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1、,医学免疫学,上海第二医科大学免疫教研室,1,医学免疫学,上海第二医科大学免疫教研室,2,T 细胞亚群与功能,根据TCR种类 TCR-1(TCR),TCR-2(TCR ),根据TCR-2(TCR )表达CD4或CD8的不同 CD4+T分子表型为CD2、CD3、CD4 CD8+T分子表型为CD2、CD3、CD8,根据功能 Th、Tc、Ts、TDTH,根据对抗原的应答不同 初始T细胞、抗原活化过的T细胞、记忆性T细胞,T细胞亚群,CD4 + 、CD8 +亚群 CD4+T细胞识别由1317个氨基酸残基组成的抗原肽,并受自身的MHC II类限制。CD8 + T细胞识别810个氨基酸组成的抗原肽,并受M
2、HC I类限制。 TCRT细胞和TCRT细胞,5,Th、Tc、Ts和TDTH细胞 Th细胞 根据所分泌的细胞因子不同,将其分为Th0、Th1和Th2亚型。 Tc细胞 Tc1细胞主要分泌IFN;Tc2细胞则主要分泌IL-4、IL-5和IL-10。 Ts细胞 TDTH 主要为CD4 + Th1,6,(一)TCR T细胞 和 TCR T细胞,TCR 极大多态性 极少多态性 分布 外周血 60-70% 5-15% 组织 外周淋巴组织 黏膜上皮 表型 CD3+CD2+ 100% 100% CD4+CD8- 60-65% 20-50% CD4-CD8+ 30-35% 20-50% CD4-CD8- 5%
3、50% 识别抗原 8-17aa 简单多肽、HSP、脂类、多糖 MHC限制 经典MHC分子 MHC类似分子 辅助细胞 Th细胞 杀伤细胞 Tc细胞 Tc细胞,特性 TCR T细胞,TCRT细胞,按CD分子不同,按功能不同,T细胞,CD4T细胞,CD8T细胞,辅助性T细胞(Th),细胞毒性T细胞(CTL或Tc),抑制性T细胞(Ts),CD4T细胞 CD表型:CD3+CD4+CD8-,主要为Th细胞亚群,识别抗原时受MHC-类分子限制 通过分泌细胞因子发挥效应功能 CD4T细胞(部分)也具有细胞杀伤功能,作用特点,1.CD4+Th细胞及其功能,2. CD8T细胞 CD表型:CD3+CD8+CD4-,
4、主要为CTL细胞亚群,识别抗原时受MHC- 类分子限制 免疫调节作用, 如释放IFN-、TNF-和TNF-等细胞因子 具有细胞杀伤功能,作用特点,CD8+杀伤性T细胞 CTL的主要作用是直接杀伤靶细胞,有两种机制:细胞裂解和细胞凋亡,11,12,CD8+Tc细胞(CTL)及其功能,免疫应答的主要效应细胞,在肿瘤免疫和抗病毒免疫中发挥重要作用(抗肿瘤),作用特点:特异直接杀伤靶细胞,在杀伤过程中自身不受损伤,可反复连续杀伤。,作用机制:细胞裂解(cytolysis) 细胞凋亡 (apoptosis),抗肿瘤,Introduction of Th1/Th2 cells,In 1986, T.R.
5、Mosman and R.L. Coffman observed that individual clones of mouse helper T cells could be separated into two classes depending upon the specific cytokines the cells secrete in response to antigenic stimulation.,Induction of Th1 and Th2 Responses,Th2,Th1,Antigens,IL-4,IL-12 IFN-,APC,Nave CD4,Effector
6、Cells,Signal 2,Signal 1,IL-2 IFN-,IL-4 IL-5 IL-10,Cellular Immune Responses,Humoral Immune Responses,Leishmania major Infection in Mice Provides a Useful Model to Study Th1 and Th2 Differentiation and Memory in vivo,Leishmania major infection: Mouse Models,Balb/C,BL/6,Th 1 response,Death,Recovery,Th
7、 2 response,IL-12,IL-12/IFN-,Signaling of IL-12 Receptor,Expression 1: Expressed on Th1, Th2, N.K., and B cells 2: Expressed on activated Nave T, Th1, and N.K. cells,Regulation Enhanced by: activation of -CD28, IL-2, IL-7, IL-15, IFN- (mouse), IFN- (human) Inhibited by: IL-4, IL-10, TGF-, PGE2, Dex,
8、Cytokines On Th1 Cell Development,Pathogen,APC,CD4+ T Cell,STAT4,TCR,IFN-,IFN-+,IL-27,TCCR/ WSX-1,IL-12,IL-12,IL-23,IL-12,IL-18,IL-18,Nave CD4+,Th1,Th1 Effector,IL-12R1,2,IL-18R,IL-18R,IL-12R1,IL-12R1,IL-12R1,2,2,STAT1,T-bet,IFN-,T-bet,STAT4,STAT4,NFKB GADD45 p3B,IRAK NFKB,如果敲除IL-12基因细胞免疫功能下降80%,T淋巴
9、细胞的功能,(1)介导细胞免疫应答,(2)分泌细胞因子参与免疫调节,21,Interleukin-9 (IL-9)-producing T cells (Th9 Cells) 肥大细胞、过敏反应,Introduction,Recently, two reports described a discrete subset of interleukin-9(IL-9)-producing T cells that might be closely related to the TH2-cell lineage. These IL-9-producing T cells seem to be a d
10、istinct population that does not show the characteristics of other described T-cell subsets-“TH9” cells.,24,25,TGF- deviates TH2 cells to a “TH-9” fate,IL-9-producing T cells could be generated from TH2 cells that were exposed to TGF- in vitro, even when the TH2 cells were highly polarized.,IL-4 inh
11、ibits TGF-induced Foxp3+ T cells IL-4 actively inhibits the induction of Foxp3 in the presence of TGF-. The inhibition of Foxp3 expression by IL-4 is mediated through the IL-4-STAT6 pathway. The Foxp3 can directly interact with GATA-3 and this association inhibits GATA-3 mediated transactivation of
12、IL-5, which is one of its target genes.,CD4+,CD8+,CD4+25+,27,效应-调控 过强和过弱,The Role of Suppressor or Regulatory T Cells (Treg) in Immunity,Introduction,Regulation of immune responses to self-antigen is a complex process Maintaining self-tolerance Retaining the capacity to mount immune responses agains
13、t invading microorganisms,Discovery of Suppressor T Cells,In 1995, Sakaguchi et al made the seminal observation: The transfer of CD4+ T cells which had been depleted of the the minor subpopulation (10%) of cells to nu/nu recepients induced organ-specific autoimmune diseases in the majority of recipi
14、ents. The minor subpopulation of cells are CD4+CD25+ T cells.,Discovery of Suppressor T cells,CD4+CD25+ Regulatory T cells,A unique lineage of regulatory T cells capable of maintaining self tolerance in vivo,32,T,CD8,CD4,CD4+ 25+,Th1,Tc2,Tc1,Th2,Th3,Tr1,Peripheral T lymphocyte,5-10%,30%,Th4?,60%,Thy
15、mus,33,Overview of phenotypes and functions of CD4+ T cells,Nave CD4,Th1,Tr,Th2,IFN-,Cell mediated immune responses,IL-4 IL-5 IL-10 IL-13,humoral immune response,Tr 1,Th 3,CD4+ CD25+,High IL-10 , low TGF-,TGF-,cell-cell contact,Natural Tr in thymus contact-dependent Adaptive Tr in peripheral lymphoi
16、d tissue cytokines-dependant,Regulatory T cells,CD4+CD25+ Tr cells: Comprise 5-10% of peripheral CD4 T cells in human and mice Produced in thymus as an unique lineage of CD4 T cells Secret IL-10 and/or TGF-b, but little IL-2 Anergic and suppressive,CD45RBlow, CTLA-4 high,35,淋巴细胞及其亚群分析,T淋巴细胞及亚群: 外周血中
17、成熟淋巴细胞主要属于TCRT细胞,可分为Th、Ts、Treg,TCRT细胞和NK1.1T细胞等,他们都有一个共同的标志CD3。,36,a、辅助/诱导性T淋巴细胞(Th)占27-51%,是主要的功能亚群,主要表达CD3CD4CD8。 b、抑制/细胞毒性T淋巴细胞(Ts)占15-44%,是主要的效应性T细胞亚群,主要表达CD3CD4 CD8。 c、Treg细胞是近年来新发现的一个T淋巴细胞亚群,具有重要的免疫调节功能,在自身免疫病、肿瘤和器官移植排斥反应中具有重要作用,主要标志为CD4CD25FoxP3。,37,d、Th /Ts比例,一般采用CD4 /CD8比例,正常值2:1,免疫力低下时比例倒置
18、。 e、T淋巴细胞的绝对计数,在某些疾病中T淋巴细胞会大量减少;CD4和CD8T细胞均减少。 f、T淋巴细胞活化;CD69正常情况下极少表达,早期出现CD69表达,中期CD69、CD25(IL-2R)表达,晚期出现CD71(转铁蛋白受体)和HLA-DR表达。 g、初始T细胞和记忆T细胞亚群表达见157;,38,B细胞及亚群;B细胞在外周血占5%-15%,与自身免疫疾病、B细胞系的肿瘤关系密切;B慢性淋巴细胞白血病与淋巴瘤等主要表达CD19、20、21、22。 NK细胞:外周血占10%,CD16、CD56是特异性标志。NK细胞在抗感染、抗肿瘤和移植排斥反应中具有重要作用。 DC:是重要的抗原提呈细胞分为髓样CD1淋巴样CD2。重要标志CD11c+、HLA-DR+。,39,临床意义,总T和总B及其亚群的意义 总T(50-84%)和总B(5-18%)可以用来判断某些免疫缺陷和自身免疫性疾病。对CD4和CD8T细胞的测定有助于免疫缺陷疾病、自身免疫性疾病、移植排斥反应的监测。 CD4 /CD8的意义 评价自身免疫失调、免疫失调或免疫缺陷病病人的免疫状态,监测骨髓移植病人以免受到急性GVHD的攻击。(自免病比值升高,病毒感染、肿瘤、再障比值降低)。 NK细胞的意义 NK(7-40%)细胞能够介导对某些肿瘤细胞和病毒感染细胞的细胞毒性作用。,40,