Literature DB >> 27001363

Treatment of blood with a pathogen reduction technology using ultraviolet light and riboflavin inactivates Ebola virus in vitro.

Andrew P Cap1, Heather F Pidcoke1, Shawn D Keil2, Hilary M Staples3, Manu Anantpadma3, Ricardo Carrion3, Robert A Davey3, Ashley Frazer-Abel4, Audra L Taylor5, Richard Gonzales2,5, Jean L Patterson3, Raymond P Goodrich2.   

Abstract

BACKGROUND: Transfusion of plasma from recovered patients after Ebolavirus (EBOV) infection, typically called "convalescent plasma," is an effective treatment for active disease available in endemic areas, but carries the risk of introducing other pathogens, including other strains of EBOV. A pathogen reduction technology using ultraviolet light and riboflavin (UV+RB) is effective against multiple enveloped, negative-sense, single-stranded RNA viruses that are similar in structure to EBOV. We hypothesized that UV+RB is effective against EBOV in blood products without activating complement or reducing protective immunoglobulin titers that are important for the treatment of Ebola virus disease (EVD). STUDY DESIGN AND METHODS: Four in vitro experiments were conducted to evaluate effects of UV+RB on green fluorescent protein EBOV (EBOV-GFP), wild-type EBOV in serum, and whole blood, respectively, and on immunoglobulins and complement in plasma. Initial titers for Experiments 1 to 3 were 4.21 log GFP units/mL, 4.96 log infectious units/mL, and 4.23 log plaque-forming units/mL. Conditions tested in the first three experiments included the following: 1-EBOV-GFP plus UV+RB; 2-EBOV-GFP plus RB only; 3-EBOV-GFP plus UV only; 4-EBOV-GFP without RB or UV; 5-virus-free control plus UV only; and 6-virus-free control without RB or UV.
RESULTS: UV+RB reduced EBOV titers to nondetectable levels in both nonhuman primate serum (≥2.8- to 3.2-log reduction) and human whole blood (≥3.0-log reduction) without decreasing protective antibody titers in human plasma.
CONCLUSION: Our in vitro results demonstrate that the UV+RB treatment efficiently reduces EBOV titers to below limits of detection in both serum and whole blood. In vivo testing to determine whether UV+RB can improve convalescent blood product safety is indicated.
© 2016 AABB.

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Year:  2016        PMID: 27001363      PMCID: PMC5943045          DOI: 10.1111/trf.13393

Source DB:  PubMed          Journal:  Transfusion        ISSN: 0041-1132            Impact factor:   3.157


  32 in total

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2.  Infection of UV-irradiated xeroderma pigmentosum fibroblasts by herpes simplex virus: study of capacity and Weigle reactivation.

Authors:  C D Lytle; R S Day; K B Hellman; L E Bockstahler
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3.  Establishment of culture systems for Genotypes 3 and 4 hepatitis E virus (HEV) obtained from human blood and application of HEV inactivation using a pathogen reduction technology system.

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4.  Immunochemical quantitation of antigens by single radial immunodiffusion.

Authors:  G Mancini; A O Carbonara; J F Heremans
Journal:  Immunochemistry       Date:  1965-09

5.  U.V. enhanced reactivation of U.V.-and gamma-irradiated adenovirus in normal human fibroblasts.

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6.  Inactivation of Orientia tsutsugamushi in red blood cells, plasma, and platelets with riboflavin and light, as demonstrated in an animal model.

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7.  Radiation enhanced reactivation of herpes simplex virus: effect of caffeine.

Authors:  K B Hellman; C D Lytle; L E Bockstahler
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8.  Transfusion-transmitted malaria in Ghana.

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  14 in total

1.  Reduced MHC alloimmunization and partial tolerance protection with pathogen reduction of whole blood.

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2.  Pathogen reduction of blood components during outbreaks of infectious diseases in the European Union: an expert opinion from the European Centre for Disease Prevention and Control consultation meeting.

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Journal:  Blood Transfus       Date:  2019-12-11       Impact factor: 3.443

3.  Haemostatic function measured by thromboelastography and metabolic activity of platelets treated with riboflavin and UV light.

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4.  Preservation of neutralizing antibody function in COVID-19 convalescent plasma treated using a riboflavin and ultraviolet light-based pathogen reduction technology.

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5.  Disinfection of Ebola Virus in Sterilized Municipal Wastewater.

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Review 6.  Pathogen reduction/inactivation of products for the treatment of bleeding disorders: what are the processes and what should we say to patients?

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7.  Proceedings of the Food and Drug Administration public workshop on pathogen reduction technologies for blood safety 2018 (Commentary, p. 3026).

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Journal:  Transfusion       Date:  2019-05-29       Impact factor: 3.157

Review 8.  Laboratory management of Crimean-Congo haemorrhagic fever virus infections: perspectives from two European networks.

Authors:  Barbara Bartolini; Cesare Em Gruber; Marion Koopmans; Tatjana Avšič; Sylvia Bino; Iva Christova; Roland Grunow; Roger Hewson; Gulay Korukluoglu; Cinthia Menel Lemos; Ali Mirazimi; Anna Papa; Maria Paz Sanchez-Seco; Aisha V Sauer; Hervè Zeller; Carla Nisii; Maria Rosaria Capobianchi; Giuseppe Ippolito; Chantal B Reusken; Antonino Di Caro
Journal:  Euro Surveill       Date:  2019-01

Review 9.  Treatment for emerging viruses: Convalescent plasma and COVID-19.

Authors:  Bethany L Brown; Jeffrey McCullough
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Review 10.  The Role of the Laboratory and Transfusion Service in the Management of Ebola Virus Disease.

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