Combination therapy with remdesivir and monoclonal antibodies protects nonhuman primates against advanced Sudan virus disease
Robert W. Cross, Zachary A. Bornholdt, Abhishek N. Prasad, Courtney Woolsey, Viktoriya Borisevich, Krystle N. Agans, Daniel J. Deer, Dafna M. Abelson, Do H. Kim, William S. Shestowsky, Lioudmila A. Campbell, Elaine Bunyan, Joan B. Geisbert, Natalie S. Dobias, Karla A. Fenton, Danielle P. Porter, Larry Zeitlin, Thomas W. Geisbert
Robert W. Cross, Zachary A. Bornholdt, Abhishek N. Prasad, Courtney Woolsey, Viktoriya Borisevich, Krystle N. Agans, Daniel J. Deer, Dafna M. Abelson, Do H. Kim, William S. Shestowsky, Lioudmila A. Campbell, Elaine Bunyan, Joan B. Geisbert, Natalie S. Dobias, Karla A. Fenton, Danielle P. Porter, Larry Zeitlin, Thomas W. Geisbert
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Research Article Virology

Combination therapy with remdesivir and monoclonal antibodies protects nonhuman primates against advanced Sudan virus disease

Abstract

A major challenge in managing acute viral infections is ameliorating disease when treatment is delayed. Previously, we reported the success of a 2-pronged mAb and antiviral remdesivir therapeutic approach to treat advanced illness in rhesus monkeys infected with Marburg virus (MARV). Here, we explored the benefit of a similar combination therapy for Sudan ebolavirus (Sudan virus; SUDV) infection. Importantly, no licensed anti-SUDV therapeutics currently exist, and infection of rhesus macaques with SUDV results in a rapid disease course similar to MARV with a mean time to death of 8.3 days. When initiation of therapy with either remdesivir or a pan-ebolavirus mAb cocktail (MBP431) was delayed until 6 days after inoculation, only 20% of macaques survived. In contrast, when remdesivir and MBP431 treatment were combined beginning 6 days after inoculation, significant protection (80%) was achieved. Our results suggest that combination therapy may be a viable treatment for patients with advanced filovirus disease that warrants further clinical testing in future outbreaks.

Authors

Robert W. Cross, Zachary A. Bornholdt, Abhishek N. Prasad, Courtney Woolsey, Viktoriya Borisevich, Krystle N. Agans, Daniel J. Deer, Dafna M. Abelson, Do H. Kim, William S. Shestowsky, Lioudmila A. Campbell, Elaine Bunyan, Joan B. Geisbert, Natalie S. Dobias, Karla A. Fenton, Danielle P. Porter, Larry Zeitlin, Thomas W. Geisbert

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Figure 4

Pathology of the liver, spleen, and lung of SUDV-challenged rhesus macaques that succumbed at 9–12 dpi.

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Pathology of the liver, spleen, and lung of SUDV-challenged rhesus macaq...
Representative photomicrographs of IHC at 20× original magnification for SUDV VP40 antigen (brown) in the liver (A, E, I, and M), spleen (B, F, J, and N), and lung (C, G, K, O). IHC positivity for rare Kupffer cells/mononuclear cells (black arrows) in the liver of D5-RDV-1 (A), small clusters in D6-RDV-3 (E) and D6-MBP-3 (I), and moderate clusters in D6-COMB-5 (M). IHC positivity for scattered mononuclear cells within the red and white pulp of the spleen for D5-RDV-1 (B), rarely the white pulp (black arrow) and red pulp (white arrow) D6-RDV-3 (F), and moderately in D6-COMB-5 (N). No appreciable immunolabeling was present in the spleen of D6-MBP-3 (J). Mononuclear cells had IHC positivity within clustered/nodular lesions of the lung of D5-RDV-1 (C, arrows), D6-RDV-3 (G, arrow), D6-MBP-3 (K, arrow), and D6-COMB-5 (O). Multifocal raised white nodules consistent with pneumonia on histology were present in D6-COMB-5 at gross examination (D). Representative positive ISH (red) at 20× original magnification of pulmonary nodules for D6-RDV-3 (H), D6-MBP-3 (L), and D6-COMB-5 (P).