探讨外周血细胞毒性T淋巴细胞相关抗原-4(CTLA-4)、可溶性CD14(sCD14)和膜结合性CD14(mCD14)在布鲁氏菌病患者中表达水平及其相关性。方法选取2019-06-01-2021-06-01郑州市第六人民医院收治的116例布鲁氏菌患者为研究对象,其中急性布鲁氏菌患者63例(急性布鲁病组),慢性布鲁氏菌患者53例(慢性布鲁病组)。选取同期同院116例体检健康者为对照组。酶联免疫吸附法检测血清中CTLA-4、sCD14、肿瘤坏死因子-α(TNF-α)、白细胞介素(IL)-6、IL-2水平,采用流式细胞术检测外周血单个细胞核mCD14表达水平。采用Pearson法分析血清CTLA-4、sCD14水平与TNF-α、IL-6、IL-2的相关性。多因素Logistic回归分析布鲁氏菌病的影响因素。结果与对照组sCD14[(943.47±124.28)ng/mL]、CTLA-4[(41.27±8.17)pg/mL]、mCD14[(7.25±1.63)%]相比,慢性布鲁病组外周血血清sCD14水平[(1568.17±309.52)ng/mL]、CTLA-4水平[(76.28±14.39)pg/mL]、外周血单个核细胞中mCD14[(11.72±3.08)%]表达较高,均P<0.05;与慢性布鲁病组相比,急性布鲁病组血清sCD14水平[(2075.48±325.16)ng/mL]、CTLA-4水平[(126.73±28.44)pg/mL]、外周血单个核细胞中mCD14[(27.49±6.05)%]表达较高,均P<0.05。与慢性布鲁病组TNF-α[(22.94±5.02)pg/mL]、IL-6[(23.84±5.61)pg/mL]、IL-2[(2.94±0.62)pg/mL]相比,急性布鲁病组血清TNF-α水平[(30.28±5.86)pg/mL,t=7.169,P<0.001]、IL-6水平[(58.73±6.68)pg/mL,t=30.120,P<0.001]较高,血清IL-2水平[(2.32±0.51)pg/mL,t=5.912,P<0.001]降低。Pearson法分析结果显示,CTLA-4、sCD14与TNF-α、IL-6呈正相关(P<0.001),与IL-2呈负相关(P<0.001)。Logistic回归分析结果显示,CTLA-4(OR=1.941,95%CI为1.251~3.011,P=0.004)、TNF-α(OR=1.914,95%CI为1.053~3.479,P=0.033)、IL-6(OR=2.111,95%CI为1.152~3.868,P=0.015)、sCD14(OR=2.229,95%CI为1.454~3.417,P<0.001)是布鲁氏菌病的独立危险因素,IL-2(OR=0.502,95%CI为0.315~0.799,P=0.004)是布鲁氏菌病的保护因素。结论外周血CD14及血清CTLA-4在布鲁氏菌病患者中高表达,CTLA-4、CD14共同参与布鲁氏菌对宿主的免疫调控作用。

初发1型糖尿病患儿外周血单个核细胞FOXP3和CTLA-4表达的研究

目的：研究初发1型糖尿病患儿外周血叉状头转录因子（ FOXP3）和细胞毒性T细胞相关抗原-4（CTLA-4）表达水平,探讨它们在1型糖尿病发病中的作用。方法选取50例初发1型糖尿病患儿和30例健康儿童,采用real-time PCR法研究FOXP3和CTLA-4 mRNA表达；ELISA方法检测血清中可溶性FOXP3（ sFOXP3）和CTLA-4（ sCTLA-4）蛋白水平；分别应用免疫印记法、高效液相离子层析法和电化学发光法测量糖尿病抗体、HbA1C及C肽。结果1型糖尿病患儿FOXP3 mRNA及蛋白表达低于对照组[0.95±0.48 vs.2.11±0.79,（6.27±1.49） ng/ml vs.（9.02±2.37） ng/ml,均P〈0.01],而CTLA-4 mRNA及蛋白表达高于对照组[2.43±0.83 vs.1.94±0.84,（77.88±22.34） ng/ml vs.（65.97±12.11） ng/ml,P〈0.01]；1型糖尿病患儿FOXP3和CTLA-4基因与蛋白表达均呈正相关（r＝0.758、0.396,均P〈0.05）；FOXP3与CTLA-4蛋白表达具有相关性（r＝－0.624,P〈0.05）。结论初发1型糖尿病患儿外周血FOXP3和CTLA-4的基因及蛋白表达异常,FOXP3调控CTLA-4在调节性T 细胞的表达,提示免疫机制参与1型糖尿病的发生。

血清可溶性细胞毒T淋巴细胞相关抗原-4在胃癌早期诊断中价值

目的探讨胃癌患者可溶性细胞毒T淋巴细胞相关抗原-4(soluble cytotoxic T lymphocyte associated antigen-4,sCTLA-4)表达情况及其对胃癌的诊断价值。方法胃癌患者63例(胃癌组)、慢性萎缩性胃炎患者15例(胃炎组)、胃溃疡患者12例(胃溃疡组)、体检健康者24例(对照组),采用ELISA法检测4组血清sCTLA-4水平,电化学发光法检测癌胚抗原(carcino-embryonic antigen,CEA)和糖类抗原72-4(carbohydrate antigen 72-4,CA72-4)水平,ROC曲线评价sCTLA-4单独及与CEA,CA72-4联合检测在胃癌诊断中的应用价值。结果胃癌组血清sCTLA-4,CEA及CA72-4水平明显高于胃炎组、胃溃疡组及对照组(P<0.05),胃炎组与胃溃疡组血清sCTLA-4水平明显高于对照组(P<0.05),胃炎组与胃溃疡组血清sCTLA-4水平比较差异无统计学意义(P>0.05),胃炎组、胃溃疡组与对照组血清CEA及CA72-4水平比较差异均无统计学意义(P>0.05);胃癌组血清sCTLA-4水平在临床分期与淋巴结转移上差异有统计学意义(P<0.05);sCTLA-4诊断胃癌的AUC为0.618,临界值为8.31ng/mL,灵敏度和特异度分别为72.4%,79.3%,与CEA及CA72-4联合检测诊断胃癌的AUC为0.835,灵敏度和特异度分别为88.9%,94.2%。结论胃癌患者sCTLA-4表达明显升高,其对胃癌早期诊断有重要价值。

Advances in targeted therapy and immunotherapy for esophageal cancer

Esophageal cancer(EC)is one of the most common aggressive malignant tumors in the digestive system with a severe epidemiological situation and poor prognosis.The early diagnostic rate of EC is low,and most EC patients are diagnosed at an advanced stage.Multiple multimodality treatments have gradually evolved into the main treatment for advanced EC,including surgery,chemotherapy,radiotherapy,targeted therapy,and immunotherapy.And the emergence of targeted therapy and immunotherapy has greatly improved the survival of EC patients.This review highlights the latest advances in targeted therapy and immunotherapy for EC,discusses the efficacy and safety of relevant drugs,summarizes related important clinical trials,and tries to provide references for therapeutic strategy of EC.