Structural Characterization of Protective Non-Neutralizing Antibodies targeting Crimean-Congo Hemorrhagic Fever Virus

Author:

Durie Ian1,Tehrani Zahra2,Karaaslan Elif3,Sorvillo Teresa4,McGuire Jack5,Golden Joseph6ORCID,Welch Stephen4ORCID,Kainulainen Markus4ORCID,Harmon Jessica4ORCID,Mousa Jarrod1ORCID,Gonzalez David5,Enos Suzanne1,Koksal Iftihar7,Yilmaz Gurdal8,Karakoc Hanife9,Hamidi Sanaz8,Albay Cansu8,Spengler Jessica4ORCID,Spiropoulou Christina4,Garrison Aura6ORCID,Sajadi Mohammad2,Bergeron Éric4ORCID,Pegan Scott5ORCID

Affiliation:

1. University of Georgia

2. University of Maryland School of Medicine

3. University of California Riverside; Centers for Disease Control and Prevention

4. Centers for Disease Control and Prevention

5. University of California Riverside

6. USAMRIID

7. Acibadem University Atakent Hospital

8. Karadeniz Technical University School of Medicine

9. Bitlis State Hospital

Abstract

Abstract Crimean-Congo Hemorrhagic Fever Virus (CCHFV) causes a life-threatening disease with up to a 40% mortality rate. With no approved medical countermeasures, CCHFV is considered a public health priority agent. The non-neutralizing mouse monoclonal antibody (mAb) 13G8 targets CCHFV glycoprotein GP38 and protects mice from lethal CCHFV challenge when administered prophylactically or therapeutically. Here, we reveal the structures of GP38 bound with a human chimeric 13G8 mAb and a newly isolated CC5-17 mAb from a human survivor. These mAbs bind overlapping epitopes with a shifted angle. The broad-spectrum potential of c13G8 and CC5-17 and the practicality of using them against Aigai virus, a closely related nairovirus were examined. Binding studies demonstrate that the presence of non-conserved amino acids in Aigai virus corresponding region prevent CCHFV mAbs from binding Aigai virus GP38. This information, coupled with in vivo efficacy, paves the way for future mAb therapeutics effective against a wide swath of CCHFV strains.

Publisher

Research Square Platform LLC

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