Toll样受体与树突状细胞介导的天然免疫和获得性免疫

树突状细胞(dendritic cells,DCs)作为迄今所发现的抗原提呈功能最强的一类抗原提呈细胞,是联结天然免疫和获得性免疫的桥梁。Toll样受体(Toll-like receptors,TLRs)是一类进化保守的胚系编码的模式识别受体,在DCs的抗原识别、递呈及激活T细胞等方面具有重要作用,是机体受外来抗原入侵后作出适当免疫反应的调控点。现就TLRs在不同DCs亚群中的分布、与DCs介导的天然免疫和获得性免疫的关系及DCs功能可塑性的分子基础作一综述。     

野猪Toll 样受体基因的结构和功能鉴定

Toll样受体(Toll-like receptors,TLRs)是介导天然免疫和获得性免疫的病原模式识别受体(Pattern recognition receptor,PRRs),能识别表达在病原微生物上高度保守的病原相关分子模式(Pathogen associated molecular patterns,PAMPs),并通过一定的信号转导途径引起核内相关基因的表达,启动和调节机体的免疫反应。     

趋化因子及其受体在连接天然免疫与获得性免疫中的作用

病原侵入组织引起天然免疫中巨噬细胞(Mφ)分泌趋化因子,趋化因子／趋化因子受体的表达与非成熟树突状细胞(DC)的迁移、成熟、归巢以及获得性免疫应答密切相关。整个过程涉及许多趋化因子和趋化因子受体的表达变化,正是这种表达变化的精细调节启动了免疫细胞的定向迁移、归巢和游走,搭起天然免疫和获得性免疫的桥梁。本文综述了趋化因子和趋化因子受体在连接天然免疫和获得性免疫应答中的重要作用。     

Toll样受体对病原真菌的天然免疫识别

天然免疫系统是宿主抵御病原入侵的第一道防线,在机体抗感染免疫中发挥重要作用。Toll样受体(Toll-like receptors,TLRs)是天然免疫系统最重要的模式识别受体(pattern recognitionreceptors,PRRs)之一,通过识别病原真菌的病原相关分子模式(pathogen-associated molecularpatterns,PAMPs),招募特异接头蛋白,激活一系列信号级联反应,引发炎症因子、趋化因子等的释放和树突状细胞(dendritic cells,DCs)的成熟,发挥抗真菌感染作用。通过简要介绍宿主的TLRs及信号通路的研究进展,总结了目前TLRs对不同病原真菌PAMPs的天然免疫识别及信号通路研究现状,以期对进一步研究宿主天然免疫系统与病原真菌相互作用的分子机制提供参考。     

Toll样受体的研究进展

Toll样受体是近几年发现的天然免疫受体,它们不仅能特异性地识别病原微生物的结构成分,激活天然免疫,同时也为激活获得性免疫提供共刺激信号。Toll样受体是天然免疫与获得性免疫之间的连接点。     

TLR9的特性及其介导的TLR9/CpG-DNA免疫信号通路

TLRs在天然免疫应答中发挥着重要作用,构成了机体抗感染的第一道防线,是沟通天然免疫和获得性免疫的桥梁。其中TLR9已经被证实能够识别细菌DNA中免疫刺激序列CpG,从而激活哺乳动物细胞的天然免疫机制,这一发现具有重要的生物学意义与应用价值。它不仅进一步推进了外源DNA激活哺乳动物抗感染天然免疫的进一步研究,更为CpG-DNA应用于抗感染、肿瘤和免疫缺陷疾病等的治疗提供新的思路,为改进DNA疫苗效果提供非常有益的帮助。     

TLR4及其作用的研究进展

Toll样受体(toll-like receptors,TLRs)因其积极的研究成果而成为近年来广受关注的一种病原体识别受体,TLRs分布相对比较广泛,不但在小肠上皮、呼吸上皮细胞表达,同时也在血管内皮细胞、树突状细胞[1]、大鼠脾及心肌细胞[2]等细胞中表达.研究证实,它属于模式识别受体(pattern recognition receptors,PRRs),病原相关分子模式(pathogen-associated molecule pattern,PAMPs)可被其辨别,然后引发一系列的信号转导,TLRs 是备受关注的一种PRRs.Toll样受体4(toll-like receptor 4,TLR4)是TLRs家族中极为重要的成员,是天然免疫系统识别病原微生物的主要受体,在天然免疫反应中扮演着关键性作用.细菌脂多糖(lipopolysaccharide,LPS)作为一类受体,主要作用是介导信号跨膜转导,尤其对革兰氏阴性菌所引起的感染性炎症起着极为关键的作用.由于近年来对TLR4介导的信号转导及TLR4与疾病的关系研究成为热点,本文就TLR4的信号转导、TLR4与LPS的关系及TLR4信号通路调节进行综述如下.     

模式识别受体介导的天然免疫反应调节获得性免疫的机理

模式识别受体（PRR）的发现推动了免疫学领域的迅速发展.在近15年时间里,揭示了PRR启动的天然免疫反应机制及信号转导途径,并对天然免疫反应调节获得性免疫产生的机制进行了广泛研究.本文综述该领域一些新的重要发现,集中讨论病原体激活抗原递呈细胞的天然免疫反应调节淋巴细胞介导的抗原特异性获得性免疫机理,以及不同天然免疫途径在宿主抵抗感染和修复组织损伤中的作用,并讨论该领域尚未解决的重要问题.     

流感病毒感染的模式识别及下游相关信号通路

流感病毒(influenza virus)轻症感染可由机体免疫系统清除,但重症感染则诱发肺脏免疫损伤。流感病毒的病原体相关分子模式(pathogen-associated molecular patterns,PAMPs)可被位于细胞膜、细胞器膜及胞质内的重要模式识别受体(pattern recognition receptors,PRRs)介导识别,活化一系列激酶及转录因子,诱导促炎细胞因子和趋化因子的表达、成熟和分泌,进一步激活天然免疫及获得性免疫应答细胞,介导炎症反应和诱导免疫病理损伤。PRRs是研究天然免疫应答启动机制及抑制重症感染诱导免疫病理损伤的重要靶点。现就Toll样受体(toll-like receptors,TLRs)中的TLR3、TLR7/8、TLR4、RIG-I样受体(RIG-I like receptors,RLRs)和NOD样受体(NOD-like receptor,NLR)在流感病毒感染中的识别及下游信号通路在免疫病理损伤中的作用机制作一综述。     

Toll样受体与抗感染免疫

Toll样受体家族是新近发现的天然免疫受体,它们不仅泛特异性地识别病原微生物的结构成分,而且也为获得性免疫中免疫细胞的活化提供共刺激信号,因此在抗感染免疫中具有重要作用.本文重点介绍Toll样受体与病原微生物结构成分的相应关系,信号转导途径及其他抗感染免疫中的作用.     

靶向 Toll 样受体的免疫调节剂研究进展

Toll 样受体是一类相对保守的模式识别受体,可以识别损伤相关分子模式和病原相关分子模式,从而启动天然免疫应答,在天然免 疫过程中发挥非常重要的作用。其介导的信号通路失调会引发各种炎症反应、癌症和自身免疫病等疾病。综述近年与 Toll 样受体有关的免 疫调节剂的研究进展,并概括与之相关的疾病,为靶向 Toll 样受体的免疫调节剂的研发提供一定参考。     

Toll样受体信号转导途径研究进展

Toll样受体(Toll-like receptors,TLRs)属于模式识别受体(pattern recognition receptors,PRRs)家族,识别高度保守的微生物组分-病原相关分子模式(pathogen-associated molecular pat-terns,PAMPS)。迄今为止,在人类基因组中已发现10个Toll样受体。这些受体通过感知不同的微生物刺激,招募特异接头蛋白,激活一系列信号级联反应,引发针对病原体的特异性免疫应答,是连接天然免疫和适应性免疫应答的桥梁。哺乳动物Toll样受体的发现引领天然免疫的研究进入飞速发展的时代。本文将对Toll样受体信号转导途径的最新进展作一综述,以便更好地理解Toll样受体介导的分子免疫机制,这将有助于研发免疫治疗的分子靶标,最终有效预防、控制Toll样受体介导的疾病。     

Toll样受体信号传导途径的研究进展

Toll样受体家族（Toll-like receptors,TLRs）成员在固有免疫反应,尤其是调节吞噬细胞（如巨噬细胞等）特异性识别微生物病原体抗原,分泌促炎细胞因子,上调共刺激分子,并诱导机体适应性免疫反应抗微生物病原体感染中发挥重要调控作用,被称为机体固有免疫和适应性免疫调节中的辅助受体（adjuvant receptor）。目前,对Toll样受体家族成员调控免疫反应信号传导途径的研究已成为分子免疫学领域的研究热点,认为主要存在髓样分化蛋白88（MyD88,是一种转接蛋白）依赖性和MyrD88非依赖性两条主要调控途径。本文仅就Toll样受体信号传导途径的研究进展作以简要综述。     

甲型流感病毒感染过程中干扰素介导的天然免疫应答机制

甲型流感病毒作为引起人类和动物急性呼吸道传染病的一个主要病原体,在世界范围内广泛流行。研究表明,甲型流感病毒感染宿主后会诱导宿主的天然免疫应答。甲型流感病毒感染可引起Toll样受体(Toll like receptors,TLRs)和RIG-Ⅰ样受体(RIG-Ⅰ like receptors,RLRs)等宿主模式识别受体介导的抗病毒信号通路的活化,并在多种机制调控下诱导干扰素和其他细胞因子的表达,如Ⅰ型干扰素、Ⅲ型干扰素等,从而启动干扰素刺激基因(Interferon stimulated genes,ISGs)的转录及其抗病毒蛋白的表达,进而实现抗病毒作用。本文就甲型流感病毒感染与干扰素介导的天然免疫应答相关的信号通路和调控机制进行综述。     

Toll-like receptors in autoimmunity with special reference to systemic lupus erythematosus

The Toll-like receptor (TLR) family plays a fundamental role in host innate immunity by mounting a rapid and potent inflammatory response to pathogen infection. TLRs recognize distinct microbial components and activate intracellular signaling pathways that induce expression of host inflammatory genes. Several studies have indicated that TLRs are implicated in many inflammatory and immune disorders. Extensive research in the past decade to understand TLR-mediated mechanisms of innate immunity has enabled pharmaceutical companies to begin to develop novel therapeutics for the purpose of controlling an inflammatory disease. The roles of TLRs in the development of autoimmune diseases have been studied. TLR7 and TLR9 have key roles in production of autoantibodies and/or in development of systemic autoimmune disease. It remains to be determined their role in apoptosis, in the pathogenesis of RNA containing immune complexes, differential expression of TLRs by T regulatory cells.     

Origin of Toll-Like Receptor-Mediated Innate Immunity

Toll-related receptors (TLR) have been found in four animal phyla: Nematoda, Arthropoda, Echinodermata, and Chordata. No TLR has been identified thus far in acoelomates. TLR genes play a pivotal role in the innate immunity in both fruit fly and mammals. The prevailing view is that TLR-mediated immunity is ancient. The two pseudocoelomate TLRs, one each from Caenorhabditis elegans and Strongyloides stercoralis, were distinct from the coelomate ones. Further, the only TLR gene (Tol-1) in Ca. elegans did not appear to play a role in innate immunity. We argue that TLR-mediated innate immunity developed only in the coelomates, after they split from pseudocoelomates and acoelomates. We hypothesize that the function of TLR-mediated immunity is to prevent microbial infection in the body cavity present only in the coelomates. Phylogenetic analysis showed that almost all arthropod TLRs form a separate cluster from the mammalian counterparts. We further hypothesize that TLR-mediated immunity developed independently in the protostomia and deuterostomia coelomates.     

抗病毒感染固有免疫应答的信号转导

入侵病毒的探知和适应性免疫应答启动均依靠固有免疫系统。三种模式识别受体(PRRs)在宿主防御系统第一线占据极其重要地位:Toll样受体、维甲酸诱导基因I样受体、核苷酸结合寡聚化结构域样受体。PRRs识别病原相关分子模式(PAMP)或危险信号分子模式(DAMPs)启动和调节固有免疫和适应性免疫应答。每种PRR都有单独的识别配体和细胞定位。激活的PRRs将信号分子传递给其配体分子(MyD88,TRIF,IRAK,IPS-1),配体活化后作为信使激活信号途径下游激酶(IKK复合物,MAPKs,TBK1,RIP-1)和转录因子(NF-κB,AP-1,IRF3),最终产生细胞因子、趋化因子、促炎细胞因子和I型干扰素。本文重点讨论PRRs信号通路及该领域取得的成果,以期为人类健康和免疫疾病防治提供策略。     

Autophagy in regulation of Toll-like receptor signaling

Toll-like receptors (TLRs) serve as the major innate immune sensors for detection of specific molecular patterns on various pathogens. TLRs activate signaling events mainly by utilizing ubiquitin-dependent mechanisms. Recent research advances have provided evidence that TLR signaling is linked to induction of autophagy. Autophagy is currently known to affect both of the immune defense and suppression of inflammatory responses. In TLR-associated immune responses, autophagic lysis of intracellular microbes (called xenophagy) contributes to the former mechanism, while the latter seems to be mediated by the control of the mitochondrial integrity or selective autophagic clearance of aggregated signaling proteins (called aggrephagy). Several autophagy-related ubiquitin-binding proteins, such as SQSTM1/p62 and NDP52, mediate xenophagy and aggrephagy. In this review, we summarize the expanded knowledge regarding TLR signaling and autophagy signaling. After that, we will focus on autophagy-associated signaling downstream of TLRs and the effect of autophagy on TLR signaling, thus highlighting the signaling crosstalk between the TLR-associated innate immune responses and the regulation of innate immunity by xenophagy and aggrephagy.     

Microbe‐inducible trafficking pathways that control Toll‐like receptor signaling

The receptors of the mammalian innate immune system are designed for rapid microbial detection, and are located in organelles that are conducive to serve these needs. However, emerging evidence indicates that the sites of microbial detection are not the sites of innate immune signal transduction. Rather, microbial detection triggers the movement of receptors to regions of the cell where factors called sorting adaptors detect active receptors and promote downstream inflammatory responses. These findings highlight the critical role that membrane trafficking pathways play in the initiation of innate immunity to infection. In this review, we describe pathways that promote the microbe‐inducible endocytosis of Toll‐like receptors (TLRs), and the microbe‐inducible movement of TLRs between intracellular compartments. We highlight a new class of proteins called Transporters Associated with the eXecution of Inflammation (TAXI), which have the unique ability to transport TLRs and their microbial ligands to signaling‐competent regions of the cell, and we discuss the means by which the subcellular sites of signal transduction are defined.      

鱼类模式识别受体的研究进展

天然免疫（innate immunity）是基于对病原微生物成分的非克隆性识别而启动的快速防御反应。天然免疫系统可通过胚系编码的模式识别受体（pattern-recognition receptors,PRR）识别恒定不变的病原基元,即病原相关分子模式（pathogen-associated molecular patterns,PAMPs）,启动信号级联转导,最终PRRs信号激活宿主免疫和前炎性基因的表达,引发针对所识别病原的免疫反应。目前PRRs主要分为5类,即C-型Lectins、Toll样受体（Toll-like receptors,TLRs）、视黄酸诱导基因I样受体（retinoic acid inducible gene I-like receptors,RLRs）、包含核苷酸结合区和亮氨酸富集区蛋白（the nucleotide-binding domain,leucine-rich repeatcontaining proteins,NLRs,也称NOD样受体）和最近发现的AIM样受体（absent in melanoma（AIM）-like receptors,ALRs）。近年来,随着5种鱼类基因组序列草图的完成,大量鱼类PRRs基因被发现,一些PRRs的配体特异性及其相关信号途径正在逐渐明晰。为此,将对鱼类Toll样受体（TLRs）、视黄酸诱导基因I样受体（RLRs）和NOD样受体（NLRs）的研究进展进行综述。