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小鼠母体无细胞百日咳疫苗接种可损害后代对百日咳博德特氏菌感染的细胞免疫。

Maternal acellular pertussis vaccination in mice impairs cellular immunity to Bordetella pertussis infection in offspring.

出版信息

JCI Insight. 2023 Sep 22;8(18):e167210. doi: 10.1172/jci.insight.167210.

Abstract

Given the resurgence of pertussis, several countries have introduced maternal tetanus, diphtheria, and acellular pertussis (aP) vaccination during pregnancy to protect young infants against severe pertussis. Although protective against the disease, the effect of maternal aP vaccination on bacterial colonization of the offspring is unknown. Here, we used a mouse model to demonstrate that maternal aP immunization, either before or during pregnancy, protects pups from lung colonization by Bordetella pertussis. However, maternal aP vaccination resulted in significantly prolonged nasal carriage of B. pertussis by inhibiting the natural recruitment of IL-17-producing resident memory T cells and ensuing neutrophil influx in the nasal tissue, especially of those with proinflammatory and cytotoxic properties. Prolonged nasal carriage after aP vaccination is due to IL-4 signaling, as prolonged nasal carriage is abolished in IL-4Rα-/- mice. The effect of maternal aP vaccination can be transferred transplacentally to the offspring or via breastfeeding and is long-lasting, as it persists into adulthood. Maternal aP vaccination may, thus, augment the B. pertussis reservoir.

摘要

鉴于百日咳的死灰复燃,一些国家在孕妇怀孕期间引入破伤风、白喉和无细胞百日咳(aP)疫苗,以保护幼儿免受严重百日咳的侵害。尽管能预防这种疾病,但母体 aP 疫苗接种对后代细菌定植的影响尚不清楚。在这里,我们使用小鼠模型证明,母体 aP 免疫接种,无论是在怀孕前还是怀孕期间,都可以保护幼崽免受百日咳博德特氏菌肺部定植。然而,母体 aP 疫苗接种导致 B. pertussis 在鼻腔中的携带时间明显延长,这是通过抑制天然募集产生白细胞介素-17 的常驻记忆 T 细胞以及随后在鼻组织中中性粒细胞的涌入来实现的,特别是那些具有促炎和细胞毒性特性的细胞。aP 疫苗接种后的延长鼻腔携带是由于 IL-4 信号,因为在 IL-4Rα-/-小鼠中,延长的鼻腔携带被消除。母体 aP 疫苗接种的效果可以通过胎盘转移给后代,也可以通过母乳喂养传递,并且是持久的,因为它会持续到成年期。因此,母体 aP 疫苗接种可能会增加 B. pertussis 的储存库。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a04b/10561720/01a8ad5d3bfa/jciinsight-8-167210-g016.jpg

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