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皂苷佐剂皂苷/单磷酰脂质A纳米颗粒对非人灵长类动物抗原递送和淋巴结激活的调节作用。

Modulation of antigen delivery and lymph node activation in nonhuman primates by saponin adjuvant saponin/monophosphoryl lipid A nanoparticle.

作者信息

Yousefpour Parisa, Zhang Yiming J, Maiorino Laura, Melo Mariane B, Arainga Ramirez Mariluz A, Kumarapperuma Sidath C, Xiao Peng, Silva Murillo, Li Na, Michaels Katarzyna K, Georgeson Erik, Eskandarzadeh Saman, Kubitz Michael, Groschel Bettina, Qureshi Kashif, Fontenot Jane, Hangartner Lars, Nedellec Rebecca, Love J Christopher, Burton Dennis R, Schief William R, Villinger Francois J, Irvine Darrell J

机构信息

Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

Ragon Institute of Massachusetts General Hospital, Massachusetts Institute of Technology and Harvard University, Cambridge, MA 02139, USA.

出版信息

PNAS Nexus. 2024 Nov 25;3(12):pgae529. doi: 10.1093/pnasnexus/pgae529. eCollection 2024 Dec.

Abstract

Saponin-based vaccine adjuvants are potent in preclinical animal models and humans, but their mechanisms of action remain poorly understood. Here, using a stabilized HIV envelope trimer immunogen, we carried out studies in nonhuman primates (NHPs) comparing the most common clinical adjuvant aluminum hydroxide (alum) with saponin/monophosphoryl lipid A nanoparticles (SMNP), an immune-stimulating complex-like adjuvant. SMNP elicited substantially stronger humoral immune responses than alum, including 7-fold higher peak antigen-specific germinal center B-cell responses, 18-fold higher autologous neutralizing antibody titers, and higher levels of antigen-specific plasma and memory B cells. Positron emission tomography and computed tomography imaging in live NHPs showed that, unlike alum, SMNP promoted rapid antigen accumulation in both proximal and distal lymph nodes (LNs). SMNP also induced strong type I interferon transcriptional signatures, expansion of innate immune cells, and increased antigen-presenting cell activation in LNs. These findings indicate that SMNP promotes multiple facets of the early immune response relevant for enhanced immunity to vaccination.

摘要

基于皂苷的疫苗佐剂在临床前动物模型和人体中都具有强大作用,但其作用机制仍知之甚少。在此,我们使用一种稳定的HIV包膜三聚体免疫原,在非人灵长类动物(NHP)中开展研究,将最常用的临床佐剂氢氧化铝(明矾)与皂苷/单磷酰脂质A纳米颗粒(SMNP,一种类似免疫刺激复合物的佐剂)进行比较。SMNP引发的体液免疫反应比明矾强得多,包括峰值抗原特异性生发中心B细胞反应高7倍、自体中和抗体滴度高18倍,以及抗原特异性血浆和记忆B细胞水平更高。对活体NHP进行的正电子发射断层扫描和计算机断层扫描成像显示,与明矾不同,SMNP促进抗原在近端和远端淋巴结(LN)中快速积累。SMNP还诱导强烈的I型干扰素转录特征、先天免疫细胞扩增,并增加LN中抗原呈递细胞的活化。这些发现表明,SMNP促进了与增强疫苗免疫相关的早期免疫反应的多个方面。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/31ca/11645456/526631add361/pgae529f1.jpg

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