Plasma transfusion–transmission of Zika virus in mice and macaques

Author:

Van Rompay Koen K. A.12,Coffey Lark L.2,Yee JoAnn L.1,Singapuri Anil2,Stuart Jackson2,Lanteri Marion C.3ORCID,Santa Maria Felicia3,Lu Kai4,Singh Inderdeep4,Bakkour Sonia4ORCID,Stone Mars45,Williamson Phillip C.6,Muench Marcus O.45ORCID,Busch Michael P.45,Simmons Graham45ORCID

Affiliation:

1. California National Primate Research Center University of California Davis California USA

2. Department of Pathology, Microbiology and Immunology University of California Davis California USA

3. Cerus Corporation Concord California USA

4. Vitalant Research Institute San Francisco California USA

5. Department of Laboratory Medicine University of California San Francisco San Francisco California USA

6. Creative Testing Solutions Tempe Arizona USA

Abstract

AbstractBackgroundZika virus (ZIKV) epidemics with infections in pregnant women are associated with severe neurological disease in newborns. Although an arbovirus, ZIKV is also blood transfusion‐transmitted (TT). Greater knowledge of the efficiency of ZIKV TT would aid decisions on testing and pathogen reduction technologies (PRT).Study Design and MethodsPlasma units from ZIKV RNA‐reactive blood donors were used to study infectivity in vitro, in mice, and in macaques. Furthermore, plasma units were subjected to PRT using amotosalen/ultraviolet light A (A/UVA) before transfusion.ResultsIn vitro infectivity of ZIKV RNA‐reactive plasma varied between 100 and 1000 international units (IU) of ZIKV RNA. Immunodeficient mice were more sensitive with as low as 32 IU sufficient to infect 50% of mice. 50–5500 IU of RNA led to TT in macaques using dose escalation of three different RNA‐positive, seronegative plasma units. In contrast, RNA‐reactive units collected postseroconversion were not infectious in macaques, even at a dose of 9 million IU RNA. After A/UVA PRT, transfusion of plasma containing up to 18 million IU was no longer infectious in vitro and did not result in ZIKV TT in macaques.ConclusionSignificant risks of ZIKV TT are likely confined to a relatively short viremic window before seroconversion, and that sensitive nucleic acid amplification testing likely identifies the majority of infectious plasma. PRT was demonstrated to be effective at preventing ZIKV TT. Considering that there is no approved ZIKV vaccine, these data are relevant to mitigate the risk of TT during the future ZIKV outbreaks.

Publisher

Wiley

Subject

Hematology,Immunology,Immunology and Allergy

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