Detection of Virus-specific T Cells Via ELISpot Corroborates Early Diagnosis in Human Borna Disease Virus 1 (BoDV-1) Encephalitis

Overview

Journal Infection

Date 2024 Apr 12

PMID 38607591

Authors

Markus Bauswein

Ehab Eid

Lisa Eidenschink

Barbara Schmidt

Andre Gessner

Dennis Tappe

Daniel Cadar

Merle M Bohmer

Laura Jockel

Nora van Wickeren

Tamara Garibashvili

Isabel Wiesinger

Christina Wendl

Josef G Heckmann

Klemens Angstwurm

Martin Freyer

Affiliations

Soon will be listed here.

Abstract

Background: Within endemic regions in southern and eastern Germany, Borna disease virus 1 (BoDV-1) causes rare zoonotic spill-over infections in humans, leading to encephalitis with a high case-fatality risk. So far, intra-vitam diagnosis has mainly been based on RT-qPCR from cerebrospinal fluid (CSF) and serology, both being associated with diagnostic challenges. Whilst low RNA copy numbers in CSF limit the sensitivity of RT-qPCR from this material, seroconversion often occurs late during the course of the disease.

Case Presentation: Here, we report the new case of a 40 - 50 year-old patient in whom the detection of virus-specific T cells via ELISpot corroborated the diagnosis of BoDV-1 infection. The patient showed a typical course of the disease with prodromal symptoms like fever and headaches 2.5 weeks prior to hospital admission, required mechanical ventilation from day three after hospitalisation and remained in deep coma until death ten days after admission.

Results: Infection was first detected by positive RT-qPCR from a CSF sample drawn four days after admission (viral load 890 copies/mL). A positive ELISpot result was obtained from peripheral blood collected on day seven, when virus-specific IgG antibodies were not detectable in serum, possibly due to previous immune adsorption for suspected autoimmune-mediated encephalitis.

Conclusion: This case demonstrates that BoDV-1 ELISpot serves as additional diagnostic tool even in the first week after hospitalisation of patients with BoDV-1 encephalitis.

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