复发性流产孕激素水平与免疫应答类型的相关性研究

孕龄妇女与同一性伴侣连续发生3次或3次以上自然流产,称复发性流产（recurrent spontaneousabortion,RSA）,是妇产科常见的并发症之一。RSA病因复杂,现在认为涉及生殖道解剖畸形、染色体异常、内分泌失调、免疫因素、感染性疾病、血型不合及环境和饮食等多种因素。近年来越来越多的国内外学者认为免疫因素与RSA密切相关,

基因枪接种乙型肝炎表面抗原促进DNA疫苗诱生的免疫应答转换

目的为了克服基因枪接种乙型肝炎表面抗原(HBsAg)DNA疫苗诱生的免疫应答以Th2为主的缺点,在基因枪接种质粒HBsAg DNA疫苗的同时共导入或共表达乙型肝炎病毒壳(HBV core)基因作为佐剂,以促进其所诱生的HBsAg特异性的Th2型免疫应答向Tn1型转换。方法构建可单独或共同表达HBsAg或核心抗原(HBcAg)的DNA免疫用载体pIRKS／core、pIRES／C149、pIRES／S、pIRES／S／Core和pIRES／S／C149,并在真核细胞进行表达验证。对BALB／c雌鼠进行免疫并检测小鼠免疫后的特异性体液免疫和细胞免疫指标。结果共导入或共表达HBV core基因能增强基因枪接种HBsAg DNA疫苗诱生的Th1型免疫应答水平,包括HBsAg特异的IgG2a应答、CTL活性、IFN-γ产生能力等。结论以HBV core基因为佐剂能促进基因枪接种HBsAg DNA疫苗诱生的Th2型免疫应答向Th1型免疫应答转换。

日本血吸虫童虫细胞免疫小鼠抗血吸虫病的免疫保护性研究

为确定用日本血吸虫(Schistosoma japonicum,S.j)童虫细胞免疫小鼠抗血吸虫病的免疫保护性效应和分析与之可能的相关因素,本研究进行了两个独立重复的免疫实验.经皮下3次免疫后,实验1在无佐剂的情况下,与磷酸盐绥冲液(PBS)对照组比,S.j童虫原代细胞(primary juvenile worm cells,pJCs)诱导小鼠产生了明显的减虫率(平均54.3%)、每克肝卵(liver eggs per gram,LEPG)减少率(平均59.8%)和肝卵肉芽肿面积减少率(平均66.5%)(P<0.01),均明显高于童虫原代细胞碎片(fractions of juvenile worm cells,JCFs)或童虫虫体碎片(fractions of juvenile worms,JWFs)免疫组相应的减少率(P<0.05),而虫体的非细胞成分(non-cell components of worms,WNCs)免疫组无明显保护作用.实验2中,与PBS对照组比,培养的童虫细胞(cultured juvenile worm cells,cJCs)也诱导了明显的平均58.4%的减虫率、68.1%的LEPG减少率(P<0.01),而培养的成虫细胞(cultured adult worms cells,cACs)组的虫荷(P<0.05)和卵荷(P<0.01)明显高于cJCs组.实验2的免疫学分析显示,cJCs诱导小鼠产生Th1型为主的Th1/Th2混合类型的免疫应答,而cACs则诱导Th2型偏向的应答类型.这些资料显示,用S.j原代和培养的童虫细胞都可诱导小鼠产生明显的抗血吸虫高保护效应,可能与免疫原的物理性状、虫期特异性及诱导的免疫类型有关,提示用S.j童虫全细胞免疫小鼠是一种有希望的诱导抗血吸虫病保护性免疫的方法.

New progress in active immunotherapy targeting to amyloid beta

Alzheimer's disease(AD) is one of the most common types of dementia whose hallmarks include neurofibrillary tangles and senile plaques. The latter are mainly composed of amyloid-β proteins(Aβ), and it's suggested that Aβ may be the causative factor in AD pathogenesis. Immunotherapy targeting Aβ for preventing aggregation of Aβ and mildly clearing amyloid plaques has been a hot topic since 1999. Although the first clinical trial of Aβ vaccine, AN-1792, failed in phase II, its results suggested some key points in the design of Aβ vaccines. Avoiding the possible toxic Aβ specific T cell response and inducing a Th2 type cellular immune response may be beneficial for Aβ immunotherapy. Many associations and research groups are working on Aβ vaccine and some progress has been made in recent years. In this review, we have provided a detailed summary of past Aβ vaccines, which have been sorted by the immunogen, and we also discuss some recent progress and future perspectives.