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比较尿苷和 N1-甲基假尿苷 mRNA 平台在开发安第斯病毒疫苗中的应用。

Comparison of uridine and N1-methylpseudouridine mRNA platforms in development of an Andes virus vaccine.

机构信息

Department of Pathology, University of Texas Medical Branch, Galveston, TX, USA.

Galveston National Laboratory, Galveston, TX, USA.

出版信息

Nat Commun. 2024 Jul 30;15(1):6421. doi: 10.1038/s41467-024-50774-3.

Abstract

The rodent-borne Andes virus (ANDV) causes a severe disease in humans. We developed an ANDV mRNA vaccine based on the M segment of the viral genome, either with regular uridine (U-mRNA) or N1-methylpseudouridine (m1Ψ-mRNA). Female mice immunized by m1Ψ-mRNA developed slightly greater germinal center (GC) responses than U-mRNA-immunized mice. Single cell RNA and BCR sequencing of the GC B cells revealed similar levels of activation, except an additional cluster of cells exhibiting interferon response in animals vaccinated with U-mRNA but not m1Ψ-mRNA. Similar immunoglobulin class-switching and somatic hypermutations were observed in response to the vaccines. Female Syrian hamsters were immunized via a prime-boost regimen with two doses of each vaccine. The titers of glycoprotein-binding antibodies were greater for U-mRNA construct than for m1Ψ-mRNA construct; however, the titers of ANDV-neutralizing antibodies were similar. Vaccinated animals were challenged with a lethal dose of ANDV, along with a naïve control group. All control animals and two animals vaccinated with a lower dose of m1Ψ-mRNA succumbed to infection whereas other vaccinated animals survived without evidence of virus replication. The data demonstrate the development of a protective vaccine against ANDV and the lack of a substantial effect of m1Ψ modification on immunogenicity and protection in rodents.

摘要

携带啮齿动物的安第斯病毒 (ANDV) 可导致人类严重疾病。我们基于病毒基因组的 M 片段开发了一种 ANDV mRNA 疫苗,该疫苗使用常规尿嘧啶 (U-mRNA) 或 N1-甲基假尿嘧啶 (m1Ψ-mRNA)。用 m1Ψ-mRNA 免疫的雌性小鼠比用 U-mRNA 免疫的小鼠产生稍大的生发中心 (GC) 反应。GC B 细胞的单细胞 RNA 和 BCR 测序显示,除了在接种 U-mRNA 而不是 m1Ψ-mRNA 的动物中观察到干扰素反应的另外一个细胞簇外,激活水平相似。针对疫苗观察到相似的免疫球蛋白类别转换和体细胞超突变。雌性叙利亚仓鼠通过两剂每种疫苗的初免-加强方案进行免疫。糖蛋白结合抗体的滴度对于 U-mRNA 构建体大于 m1Ψ-mRNA 构建体;然而,中和 ANDV 的抗体滴度相似。接种疫苗的动物用致死剂量的 ANDV 以及一个未接种的对照组进行了挑战。所有对照动物和用较低剂量的 m1Ψ-mRNA 接种的两只动物都因感染而死亡,而其他接种疫苗的动物则存活下来,没有病毒复制的证据。该数据表明开发了针对 ANDV 的保护性疫苗,并且 m1Ψ 修饰对啮齿动物的免疫原性和保护作用没有实质性影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/592e/11289437/1342bf025c79/41467_2024_50774_Fig1_HTML.jpg

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