Literature DB >> 22933398

Acquisition of maternal antibodies both from the placenta and by lactation protects mouse offspring from Yersinia pestis challenge.

Zhizhen Qi1, Haihong Zhao, Qingwen Zhang, Yujing Bi, Lingling Ren, Xuecan Zhang, Hanqing Yang, Xiaoyan Yang, Qiong Wang, Cunxiang Li, Jiyuan Zhou, Youquan Xin, Yonghai Yang, Huiying Yang, Zongmin Du, Yafang Tan, Yanping Han, Yajun Song, Lei Zhou, Pingping Zhang, Yujun Cui, Yanfeng Yan, Dongsheng Zhou, Ruifu Yang, Xiaoyi Wang.   

Abstract

Artificially passive immunization has been demonstrated to be effective against Yersinia pestis infection in animals. However, maternal antibodies' protective efficacy against plague has not yet been demonstrated. Here, we evaluated the kinetics, protective efficacy, and transmission modes of maternal antibodies, using mice immunized with plague subunit vaccine SV1 (20 μg of F1 and 10 μg of rV270). The results showed that the rV270- and F1-specific antibodies could be detected in the sera of newborn mice (NM) until 10 and 14 weeks of age, respectively. There was no antibody titer difference between the parturient mice immunized with SV1 (PM-S) and the caesarean-section newborns (CSN) from the PM-S or between the lactating mice immunized by SV1 (LM-S) and the cross-fostered mice (CFM) during 3 weeks of lactation. The NM had a 72% protection against 4,800 CFU Y. pestis strain 141 challenge at 6 weeks of age, whereas at 14 weeks of age, NM all succumbed to 5,700 CFU of Y. pestis challenge. After 7 weeks of age, CFM had an 84% protection against 5,000 CFU of Y. pestis challenge. These results indicated that maternal antibodies induced by the plague subunit vaccine in mother mice can be transferred to NM by both placenta and lactation. Passive antibodies from the immunized mothers could persist for 3 months and provide early protection for NM. The degree of early protection is dependent on levels of the passively acquired antibody. The results indicate that passive immunization should be an effective countermeasure against plague during its epidemics.

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Year:  2012        PMID: 22933398      PMCID: PMC3491559          DOI: 10.1128/CVI.00455-12

Source DB:  PubMed          Journal:  Clin Vaccine Immunol        ISSN: 1556-679X


  30 in total

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