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通过用强毒马红球菌进行口服免疫而受到保护、免受马红球菌肺炎侵害的幼驹中,与毒力相关蛋白特异性血清免疫球蛋白G同种型的表达

Virulence-associated protein-specific serum immunoglobulin G-isotype expression in young foals protected against Rhodococcus equi pneumonia by oral immunization with virulent R. equi.

作者信息

Hooper-McGrevy K E, Wilkie B N, Prescott J F

机构信息

Department of Pathobiology, University of Guelph, Guelph, Ont., Canada.

出版信息

Vaccine. 2005 Dec 30;23(50):5760-7. doi: 10.1016/j.vaccine.2005.07.050. Epub 2005 Aug 9.

Abstract

The purpose of this study was to determine whether foals immunized orally from 2 days of age with virulent Rhodococcus equi developed a protective pulmonary immune response and to characterise the antibody response of the immunized foals to the virulence-associated proteins (Vaps) of the bacterium. Two groups of foals were used. One (n=4) was given live R. equi ATCC 33701 orally at 2, 7, and 14 days of age. The second group comprised three non-immunized foals age-matched to the vaccinates. At 3 weeks of age, 1 week after the final immunization, both groups were challenged intrabronchially with virulent R. equi ATCC 33701 and observed for 2 weeks post-challenge. Unvaccinated foals became clinically pneumonic and had high fever with increased heart and respiratory rates and severe pneumonia evident at necropsy. Foals of the immunized group remained healthy and lung lesions were not found post-mortem. Thus, it is possible to immunize young foals orally to protect them by 3 weeks of age against lung challenge with R. equi, even in the presence of maternal antibodies. The antibody response of the immunized foals confirmed that VapA and VapC are highly immunogenic. The immunoglobulin G isotype-related serum antibody response of immunized compared to non-immunized foals had an IgGT bias and a relatively low IgGa:IgGb ratio, both features different from what has been previously observed in immune adults and immune foals. This suggests that the serum IgG isotype profile of antibody cannot be used as a measure of evidence of protection against R. equi pneumonia.

摘要

本研究的目的是确定从2日龄开始口服接种强毒马红球菌的幼驹是否能产生保护性肺部免疫反应,并表征免疫幼驹对该细菌毒力相关蛋白(Vaps)的抗体反应。使用了两组幼驹。一组(n = 4)在2日龄、7日龄和14日龄时口服接种活的马红球菌ATCC 33701。第二组由三头与接种疫苗的幼驹年龄匹配的未免疫幼驹组成。在3周龄时,即最后一次免疫后1周,两组均经支气管内接种强毒马红球菌ATCC 33701,并在攻毒后观察2周。未接种疫苗的幼驹出现临床肺炎,高热,心率和呼吸频率增加,尸检时可见严重肺炎。免疫组的幼驹保持健康,死后未发现肺部病变。因此,即使存在母源抗体,也有可能通过口服免疫幼驹,使其在3周龄时免受马红球菌肺部攻毒的影响。免疫幼驹的抗体反应证实VapA和VapC具有高度免疫原性。与未免疫幼驹相比,免疫幼驹的免疫球蛋白G同种型相关血清抗体反应具有IgGT偏向性和相对较低的IgGa:IgGb比值,这两个特征均与先前在免疫成年动物和免疫幼驹中观察到的不同。这表明血清IgG同种型抗体谱不能用作预防马红球菌肺炎的保护证据的衡量标准。

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