# Internal gene segments from a mouse-adapted influenza B virus confer increased pathogenicity to mice

**Authors:** Arne Matthys, Laura Amelinck, Anouk Smet, Tine Ysenbaert, Thorsten U. Vogel, Xavier Saelens, João Paulo Portela Catani, Victor Huber, Victor Huber, Victor Huber

PMC · DOI: 10.1371/journal.pone.0335324 · PLOS One · 2026-03-23

## TL;DR

Researchers created a mouse-adapted influenza B virus that is more pathogenic in mice, offering a new tool for studying IBV in animal models.

## Contribution

A novel mouse-adapted IBV backbone was developed that increases pathogenicity in mice.

## Key findings

- Mutations in the M, PA, and PB1 gene segments contributed to increased pathogenicity in mice.
- Reassortant viruses using the new backbone showed higher pathogenicity in BALB/c mice.
- Non-synonymous mutations in five gene segments were acquired during serial passage.

## Abstract

Influenza B viruses (IBVs) contribute significantly to the annual influenza epidemics in human. Most IBV strains are non- or poorly pathogenic in mice, which are frequently used for vaccine studies. We describe the generation of a mouse-adapted IBV strain that retains pathogenicity in mice when carrying hemagglutinin (HA) and neuraminidase (NA) gene segments from a heterologous IBV strain. Serial passage of an influenza B reassortant virus, containing the HA and NA segments from B/Washington/02/2019 on a mouse-adapted B/Memphis/12/1997 backbone, resulted in the selection of an IBV that was highly pathogenic for mice. This mouse-adapted IBV strain had acquired non-synonymous mutations in 5 gene segments. Sequence analysis of the intermediate passages indicated that mutations in the matrix (M), polymerase acidic (PA), and polymerase basic 1 (PB1) gene segments appeared at passages 9 and 13, suggesting that these mutations contributed to the pathogenicity in mice. Mouse challenge studies with rescued reassortant viruses with one or multiple mutated gene segments, confirmed the importance of substitutions in the M and PA segments for pathogenicity. Using the novel mouse-adapted IBV backbone, we rescued reassortant viruses containing the HA and NA segments of B/Austria/1359417/2021 and demonstrated its increased pathogenicity in BALB/c mice compared to IBV rescued on the parental strain. This mouse-adapted IBV backbone provides a valuable tool for the study of IBV in mice.

## Linked entities

- **Genes:** ha (hair bristles) [NCBI Gene 251217], XK (X-linked Kx blood group antigen, Kell and VPS13A binding protein) [NCBI Gene 7504], m (miniature) [NCBI Gene 44835], AMY2A (amylase alpha 2A) [NCBI Gene 279], SMR3A (submaxillary gland androgen regulated protein 3A) [NCBI Gene 26952]
- **Diseases:** influenza (MONDO:0005812)
- **Species:** Mus musculus (taxon 10090), Homo sapiens (taxon 9606)

## Full-text entities

- **Genes:** Adgrg3 (adhesion G protein-coupled receptor G3) [NCBI Gene 54672] {aka A030001G24Rik, Gpr97, Pb1, Pb99}, Gnl3 (guanine nucleotide binding protein nucleolar 3) [NCBI Gene 30877] {aka Ns}, Npm1 (nucleophosmin 1) [NCBI Gene 18148] {aka B23, NO38, Npm}, Ivns1abp (influenza virus NS1A binding protein) [NCBI Gene 117198] {aka 1190004M08Rik, 1700126I16Rik, HSPC068, ND1, NS-1, NS1-BP}
- **Diseases:** infected (MESH:D007239), viral infection (MESH:D014777), dislocation (MESH:D004204), deaths (MESH:D003643), pneumonia (MESH:D011014), Weight loss (MESH:D015431), influenza (MESH:D007251)
- **Chemicals:** 5Amino acid (-), isoflurane (MESH:D007530), PBS (MESH:D007854), B (MESH:D001895), TPCK (MESH:D014108)
- **Species:** Mus musculus (house mouse, species) [taxon 10090], H3N2 subtype (serotype) [taxon 119210], H1N1 subtype (serotype) [taxon 114727], Homo sapiens (human, species) [taxon 9606], Orthomyxoviridae (family) [taxon 11308], Influenza B virus (no rank) [taxon 11520], Hepatovirus A (no rank) [taxon 12092]
- **Mutations:** V379I, G to R, 1465 (AAA to GAA, D424G, K338R, I to M, K to E, T214I, 1938 (TTG to TTA, 1135 (GTA to ATA, T211A, K to R, 961 (GAG to AAG, G136R, 2171 (AAG to AGG, I to L, 481 (GGA to AGA, E48K, K489E, 1929 (TTG to TTA, N221S, 2134 (AGG to AGA, V to I, methionine at position 390, 937 (ATA to CTA, 1170 (ATA to ATG, 2180 (A to G, 421 (GGA to AGA, 1345 (GAG to AGA, 645 (T to A, 411 (TAC to TAT, 1952 (ACC to GCC, I390M, E to K, D432N, M390I, 31474 (TGT to TAT, G148R
- **Cell lines:** MDCK — Canis lupus familiaris (Dog), Spontaneously immortalized cell line (CVCL_0422), /2J — Homo sapiens (Human), Transformed cell line (CVCL_N185), DBA/2J — Mus musculus (Mouse), Finite cell line (CVCL_6496), /c — Mus musculus (Mouse), Hepatocellular carcinoma of the mouse, Cancer cell line (CVCL_9103), BALB/c — Mus musculus (Mouse), Spontaneously immortalized cell line (CVCL_0184), HEK — Homo sapiens (Human), Transformed cell line (CVCL_0045)

## Full text

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## Figures

5 figures with captions in the complete paper: https://tomesphere.com/paper/PMC13008076/full.md

## References

28 references — full list in the complete paper: https://tomesphere.com/paper/PMC13008076/full.md

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Source: https://tomesphere.com/paper/PMC13008076