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雌二醇限制阴道内免疫接种后的病毒复制,导致黏膜 IgG 反应减弱和对生殖器疱疹挑战的非无菌保护。

Estradiol limits viral replication following intravaginal immunization leading to diminished mucosal IgG response and non-sterile protection against genital herpes challenge.

机构信息

Department of Pathology and Molecular Medicine, McMaster University, Hamilton, ON, Canada.

出版信息

Am J Reprod Immunol. 2010 Apr 1;63(4):299-309. doi: 10.1111/j.1600-0897.2009.00796.x. Epub 2010 Jan 11.

DOI:10.1111/j.1600-0897.2009.00796.x
PMID:20070285
Abstract

PROBLEM

Previously we reported that ovariectomized (OVX) mice receiving estradiol (E) prior to immunization with an attenuated strain of HSV-2 (TK-HSV-2) were not protected. Lack of protection in the E group was because of the inability of TK-HSV-2 to penetrate the thick keratinized epithelium. In this study, we determined the outcome of immunization after the thickening of vaginal epithelium following E-treatment waned. OVX, C57BL/6 mice were given Progesterone (P), E or saline (S) for 3 days and immunized with IVAG TK-HSV-2.

METHOD OF STUDY

To determine the time point at which E-treated mice could be successfully immunized, the mice were inoculated with TK-HSV-2 between days 1 and 7 (ED1-ED7) post-E-treatment and challenged with IVAG HSV-2 three weeks later.

RESULTS

The level of infection post-immunization correlated with HSV-2-specific IgG antibody level, which correlated with sterile protection. No viral infection was observed in ED1-ED3 groups and no specific antibodies were detected, resulting in no protection. Moderate infection was seen in ED5 group, resulting in low antibody production and non-sterile protection in 87.5% of mice. High antibody titers and sterile protection were observed in all groups that experienced robust infection post-immunization.

CONCLUSION

The results show that estradiol leads to limited viral replication and diminished mucosal IgG response, resulting in non-sterile immune protection against genital herpes infection.

摘要

问题

我们之前曾报道过,在接受弱毒 HSV-2(TK-HSV-2)免疫之前接受雌二醇(E)治疗的去卵巢(OVX)小鼠未得到保护。E 组缺乏保护作用是因为 TK-HSV-2 无法穿透厚厚的角化上皮。在这项研究中,我们确定了 E 治疗后阴道上皮增厚消退后免疫接种的结果。OVX、C57BL/6 小鼠接受孕激素(P)、E 或生理盐水(S)治疗 3 天,然后经 IVAG 接种 TK-HSV-2。

研究方法

为了确定可以成功对 E 治疗小鼠进行免疫接种的时间点,将小鼠在 E 治疗后第 1 至 7 天(ED1-ED7)接种 TK-HSV-2,并在 3 周后经 IVAG 接种 HSV-2 进行挑战。

结果

免疫接种后的感染水平与 HSV-2 特异性 IgG 抗体水平相关,而后者与无菌保护相关。在 ED1-ED3 组中未观察到病毒感染,也未检测到特异性抗体,因此没有保护作用。在 ED5 组中观察到中度感染,导致 87.5%的小鼠产生低水平抗体,产生非无菌保护。在所有经历强烈免疫接种后感染的组中均观察到高抗体滴度和无菌保护。

结论

结果表明,雌二醇导致病毒复制受限和黏膜 IgG 反应减弱,从而对生殖器疱疹感染产生非无菌免疫保护。

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