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保留流感病毒的记忆。

Keeping the memory of influenza viruses.

作者信息

Combadière B, Sibéril S, Duffy D

机构信息

Institut national de la santé et de la recherche médicale (Inserm) U945, University of Pierre-and-Marie-Curie (UPMC), University Paris 06, France.

出版信息

Pathol Biol (Paris). 2010 Apr;58(2):e79-86. doi: 10.1016/j.patbio.2010.01.010. Epub 2010 Mar 19.

Abstract

Protection against pathogens is mediated by both humoral responses (neutralizing antibodies) and cellular immunity, both CD4+ and CD8+ cells. In the case of influenza viruses, circulating strains contain both variable and conserved T and B cell epitopes that are challenged after vaccination and/or infection. During infection, the role of T cells is to prevent viral dissemination in the organism by killing the infected cells and helping B cell antibody production to neutralize the virus. The threat of influenza virus increases the preparedness of protective immunity to pandemic and seasonal infection by vaccination. Several questions remain that need to be further addressed for the future development of innovative and rapidly efficient vaccines strategies. Firstly, what are the correlates of long-term protection (antibodies and/or T cells) against variant strains of influenza? How does the individual factors (age, natural immunity, vaccination and/or infection history) influence the generation and maintenance of memory cells? What are the factors allowing the maintenance of immune memory (regular contact with the pathogen or re-vaccination)? Secondly, what is the nature and quality (function / phenotype / location) of memory B and T cells? Finally, is it necessary to induce and maintain immunological memory against conserved proteins and/or to re-vaccinate against viral variants? What would be the consequences of repeated vaccination? These questions remain a subject of debate that will be further discussed. Since immunological memory is the cornerstone of vaccination, it is essential that we have a better understanding of its generation and maintenance over time as well as its contribution to recall responses during pandemics or after vaccination.

摘要

对病原体的保护由体液免疫反应(中和抗体)和细胞免疫介导,包括CD4+和CD8+细胞。就流感病毒而言,流行毒株同时含有可变和保守的T细胞和B细胞表位,这些表位在接种疫苗和/或感染后会受到挑战。在感染期间,T细胞的作用是通过杀死被感染细胞并帮助B细胞产生抗体来中和病毒,从而防止病毒在体内传播。流感病毒的威胁通过接种疫苗提高了对大流行和季节性感染的保护性免疫的准备程度。对于创新且高效的疫苗策略的未来发展,仍有几个问题需要进一步探讨。首先,针对流感变异株的长期保护(抗体和/或T细胞)的相关因素是什么?个体因素(年龄、天然免疫、接种疫苗和/或感染史)如何影响记忆细胞的产生和维持?允许维持免疫记忆的因素是什么(与病原体定期接触或再次接种疫苗)?其次,记忆B细胞和T细胞的性质和质量(功能/表型/位置)是什么?最后,是否有必要诱导并维持针对保守蛋白的免疫记忆和/或针对病毒变异株再次接种疫苗?重复接种疫苗会有什么后果?这些问题仍然是一个有争议的话题,将进一步讨论。由于免疫记忆是疫苗接种的基石,我们必须更好地了解其随时间的产生和维持,以及它在大流行期间或接种疫苗后对回忆反应的贡献。

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