Virological Characteristics of the SARS-CoV-2 BA.2.86 Variant

Overview

Journal Cell Host Microbe

Publisher Cell Press

Specialties Infectious Diseases
Microbiology

Date 2024 Jan 27

PMID 38280382

Authors

Tomokazu Tamura

Keita Mizuma

Hesham Nasser

Sayaka Deguchi

Miguel Padilla-Blanco

Yoshitaka Oda

Keiya Uriu

Jarel E M Tolentino

Shuhei Tsujino

Rigel Suzuki

Isshu Kojima

Naganori Nao

Ryo Shimizu

Lei Wang

Masumi Tsuda

Michael Jonathan

Yusuke Kosugi

Ziyi Guo

Alfredo A Hinay Jr

Olivia Putri

Yoonjin Kim

Yuri L Tanaka

Hiroyuki Asakura

Mami Nagashima

Kenji Sadamasu

Kazuhisa Yoshimura

Akatsuki Saito

Jumpei Ito

Takashi Irie

Shinya Tanaka

Jiri Zahradnik

Terumasa Ikeda

Kazuo Takayama

Keita Matsuno

Takasuke Fukuhara

Kei Sato

Affiliations

Soon will be listed here.

Abstract

In late 2023, several SARS-CoV-2 XBB descendants, notably EG.5.1, were predominant worldwide. However, a distinct SARS-CoV-2 lineage, the BA.2.86 variant, also emerged. BA.2.86 is phylogenetically distinct from other Omicron sublineages, accumulating over 30 amino acid mutations in its spike protein. Here, we examined the virological characteristics of the BA.2.86 variant. Our epidemic dynamics modeling suggested that the relative reproduction number of BA.2.86 is significantly higher than that of EG.5.1. Additionally, four clinically available antivirals were effective against BA.2.86. Although the fusogenicity of BA.2.86 spike is similar to that of the parental BA.2 spike, the intrinsic pathogenicity of BA.2.86 in hamsters was significantly lower than that of BA.2. Since the growth kinetics of BA.2.86 are significantly lower than those of BA.2 both in vitro and in vivo, the attenuated pathogenicity of BA.2.86 is likely due to its decreased replication capacity. These findings uncover the features of BA.2.86, providing insights for control and treatment.

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