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鸡体内抗多糖抗体反应不足。

Inadequate anti-polysaccharide antibody responses in the chicken.

作者信息

Jeurissen S H, Janse E M, van Rooijen N, Claassen E

机构信息

Dept. of Immunology, Institute for Animal Science and Health ID-DLO, Lelystad, The Netherlands.

出版信息

Immunobiology. 1998 Feb;198(4):385-95. doi: 10.1016/S0171-2985(98)80047-8.

Abstract

Chickens are notorious for the fact that they carry bacteria such as Salmonellae and Campylobacter, which can cause zoonoses by contamination of the end product, without hampering growth and development of the chicken itself. This carrier status can only been explained by the inability of the chickens immune system to eliminate the pathogen, this in turn being due to insufficient humoral responses towards the polysaccharides of the bacterial capsule. In a previous study, we demonstrated that in chickens a model thymus-independent type 2 (TI-2) polysaccharide antigen, trinitrophenylated Ficoll (TNP-Ficoll), hardly evokes a humoral immune response. Furthermore this TI-2 antigen was shown to exhibit a very specific initial localization pattern after intravenous injection, i.e. in the periellipsoidal lymphocyte sheaths (PELS) and the surrounding ring of macrophages. The functional equivalent of these macrophages in mammals, the marginal zone macrophages, were shown to suppress the humoral responses against TI-2 antigens. Therefore we investigated whether other standard TI-2 antigen models also induce low antibody responses, whether this low response is dose-dependent, and whether macrophages are responsible for this low response. It was found that other TI-2 antigens, such as hydroxyethyl starch and detoxified lipopolysaccharides, also induced very low IgM and IgG responses, indicating a general phenomenon that could not be overcome by using a higher dose of antigen. In addition, selective depletion of splenic macrophages with liposomes containing dichloromethylene diphosphonate prior to immunization increased the specific humoral response to TD and TI-1 antigens, but failed to do so for TI-2 antigen. This result indicates that the low humoral responses are not (only) due to a macrophage suppressive activity but also to other yet unknown mechanisms, for example the lack of responsive B cells in the splenic PELS.

摘要

鸡因携带诸如沙门氏菌和弯曲杆菌等细菌而声名狼藉,这些细菌可通过污染最终产品导致人畜共患病,却不妨碍鸡自身的生长发育。这种携带状态只能解释为鸡的免疫系统无法消除病原体,而这又是由于对细菌荚膜多糖的体液免疫反应不足所致。在先前的一项研究中,我们证明,在鸡体内,一种典型的非胸腺依赖性2型(TI-2)多糖抗原,三硝基苯基化的菲可(TNP-菲可),几乎不会引发体液免疫反应。此外,静脉注射后,这种TI-2抗原显示出非常特殊的初始定位模式,即在椭球周围淋巴细胞鞘(PELS)和周围的巨噬细胞环中。哺乳动物中这些巨噬细胞的功能等效物,边缘区巨噬细胞,被证明可抑制针对TI-2抗原的体液免疫反应。因此,我们研究了其他标准的TI-2抗原模型是否也诱导低抗体反应,这种低反应是否呈剂量依赖性,以及巨噬细胞是否对此低反应负责。结果发现,其他TI-2抗原,如羟乙基淀粉和解毒脂多糖,也诱导了非常低的IgM和IgG反应,表明这是一种普遍现象,无法通过使用更高剂量的抗原克服。此外,在免疫前用含有二氯亚甲基二膦酸盐的脂质体选择性清除脾脏巨噬细胞,增加了对TD和TI-1抗原的特异性体液反应,但对TI-2抗原却没有效果。这一结果表明,低体液免疫反应并非(仅)由于巨噬细胞的抑制活性,还由于其他未知机制,例如脾脏PELS中缺乏反应性B细胞。

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