Emoto M, Neuhaus O, Emoto Y, Kaufmann S H
Department of Immunology, University of Ulm, Germany.
Infect Immun. 1996 Feb;64(2):569-75. doi: 10.1128/iai.64.2.569-575.1996.
Numerous microbial pathogens, including Listeria monocytogenes, enter the host through the intestine. Although relatively little is known about the biological functions of intestinal intraepithelial lymphocytes (i-IEL), they are generally considered a first line of defense against intestinal infections. In the mouse, the vast majority of i-IEL express the CD8 coreceptor either as a CD8 alpha/alpha homodimer or as a CD8 alpha/beta heterodimer. The CD8 receptor of T-cell receptor TcR gamma/delta i-IEL is exclusively homodimeric, whereas the CD8-expressing TcR alpha/beta i-IEL segregate into equal fractions of CD8 alpha/alpha and CD8 alpha/beta cells. We infected beta 2-microglobulin (beta 2m)+/- mice (possessing all i-IEL populations) and beta 2m -/- mutant mice (lacking all CD8 alpha/beta + i-IEL and having few CD8 alpha/alpha + TcR alpha/beta i-IEL) with L. monocytogenes per os and determined their biological functions after TcR ligation with monoclonal antibodies. Cytolytic activities of TcR alpha/beta and TcR gamma/delta i-IEL from beta 2m +/- mice were not influenced by intestinal listeriosis. Cytolytic activities of TcR alpha/beta i-IEL were impaired in uninfected beta 2m -/- mice, but this reduction was reestablished as a consequence of intestinal listeriosis. Frequencies of gamma interferon (IFN-gamma)-producing TcR alpha/beta i-IEL in uninfected beta 2m -/- mice were reduced, compared with that in their heterozygous controls. Equally low frequencies of IFN-gamma-producing TcR gamma/delta i-IEL in beta 2M +/- and beta 2m-/- mutants were found. Listeriosis increased frequencies of INF-gamma-producing TcR alpha/beta and TcR gamma/delta i-IEL in both mouse strains. Most remarkably, the proportion of IFN-gamma-producing TcR gamma/delta i-IEL was elevated 10-fold in listeria-infected beta 2M -/- mice. Our findings show that the beta 2m-independent CD8 beta- i-IEL expressing either TcR alpha/beta or TcR gamma/delta are stimulated by intestinal listeriosis independent of regional beta 2m expression. We conclude that the three major CD8+ i-IEL populations are stimulated by intestinal listeriosis and that CD8 beta- i-IEL compensate for the total lack of CD8 beta+ i-IEL in beta 2M -/- mutant mice. Hence, in contrast to the peripheral immune system, which crucially depends on CD8 alpha/beta + TcR alpha/beta lymphocytes, the mucosal immune system can rely on additional lymphocytes expressing the CD8 alpha/alpha homodimer.
包括单核细胞增生李斯特菌在内的众多微生物病原体通过肠道进入宿主。尽管人们对肠道上皮内淋巴细胞(i-IEL)的生物学功能了解相对较少,但它们通常被认为是抵御肠道感染的第一道防线。在小鼠中,绝大多数i-IEL表达CD8共受体,其形式为CD8α/α同二聚体或CD8α/β异二聚体。T细胞受体TcRγ/δ i-IEL的CD8受体仅为同二聚体,而表达CD8的TcRα/β i-IEL则等量分为CD8α/α和CD8α/β细胞。我们经口用单核细胞增生李斯特菌感染β2微球蛋白(β2m)+/-小鼠(拥有所有i-IEL群体)和β2m -/-突变小鼠(缺乏所有CD8α/β + i-IEL且仅有少量CD8α/α + TcRα/β i-IEL),并用单克隆抗体与TcR连接后测定它们的生物学功能。来自β2m +/-小鼠的TcRα/β和TcRγ/δ i-IEL的细胞溶解活性不受肠道李斯特菌病的影响。未感染的β2m -/-小鼠中TcRα/β i-IEL的细胞溶解活性受损,但这种降低因肠道李斯特菌病而恢复。与杂合对照相比,未感染的β2m -/-小鼠中产生γ干扰素(IFN-γ)的TcRα/β i-IEL的频率降低。在β2M +/-和β2m-/-突变体中发现产生IFN-γ的TcRγ/δ i-IEL的频率同样低。李斯特菌病增加了两种小鼠品系中产生INF-γ的TcRα/β和TcRγ/δ i-IEL的频率。最显著的是,在感染李斯特菌的β2M -/-小鼠中,产生IFN-γ的TcRγ/δ i-IEL的比例提高了10倍。我们的研究结果表明,表达TcRα/β或TcRγ/δ的不依赖β2m的CD8β- i-IEL受到肠道李斯特菌病的刺激,而与局部β2m表达无关。我们得出结论,三种主要的CD8+ i-IEL群体受到肠道李斯特菌病的刺激,并且CD8β- i-IEL弥补了β2M -/-突变小鼠中完全缺乏的CD8β+ i-IEL。因此,与严重依赖CD8α/β + TcRα/β淋巴细胞的外周免疫系统不同,黏膜免疫系统可以依赖表达CD8α/α同二聚体的其他淋巴细胞。
