ArXiv TLDR

Shared quasispecies architecture in experimental and natural RNA virus populations

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2605.13535

Samuel Martínez-Alcalá, Iker Atienza-Diez, Pilar Somovilla, Brenda Martínez-González, Celia Perales + 3 more

q-bio.PE

TLDR

RNA viruses, despite diverse contexts, exhibit a shared hierarchical genotype network architecture, offering insights into predictable evolutionary patterns.

Key contributions

  • Compares genotype network architectures of bacteriophage Qβ and SARS-CoV-2.
  • Reconstructs mutationally coupled variant networks using deep sequencing data.
  • Reveals a common hierarchical structure: central haplotype with diminishing variant abundance.
  • Suggests a fundamental, shared genotype network architecture across RNA viruses.

Why it matters

This work introduces genotype networks as a unifying framework to describe viral population structure beyond conventional diversity measures. It reveals how local constraints shape mutational search, offering crucial insights into the predictability of viral evolution. Understanding this robust, shared architecture can inform strategies against viral adaptation.

Original Abstract

RNA viruses form genetically diverse populations structured as mutant spectra, or quasispecies, whose internal organization influences their evolutionary and adaptive dynamics. While genetic diversity has been extensively characterized, the structural organization of viral populations in sequence space remains less explored. Here, we compare genotype network architectures in two RNA viruses with markedly different evolutionary contexts: bacteriophage $Qβ$ evolving in controlled laboratory conditions and SARS-CoV-2 evolving within infected human hosts. Using deep sequencing data, we reconstruct the genotype network of mutationally coupled variants within viral populations and analyze their topological properties. Despite large differences in genome size, mutation rate, and ecological setting, both viruses exhibit a common organization: a highly abundant central haplotype surrounded by layers of variants of diminishing abundance as Hamming distance to the central haplotype increases. All reconstructed networks share qualitative and quantitative topological features, displaying a hierarchical structure. The robust organization of both populations under multiple conditions suggests that RNA viruses may share a common genotype network architecture governed by fundamental properties of sequence space and the generic mechanisms of replication and mutation. Genotype networks provide a unifying framework to describe viral population structure beyond conventional diversity measures and, by revealing how local constraints shape mutational search, offers insights into the predictability of viral evolution.

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