Ebola virus persistence and disease recrudescence in the brains of antibody-treated nonhuman primate survivors

脉络丛 猕猴 恒河猴 埃博拉病毒 医学 免疫学 病理 病毒学 疾病 生物 中枢神经系统 内科学 神经科学
作者
Jun Liu,John C. Trefry,April M. Babka,Christopher W. Schellhase,Kayla M. Coffin,Janice A. Williams,Jo Lynne Raymond,Paul R. Facemire,Taylor Chance,Neil M. Davis,Jennifer L. Scruggs,Franco Rossi,Andrew D. Haddow,Justine M. Zelko,Sandra L. Bixler,Ian Crozier,Patrick L. Iversen,M. Louise M. Pitt,Jens H. Kuhn,Gustavo Palacios
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:14 (631): eabi5229-eabi5229 被引量:49
标识
DOI:10.1126/scitranslmed.abi5229
摘要

Effective therapeutics have been developed against acute Ebola virus disease (EVD) in both humans and experimentally infected nonhuman primates. However, the risk of viral persistence and associated disease recrudescence in survivors receiving these therapeutics remains unclear. In contrast to rhesus macaques that survived Ebola virus (EBOV) exposure in the absence of treatment, we discovered that EBOV, despite being cleared from all other organs, persisted in the brain ventricular system of rhesus macaque survivors that had received monoclonal antibody (mAb) treatment. In mAb-treated macaque survivors, EBOV persisted in macrophages infiltrating the brain ventricular system, including the choroid plexuses. This macrophage infiltration was accompanied by severe tissue damage, including ventriculitis, choroid plexitis, and meningoencephalitis. Specifically, choroid plexus endothelium-derived EBOV infection led to viral persistence in the macaque brain ventricular system. This resulted in apoptosis of ependymal cells, which constitute the blood-cerebrospinal fluid barrier of the choroid plexuses. Fatal brain-confined recrudescence of EBOV infection manifested as severe inflammation, local pathology, and widespread infection of the ventricular system and adjacent neuropil in some of the mAb-treated macaque survivors. This study highlights organ-specific EBOV persistence and fatal recrudescent disease in rhesus macaque survivors after therapeutic treatment and has implications for the long-term follow-up of human survivors of EVD.
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