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流感病毒H2血凝素中的单个残基可增强H2疫苗接种引发的B细胞反应的广度。

A single residue in influenza virus H2 hemagglutinin enhances the breadth of the B cell response elicited by H2 vaccination.

作者信息

Andrews Sarah F, Raab Julie E, Gorman Jason, Gillespie Rebecca A, Cheung Crystal S F, Rawi Reda, Cominsky Lauren Y, Boyington Jeffrey C, Creanga Adrian, Shen Chen-Hsiang, Harris Darcy R, Olia Adam S, Nazzari Alexandra F, Zhou Tongqing, Houser Katherine V, Chen Grace L, Mascola John R, Graham Barney S, Kanekiyo Masaru, Ledgerwood Julie E, Kwong Peter D, McDermott Adrian B

机构信息

Vaccine Research Center, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD, USA.

出版信息

Nat Med. 2022 Feb;28(2):373-382. doi: 10.1038/s41591-021-01636-8. Epub 2022 Feb 3.

Abstract

Conserved epitopes on the influenza hemagglutinin (HA) stem are an attractive target for universal vaccine strategies as they elicit broadly neutralizing antibodies. Such antibody responses to stem-specific epitopes have been extensively characterized for HA subtypes H1 and H5 in humans. H2N2 influenza virus circulated 50 years ago and represents a pandemic threat due to the lack of widespread immunity, but, unlike H1 and H5, the H2 HA stem contains Phe45 predicted to sterically clash with HA stem-binding antibodies characterized to date. To understand the effect of Phe45, we compared the HA stem-specific B cell response in post hoc analyses of two phase 1 clinical trials, one testing vaccination with an H2 ferritin nanoparticle immunogen ( NCT03186781 ) and one with an inactivated H5N1 vaccine ( NCT01086657 ). In H2-naive individuals, the magnitude of the B cell response was equivalent, but H2-elicited HA stem-binding B cells displayed greater cross-reactivity than those elicited by H5. However, in individuals with childhood H2 exposure, H5-elicited HA stem-binding B cells also displayed high cross-reactivity, suggesting recall of memory B cells formed 50 years ago. Overall, we propose that a one-residue difference on an HA immunogen can alter establishment and expansion of broadly neutralizing memory B cells. These data have implications for stem-based universal influenza vaccination strategies.

摘要

流感血凝素(HA)茎部的保守表位是通用疫苗策略的一个有吸引力的靶点,因为它们能引发广泛中和抗体。人类对HA亚型H1和H5中茎部特异性表位的此类抗体反应已得到广泛表征。H2N2流感病毒在50年前传播,由于缺乏广泛免疫力而构成大流行威胁,但与H1和H5不同的是,H2 HA茎部含有苯丙氨酸45,预计会与迄今已表征的HA茎部结合抗体发生空间冲突。为了解苯丙氨酸45的作用,我们在两项1期临床试验的事后分析中比较了HA茎部特异性B细胞反应,一项试验用H2铁蛋白纳米颗粒免疫原进行疫苗接种(NCT03186781),另一项试验用灭活H5N1疫苗进行接种(NCT01086657)。在未接触过H2的个体中,B细胞反应的强度相当,但H2引发的HA茎部结合B细胞比H5引发的B细胞表现出更大的交叉反应性。然而,在儿童期接触过H2的个体中,H5引发的HA茎部结合B细胞也表现出高交叉反应性,表明对50年前形成的记忆B细胞有回忆反应。总体而言,我们提出HA免疫原上一个残基的差异可改变广泛中和记忆B细胞的建立和扩增。这些数据对基于茎部的通用流感疫苗接种策略有启示意义。

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