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曼氏血吸虫感染可能会危及针对乙肝和破伤风类毒素免疫接种产生的抗体反应的保护水平持续时间。

Schistosoma mansoni Infection Can Jeopardize the Duration of Protective Levels of Antibody Responses to Immunizations against Hepatitis B and Tetanus Toxoid.

作者信息

Riner Diana K, Ndombi Eric M, Carter Jennifer M, Omondi Amos, Kittur Nupur, Kavere Emmy, Korir Harrison K, Flaherty Briana, Karanja Diana, Colley Daniel G

机构信息

Center for Tropical and Emerging Global Diseases and Department of Microbiology, University of Georgia, Athens, Georgia, United States of America.

Centre for Global Health Research, Kenya Medical Research Institute, Kisumu, Kenya.

出版信息

PLoS Negl Trop Dis. 2016 Dec 7;10(12):e0005180. doi: 10.1371/journal.pntd.0005180. eCollection 2016 Dec.

Abstract

BACKGROUND

Schistosomiasis is a disease of major public health importance in sub-Saharan Africa. Immunoregulation begins early in schistosome infection and is characterized by hyporesponsiveness to parasite and bystander antigens, suggesting that a schistosome infection at the time of immunization could negatively impact the induction of protective vaccine responses. This study examined whether having a Schistosoma mansoni infection at the time of immunization with hepatitis B and tetanus toxoid (TT) vaccines impacts an individual's ability to achieve and maintain protective antibody levels against hepatitis B surface antigen or TT.

METHODS

Adults were recruited from Kisumu Polytechnic College in Western Kenya. At enrollment, participants were screened for schistosomiasis and soil transmitted helminths (STHs) and assigned to groups based on helminth status. The vaccines were then administered and helminth infections treated a week after the first hepatitis B boost. Over an 8 month period, 3 blood specimens were obtained for the evaluation of humoral and cytokine responses to the vaccine antigens and for immunophenotyping.

RESULTS

146 individuals were available for final analysis and 26% were S. mansoni positive (Sm+). Schistosomiasis did not impede the generation of initial minimum protective antibody levels to either hepatitis B or TT vaccines. However, median hepatitis B surface antibody levels were significantly lower in the Sm+ group after the first boost and remained lower, but not significantly lower, following praziquantel (PZQ) treatment and final boost. In addition, 8 months following TT boost and 7 months following PZQ treatment, Sm+ individuals were more likely to have anti-TT antibody levels fall below levels considered optimal for long term protection. IL-5 levels in response to in vitro TT stimulation of whole blood were significantly higher in the Sm+ group at the 8 month time period as well.

CONCLUSIONS

Individuals with schistosomiasis at the start the immunizations were capable of responding appropriately to the vaccines as measured by antibody responses. However, they may be at risk of a more rapid decline in antibody levels over time, suggesting that treating schistosome infections with praziquantel before immunizations could be beneficial. The timing of the treatment as well as its full impact on the maintenance of antibodies against vaccine antigens remains to be elucidated.

摘要

背景

血吸虫病是撒哈拉以南非洲地区具有重大公共卫生意义的疾病。免疫调节在血吸虫感染早期就开始了,其特征是对寄生虫和旁观者抗原反应低下,这表明免疫接种时的血吸虫感染可能会对保护性疫苗反应的诱导产生负面影响。本研究调查了在接种乙肝疫苗和破伤风类毒素(TT)时感染曼氏血吸虫是否会影响个体产生并维持针对乙肝表面抗原或TT的保护性抗体水平的能力。

方法

从肯尼亚西部的基苏木理工学院招募成年人。在入组时,对参与者进行血吸虫病和土壤传播蠕虫(STH)筛查,并根据蠕虫感染状况分组。然后接种疫苗,并在首次乙肝疫苗加强接种一周后治疗蠕虫感染。在8个月的时间里,采集3份血液样本,以评估对疫苗抗原的体液和细胞因子反应以及进行免疫表型分析。

结果

146名个体可用于最终分析,其中26%为曼氏血吸虫阳性(Sm+)。血吸虫病并未阻碍对乙肝疫苗或TT疫苗产生初始最低保护性抗体水平。然而,首次加强接种后,Sm+组的乙肝表面抗体水平中位数显著较低,在接受吡喹酮(PZQ)治疗和最终加强接种后仍较低,但差异不显著。此外,在TT加强接种8个月后和PZQ治疗7个月后,Sm+个体的抗TT抗体水平更有可能降至被认为对长期保护最佳的水平以下。在8个月时,Sm+组对体外TT刺激全血产生的IL-5水平也显著更高。

结论

免疫接种开始时患有血吸虫病的个体能够通过抗体反应对疫苗做出适当反应。然而,随着时间的推移,他们的抗体水平可能有更快下降的风险,这表明在免疫接种前用吡喹酮治疗血吸虫感染可能有益。治疗的时机及其对维持针对疫苗抗原的抗体的全面影响仍有待阐明。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/08c4/5142771/e14badfac802/pntd.0005180.g001.jpg

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