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接种疫苗可通过训练肺泡巨噬细胞在小鼠中快速预防细菌性肺炎。

Vaccination induces rapid protection against bacterial pneumonia via training alveolar macrophage in mice.

机构信息

West China Biopharmaceutical Research Institute,West China Hospital, Sichuan University, Chengdu, China.

National Engineering Research Center of Immunological Products, Department of Microbiology and Biochemical Pharmacy, College of Pharmacy, Third Military Medical University, Chongqing, China.

出版信息

Elife. 2021 Sep 20;10:e69951. doi: 10.7554/eLife.69951.

Abstract

Vaccination strategies for rapid protection against multidrug-resistant bacterial infection are very important, especially for hospitalized patients who have high risk of exposure to these bacteria. However, few such vaccination strategies exist due to a shortage of knowledge supporting their rapid effect. Here, we demonstrated that a single intranasal immunization of inactivated whole cell of elicits rapid protection against broad -infected pneumonia via training of innate immune response in mice. Immunization-trained alveolar macrophages (AMs) showed enhanced TNF-α production upon restimulation. Adoptive transfer of immunization-trained AMs into naive mice mediated rapid protection against infection. Elevated TLR4 expression on vaccination-trained AMs contributed to rapid protection. Moreover, immunization-induced rapid protection was also seen in and pneumonia models, but not in and model. Our data reveal that a single intranasal immunization induces rapid and efficient protection against certain Gram-negative bacterial pneumonia via training AMs response, which highlights the importance and the possibility of harnessing trained immunity of AMs to design rapid-effecting vaccine.

摘要

针对多重耐药菌感染的快速保护的疫苗接种策略非常重要,特别是对于那些有很高暴露于这些细菌风险的住院患者。然而,由于缺乏支持其快速效果的知识,这样的疫苗接种策略很少。在这里,我们证明了,通过训练先天免疫反应,单次鼻腔内接种灭活的 whole cell 可快速保护小鼠免受广泛感染的肺炎。免疫接种训练的肺泡巨噬细胞(AMs)在再刺激时显示出增强的 TNF-α 产生。将免疫接种训练的 AMs 过继转移到未致敏的小鼠中可介导对感染的快速保护。接种训练的 AMs 上 TLR4 表达的升高有助于快速保护。此外,在 和 肺炎模型中也观察到了免疫诱导的快速保护,但在 和 模型中则没有。我们的数据表明,单次鼻腔内免疫接种通过训练 AMs 反应可快速有效地预防某些革兰氏阴性菌肺炎,这凸显了利用 AMs 的训练免疫来设计快速作用疫苗的重要性和可能性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6c1d/8455131/e6fe9690406d/elife-69951-fig1.jpg

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