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Systemic and Mucosal Immune Responses in Mice after Mucosal Immunization with Group B Streptococcus Type III Capsular Polysaccharide-Cholera Toxin B Subunit Conjugate Vaccine

机译:B组链球菌III型荚膜多糖-霍乱毒素B亚基粘膜免疫后小鼠的全身和粘膜免疫反应。

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摘要

Group B streptococci (GBS) colonize the female genital and rectal tracts and can cause invasive infection in susceptible newborns. An optimally effective GBS vaccine should induce mucosal and systemic immunity. In this study, we investigate the local and systemic immune responses to GBS type III capsular polysaccharide (CPS) after mucosal vaccination of mice via intranasal, peroral, rectal, and vaginal routes, with GBS type III CPS conjugated with recombinant cholera toxin B subunit (GBS III CPS-rCTB). Cholera toxin (CT) was added as an adjuvant. Immunoglobulin G (IgG) and IgA antibodies to the CPS were tested in serum, lungs, and intestinal, rectal, and vaginal extracts by enzyme-linked immunosorbent assay. The conjugated CPS administered by intranasal, peroral, rectal, and vaginal routes was much more effective at inducing both mucosal and systemic antibody responses to GBS III CPS than was unconjugated CPS. The CPS-specific immune responses in various organs were dependent on the route of immunization. Generally, the highest levels of IgA and IgG were generated in the regions or sites of the conjugate exposure. Thus, intranasal vaccination elicited the highest anti-CPS IgA and IgG antibody levels in the lungs, whereas peroral administration in the intestinal site and vaginal vaccination elicited the highest antibody levels in the vagina. Rectal vaccination was superior to the other routes in inducing high antibody levels in the rectum. The four routes of mucosal vaccination also induced distant antibody responses to CPS. Rectal vaccination induced high specific IgA levels in the vagina and intestine, and oral administration induced high specific IgA levels in the lungs and rectum. All four routes of vaccination with the conjugate elicited similarly high levels of anti-CPS IgG in serum. Intranasal vaccination with different doses of the conjugate (10, 30, and 80 μg of CPS) did not have a significant influence on the anti-CPS specific antibody responses. Intranasal immunization induced better antibody responses when one dose of the conjugate was divided and given on three consecutive days compared to administration of the full dose on one occasion. In conclusion, rectal and vaginal vaccination may be the best way of stimulating anti-CPS immune responses in the rectal and vaginal tracts, while high levels of anti-CPS antibodies in the lungs can be achieved after intranasal administration. The vaccination regimen thus might influence the mucosal immune response to CPS. This conjugate may serve as an effective mucosal vaccine for preventing mucosal colonization and invasive infection caused by GBS.
机译:B组链球菌(GBS)定植于女性生殖道和直肠,可在易感新生儿中引起侵袭性感染。最佳效果的GBS疫苗应诱导粘膜和全身免疫。在这项研究中,我们调查了通过鼻内,经口,直肠和阴道途径对小鼠进行粘膜接种后对GBS III型荚膜多糖(CPS)的局部和全身免疫反应,其中GBS III型CPS与重组霍乱毒素B亚基结合( GBS III CPS-rCTB)。加入霍乱毒素(CT)作为佐剂。通过酶联免疫吸附测定法在血清,肺和肠,直肠和阴道提取物中检测了针对CPS的免疫球蛋白G(IgG)和IgA抗体。通过鼻内,经口,直肠和阴道途径施用的共轭CPS比未共轭CPS更有效地诱导对GBS III CPS的粘膜和全身抗体反应。各个器官中的CPS特异性免疫反应取决于免疫途径。通常,在结合物暴露的区域或部位产生最高水平的IgA和IgG。因此,鼻内疫苗接种在肺中引起最高的抗CPS IgA和IgG抗体水平,而在肠道部位经口给药和阴道疫苗接种在阴道中引起最高抗体水平。直肠接种在直肠中诱导高抗体水平方面优于其他途径。粘膜疫苗接种的四种途径也诱导了对CPS的遥远抗体反应。直肠疫苗接种可在阴道和肠道中诱导高特异性IgA水平,而口服给药可在肺和直肠中诱导高特异性IgA水平。用缀合物接种的所有四个途径在血清中引起相似高水平的抗CPS IgG。鼻内接种不同剂量的偶联物(10、30和80μgCPS)对抗CPS特异性抗体反应没有显着影响。与一剂全剂量相比,一剂偶联物被分开并连续三天给药时,鼻内免疫诱导了更好的抗体反应。总之,直肠和阴道疫苗接种可能是刺激直肠和阴道中抗CPS免疫反应的最佳方法,而鼻内给药后可以在肺中获得高水平的抗CPS抗体。因此,疫苗接种方案可能会影响粘膜对CPS的免疫反应。该缀合物可以用作预防由GBS引起的粘膜定植和侵袭性感染的有效粘膜疫苗。

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