Exploring a prolonged enterovirus C104 infection in a severely ill patient using nanopore sequencing

Hayley Cassidy; Leonard Schuele; Erley Lizarazo-Forero; Natacha Couto; John W A Rossen; Alex W Friedrich; Coretta van Leer-Buter; Hubert G M Niesters

doi:10.1093/ve/veab109

Exploring a prolonged enterovirus C104 infection in a severely ill patient using nanopore sequencing

Virus Evol. 2022 Mar 18;8(1):veab109. doi: 10.1093/ve/veab109. eCollection 2022.

Authors

Hayley Cassidy, Leonard Schuele¹, Erley Lizarazo-Forero¹, Natacha Couto¹, John W A Rossen¹, Alex W Friedrich¹, Coretta van Leer-Buter¹, Hubert G M Niesters¹

Affiliation

¹ Department of Medical Microbiology and Infection Prevention, University of Groningen, University Medical Center Groningen, Hanzeplein 1, Groningen 9713 GZ, The Netherlands.

Abstract

Chronic enterovirus infections can cause significant morbidity, particularly in immunocompromised patients. This study describes a fatal case associated with a chronic untypeable enterovirus infection in an immunocompromised patient admitted to a Dutch university hospital over nine months. We aimed to identify the enterovirus genotype responsible for the infection and to determine potential evolutionary changes. Long-read sequencing was performed using viral targeted sequence capture on four respiratory and one faecal sample. Phylogenetic analysis was performed using a maximum likelihood method, along with a root-to-tip regression and time-scaled phylogenetic analysis to estimate evolutionary changes between sample dates. Intra-host variant detection, using a Fixed Ploidy algorithm, and selection pressure, using a Fixed Effect Likelihood and a Mixed Effects Model of Evolution, were also used to explore the patient samples. Near-complete genomes of enterovirus C104 (EV-C104) were recovered in all respiratory samples but not in the faecal sample. The recovered genomes clustered with a recently reported EV-C104 from Belgium in August 2018. Phylodynamic analysis including ten available EV-C104 genomes, along with the patient sequences, estimated the most recent common ancestor to occur in the middle of 2005 with an overall estimated evolution rate of 2.97 × 10^-3 substitutions per year. Although positive selection pressure was identified in the EV-C104 reference sequences, the genomes recovered from the patient samples alone showed an overall negative selection pressure in multiple codon sites along the genome. A chronic infection resulting in respiratory failure from a relatively rare enterovirus was observed in a transplant recipient. We observed an increase in single-nucleotide variations between sample dates from a rapidly declining patient, suggesting mutations are weakly deleterious and have not been purged during selection. This is further supported by the persistence of EV-C104 in the patient, despite the clearance of other viral infections. Next-generation sequencing with viral enrichment could be used to detect and characterise challenging samples when conventional workflows are insufficient.

Keywords: chronic infection; enterovirus; immunocompromised; intra-host evolution; nanopore sequencing; virus evolution.