| 1. | Tumor antigens of hepatocellular carcinoma and its specific cellular immunity 肝癌的肿瘤抗原与特异性细胞免疫 |
| 2. | Tumor cell - derived exosomes containing tumor antigens and mhc class i molecule could present tumor antigens to dcs and induce cd8 + t cell - dependent antitumor immune responses significantly 其含有mhc类分子和lamp - 1 ,能够将肿瘤抗原呈递给抗原递呈细胞,产生显著的cd8 ~ + t细胞依赖的抗肿瘤免疫反应。 |
| 3. | It has been reported by candido et al ( 2001 ) that intratumoral delivery of dc could efficiently induce specific antitumor immunity , resulting in tumor growth inhibition in established breast cancer 若能通过直接瘤内注射的方法,让dc在肿瘤局部获得相应的肿瘤抗原以诱导机体产生抗肿瘤免疫,无疑是最经济、最简便、具有临床应用前景的方法。 |
| 4. | Objective from 1990s , the successful cloning of many tumor antigen genes of human kind has driven the development of tumor immunology enormously . and so does it to the application of tumor immunodiagno sties and immunotherapy 目的: 20世纪90年代以来,多种人类肿瘤抗原基因克隆的成功,大大推动了肿瘤免疫学理论的发展,也促进了肿瘤免疫诊断和免疫治疗的应用。 |
| 5. | These findings of the specific ctls epitopes in irbp and pedf may lead to improved understanding of the pathogenesis of uveitis . our study also provides a strategy to identify specific ctls epitopes within tumour antigen , which is helpful to make tumour vaccine for the patients 本研究也为寻找肿瘤抗原中具有诱导特异性ctls能力的肽片段提供了一种策略,为制备肽片段肿瘤疫苗提供了理论基础。 |
| 6. | Though with various advantages , these tumor vaccines are because of complicated to prepare , restricted availability of relevant tumor antigens , the lack of molecularly defined tumor antigen delivery or targeting systems and the effects are relatively not promising 这些肿瘤疫苗的制备机理均在于提高对肿瘤抗原的递呈作用。缺点是制备工艺复杂、效果相对不够理想。 exosomes是由多种细胞分泌的来源于多囊泡体的小的膜性囊泡。 |
| 7. | At present , in an attempt to stimulate specific antitumor immunity , experimental models and clinical studies are currently evaluating the potent antigen - presenting capacity of dc combined with single or multiple tumor antigen epitopes . however , there are several problems in utilizing pulsing dc with synthetic immunodominant peptides from identified antigens . 1 ) the potential induction of tolerance ; 2 ) the need to determine the patient ' s hla haplotype , the limitation of therapy to patients whose tumors express defined specific tumor antigens in the context of the correct hla phenotype , the unavailability of peptides for all hla haplotypes ; 3 ) the lack of cd4 help cell - related epitopes for most antigens ; and 4 ) the ctl resulting from such protocols have a good in vitro capacity to kill peptide - pulsed target cells but only a modest capacity to kill tumor cells 但是,学者们发现这一疗法存在着如下的缺陷:单一ctl表位抗原肽的应用其抗肿瘤作用弱于多种肿瘤抗原的联合应用,且有诱导免疫耐受的潜在危险,有时反而会促进肿瘤的生长;事先需对患者的hla单倍型进行鉴定,以确定ctl表位与hla单倍型是否匹配,目前尚缺乏能与所有hla单倍型相匹配的ctl表位,从而限制了这一疗法的应用;这一疗法所产生的ctl在体外能有效杀伤经肿瘤抗原肽共孵育过的靶细胞,但对肿瘤细胞的杀伤能力较弱:这种l表位抗原肽缺乏cd4汀h细胞相关的表位,因此,不能诱导有效的th细胞免疫应答。 |
| 8. | To circumvent these deficits , novel antigen - delivery systems utilizing cytokine gene - modified tumor cells and dc or fusion of dc with tumor cells have resulted in induction of antitumor immunity . however , this u approach is difficult in some cases ( for example in breast cancer ) because only rarely has it been possible to isolate enough viable tumor cells from an individual to prepare the vaccine 为了克服上述缺陷,有学者采用灭活的肿瘤细胞、肿瘤抗原提取物(包括肿瘤细胞裂解物、 it na和洗脱肽等)冲击致敏dc或将肿瘤细胞与dc融合后再回输体内以激发机体的抗肿瘤免疫应答,也取得了较好的疗效。 |
| 9. | Methods employed to prepare vaccine include rumor cells genetically modified with cytokines , costimulatory molecules and tumor antigenic peptides , dendritic cells ( dc ) primed with tumor antigens in vitro or genetically modified with tumor antigens , or fusion of tumor cells with antigen presenting cells ( apc ) 现有的比较受到关注的制备肿瘤疫苗的方法有各种细胞因子、共刺激分子、肿瘤抗原肽等基因修饰的肿瘤细胞疫苗;体外抗原致敏的或肿瘤抗原肽基因修饰的树突状细胞疫苗;肿瘤细胞与抗原递呈细胞融合疫苗等。 |
| 10. | Dcs play a pivotal role in the development of antitumor immunity . t lymphocytes immune response induced by direct antigen - pulsed dcs can not maintain longer for peptides - mhc department or mhc molecules degeneration . the method of dcs loading with tumor antigen gene is another potential approach to enhancing and maintaining immune response 在用抗原直接刺激dc时,由于抗原- mhc复合物解离或细胞mhc分子降解而不能维持所诱导的t细胞免疫应答,借助载体把肿瘤抗原基因导入dc后肿瘤抗原在dc内的持续表达能增强其抗原提呈能力并能维持所诱导的免疫效应。 |