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胎儿三毛滴虫感染小鼠模型中的生殖系统和全身免疫反应

Genital and systemic immune responses in a murine model of Tritrichomonas foetus infection.

作者信息

Mutwiri G K, Corbeil L B

机构信息

Department of Pathology, University of California, San Diego Medical Center, 92103-8416, USA.

出版信息

J Parasitol. 1998 Apr;84(2):321-7.

PMID:9576506
Abstract

A reliable laboratory animal model would be useful for the study of immune responses to trichomoniasis, a sexually transmitted disease of human beings and cattle. Murine models are available, but pretreatment with estrogen is used, which may influence immune responses. To evaluate whether vaginal trichomoniasis could be established in nonestrogenized mice and to define the immune responses associated with the infection, CD1 and BALB/c mice were studied with or without estrogen treatment prior to inoculation with Tritrichomonas foetus. Tritrichomonas Foetus was cultured from the vagina and uterus of both estrogen-treated and untreated control mice for up to 26 wk. The infection was sustained better in BALB/c than in CD1 mice, suggesting that the former strain was most susceptible. In CD1 mice, infection was sustained less well in estrogen-treated than in untreated control mice, but there was no difference between treatment groups of BALB/c mice. IgA and IgG antibodies in vaginal secretions, uterine secretions, and serum specific for a surface antigen of T. foetus (TF1.17) were measured by enzyme-linked immunosorbent assay. In infected CD1 mice, vaginal IgA and IgG antibodies were detected by 8 wk postinoculation (PI). In infected BALB/c mice, vaginal IgA and IgG antibodies were detected by 12 wk PI. Uterine IgG responses predominated over IgA in estrogen-treated and untreated CD1 and BALB/c mice. There were high levels of IgG, but relatively no IgA in the sera of CD1 and BALB/c mice. Overall, the highest IgA response was in the vaginal secretions of infected CD1 mice, and some animals of this strain cleared the infection. These results show that a chronic trichomonad infection was established in mice without prior treatment with estrogen. The infection was associated with antibody responses in reproductive secretions and serum. This animal model will be useful in studying immunization to protect against trichomoniasis in mice not immunocompromised by estrogen.

摘要

一种可靠的实验动物模型对于研究毛滴虫病的免疫反应将很有用,毛滴虫病是人类和牛的一种性传播疾病。小鼠模型是可用的,但使用了雌激素预处理,这可能会影响免疫反应。为了评估在未用雌激素处理的小鼠中是否能建立阴道毛滴虫感染,并确定与感染相关的免疫反应,在用胎儿三毛滴虫接种之前,对CD1和BALB/c小鼠进行了有无雌激素处理的研究。从雌激素处理和未处理的对照小鼠的阴道和子宫中培养胎儿三毛滴虫长达26周。BALB/c小鼠中的感染比CD1小鼠维持得更好,这表明前一种品系最易感。在CD1小鼠中,雌激素处理组的感染维持情况不如未处理的对照小鼠,但BALB/c小鼠的处理组之间没有差异。通过酶联免疫吸附测定法测量阴道分泌物、子宫分泌物和血清中针对胎儿三毛滴虫表面抗原(TF1.17)的IgA和IgG抗体。在感染的CD1小鼠中,接种后8周(PI)检测到阴道IgA和IgG抗体。在感染的BALB/c小鼠中,接种后12周检测到阴道IgA和IgG抗体。在雌激素处理和未处理的CD

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