Amino acid substitutions in the fusion protein of respiratory syncytial virus in Fukushima, Japan during 2008–2023 and their effects

Hisao Okabe, Koichi Hashimoto, Sakurako Norito, Yuichiro Asano, Masatoki Sato, Yohei Kume, Mina Chishiki, Hajime Maeda, Fumi Mashiyama, Aya Takeyama, Hiromichi Murai, Kenji Nemoto, Masaki Ito, Shigeo Suzuki, Hiroko Sakuma, Kazuya Shirato, Hayato Go, Mitsuaki Hosoya
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Abstract

Background Amino acid (AA) substitutions in the fusion protein of respiratory syncytial virus (RSV) and their effects remain unclear. We aimed to analyze AA substitutions in main neutralizing epitopes of the fusion (F) protein. Methods We analyzed F protein genes of 236 RSV strains isolated from children hospitalized with RSV infection in Fukushima, Japan (June 2008–February 2023). AA substitutions were detected at antigenic sites II, V, and Ø, the main neutralizing epitopes. We conducted neutralization assays using site-specific mAbs to investigate the relationship between AA substitutions and mAb susceptibility. Finally, we examined viral replicative ability. Results Site Ⅱ: RSV strains isolated from children receiving palivizumab treatment exhibited the K272M substitution in RSV-A and K272E substitution in RSV-B, showing reduced susceptibility to site Ⅱ-specific antibody. Site Ⅴ: In RSV-A, >50% of strains isolated since 2022 harbored the V178I substitution; however, this did not change susceptibility to site Ⅴ-specific antibody. In RSV-B, L172Q/S173L mutant strains became predominant around 2016, leading to reduced susceptibility to site Ⅴ-specific antibodies. Site Ø: No AA substitutions were detected in RSV-A. In RSV-B, the I206M/Q209R mutant strain became predominant around 2018, leading to improved site Ø-specific antibody susceptibility and replicative ability. However, none of the substitutions reduced susceptibility to site Ø-specific antibodies. Conclusions The RSV F protein in Fukushima has naturally undergone AA substitutions with corresponding changes in antibody susceptibility. In addition to substitutions similar to those observed globally, unique substitutions have been observed. Therefore, AA substitutions and antibody susceptibility in various regions must be monitored.
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2008-2023年日本福岛呼吸道合胞病毒融合蛋白氨基酸取代及其影响
背景呼吸道合胞病毒(RSV)融合蛋白中氨基酸(AA)的替换及其作用尚不清楚。我们的目的是分析融合蛋白(F)的主要中和表位上的AA取代。方法对2008年6月~ 2023年2月日本福岛住院RSV感染患儿分离的236株RSV蛋白基因进行分析。在主要中和表位抗原位点II、V和Ø上检测到AA取代。我们使用位点特异性单抗进行中和试验,以研究AA取代与单抗敏感性之间的关系。最后,我们检查了病毒的复制能力。结果位点Ⅱ:接受帕利珠单抗治疗的儿童分离的RSV菌株在RSV- a中表现出K272M替代,在RSV- b中表现出K272E替代,对位点Ⅱ特异性抗体的敏感性降低。网站Ⅴ:在RSV-A中,>;自2022年以来分离的菌株中有50%含有V178I替代;然而,这并没有改变位点Ⅴ特异性抗体的易感性。在RSV-B中,L172Q/S173L突变株在2016年左右占优势,导致对Ⅴ特异性抗体的易感性降低。位点Ø: RSV-A未检测到AA替换。在RSV-B中,I206M/Q209R突变株在2018年左右成为优势菌株,导致位点Ø-specific抗体敏感性和复制能力提高。然而,没有一种取代降低了位点Ø-specific抗体的易感性。结论福岛地区RSV F蛋白自然发生了AA取代,抗体敏感性发生相应变化。除了与全球观察到的类似的取代外,还观察到独特的取代。因此,必须监测各个区域的AA取代和抗体敏感性。
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