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工程化免疫原与铝佐剂结合可增强体液免疫。

Engineered immunogen binding to alum adjuvant enhances humoral immunity.

机构信息

Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA, USA.

Consortium for HIV/AIDS Vaccine Development, The Scripps Research Institute, La Jolla, CA, USA.

出版信息

Nat Med. 2020 Mar;26(3):430-440. doi: 10.1038/s41591-020-0753-3. Epub 2020 Feb 17.

Abstract

Adjuvants are central to the efficacy of subunit vaccines. Aluminum hydroxide (alum) is the most commonly used vaccine adjuvant, yet its adjuvanticity is often weak and mechanisms of triggering antibody responses remain poorly understood. We demonstrate that site-specific modification of immunogens with short peptides composed of repeating phosphoserine (pSer) residues enhances binding to alum and prolongs immunogen bioavailability. The pSer-modified immunogens formulated in alum elicited greatly increased germinal center, antibody, neutralizing antibody, memory and long-lived plasma cell responses compared to conventional alum-adsorbed immunogens. Mechanistically, pSer-immunogen:alum complexes form nanoparticles that traffic to lymph nodes and trigger B cell activation through multivalent and oriented antigen display. Direct uptake of antigen-decorated alum particles by B cells upregulated antigen processing and presentation pathways, further enhancing B cell activation. These data provide insights into mechanisms of action of alum and introduce a readily translatable approach to significantly improve humoral immunity to subunit vaccines using a clinical adjuvant.

摘要

佐剂是亚单位疫苗效力的核心。氢氧化铝(明矾)是最常用的疫苗佐剂,但它的佐剂活性往往较弱,其触发抗体反应的机制仍知之甚少。我们证明,用由重复磷酸丝氨酸(pSer)残基组成的短肽对免疫原进行定点修饰,可以增强与明矾的结合,并延长免疫原的生物利用度。与传统的明矾吸附免疫原相比,明矾中配制的 pSer 修饰免疫原引发了大大增加的生发中心、抗体、中和抗体、记忆和长寿浆细胞反应。从机制上讲,pSer-免疫原:明矾复合物形成纳米颗粒,这些颗粒可以运送到淋巴结,并通过多价和定向的抗原呈递来触发 B 细胞激活。抗原修饰的明矾颗粒被 B 细胞直接摄取,上调了抗原加工和呈递途径,进一步增强了 B 细胞的激活。这些数据提供了对明矾作用机制的深入了解,并引入了一种易于转化的方法,使用临床佐剂显著提高亚单位疫苗的体液免疫。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c59/7223691/d0454af17803/41591_2020_753_Fig1_HTML.jpg

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