Inactivation and Removal of Chikungunya Virus and Mayaro Virus from Plasma-derived Medicinal Products

Yue, Constanze; Teitz, Sebastian; Miyabashi, Tomoyuki; Boller, Klaus; Lewis-Ximenez, Lia Laura; Baylis, Sally A.; Blümel, Johannes

doi:10.3390/v11030234

Cited by 13 publications

(18 citation statements)

References 45 publications

(50 reference statements)

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“…Viral inactivation occurs when the proteins on the surface of the particle change shape, and as a result, lose their ability to function properly, removing their ability to infect cells (Keller et al 2018;Snyder et al 2019;Whitehurst et al 2007). Understanding viral inactivation is important for determining transmission of viruses (Yue et al 2019;Pinon and Vialette 2018;Predmore et al 2015), but also plays a role in vaccine development (Dumard et al 2017;Silva et al 2015).…”

Section: Introductionmentioning

confidence: 99%

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Energy Requirements for Loss of Viral Infectivity

Rowell

Dobrovolny

2020

Food Environ Virol

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Outside the host, viruses will eventually lose their ability to infect cells due to conformational changes that occur to proteins on the viral capsid. In order to undergo a conformational change, these proteins require energy to activate the chemical reaction that leads to the conformational change. In this study, data from the literature is used to calculate the energy required for viral inactivation for a variety of different viruses by means of the Arrhenius equation. We find that some viruses (rhinovirus, poliovirus, human immunodeficiency virus, Alkhumra hemorrhagic fever virus, and hepatitis A virus) have high inactivation energies, indicative of breaking of a chemical double bond. We also find that several viruses (respiratory syncytial virus, poliovirus, and norovirus) have nonlinear Arrhenius plots, suggesting that there is more than a single pathway for inactivation of these viruses.

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Section: Introductionmentioning

confidence: 99%

“…Understanding viral inactivation is important for determining transmission of viruses (Yue et al. 2019 ; Pinon and Vialette 2018 ; Predmore et al. 2015 ), but also plays a role in vaccine development (Dumard et al.…”

Section: Introductionmentioning

confidence: 99%

Energy Requirements for Loss of Viral Infectivity

Rowell

Dobrovolny

2020

Food Environ Virol

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“…The time of pasteurization is critical for efficient inactivation of virus particles, e.g., 4 h pasteurization may not be sufficient to inactivate hepatitis B viruses as opposed to a 10 h treatment [12]. While the method has been widely accepted in manufacturing of HSA in industry, the emergence of new viruses, e.g., Zika virus and Chikungunya virus, stipulates constant revalidation of the process [13][14][15][16][17]. Pasteurization of HSA (60 • C, 10 h) was shown to reduce the infectivity of most known human viruses including human parvovirus B19, hepatitis A virus, human immunodeficiency virus and West Nile virus [18][19][20][21], but it may be ineffective against animal parvoviruses, e.g., canine parvovirus (CPV) and minute virus of mice (MVM) [21].…”

Section: Introductionmentioning

confidence: 99%

Aggregate Removal Nanofiltration of Human Serum Albumin Solution Using Nanocellulose-Based Filter Paper

Mantas

Gustafsson

et al. 2020

Biomedicines

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This study is dedicated to the rapid removal of protein aggregates and viruses from plasma-derived human serum albumin (HSA) product to reduce the risk of viral contamination and increase biosafety. A two-step filtration approach was implemented to first remove HSA aggregates and then achieve high model virus clearance using a nanocellulose-based filter paper of different thicknesses, i.e., 11 μm (prefilter) and 22 μm (virus filter) at pH 7.4 and room temperature. The pore size distribution of these filters was characterized by nitrogen gas sorption analysis. Dynamic light scattering (DLS) and size-exclusion high performance liquid chromatography (SE-HPLC) were performed to analyze the presence of HSA aggregates in process intermediates. The virus filter showed high clearance of a small-size model virus, i.e., log10 reduction value (LRV) > 5, when operated at 3 and 5 bar, but a distinct decrease in LRV was detected at 1 bar, i.e., LRV 2.65–3.75. The throughput of HSA was also dependent on applied transmembrane pressure as was seen by Vmax values of 110 ± 2.5 L m−2 and 63.6 ± 5.8 L m−2 at 3 bar and 5 bar, respectively. Protein loss was low, i.e., recovery > 90%. A distribution of pore sizes between 40 nm and 60 nm, which was present in the prefilter and absent in the virus filter, played a crucial part in removing the HSA aggregates and minimizing the risk of virus filter fouling. The presented results enable the application of virus removal nanofiltration of HSA in bioprocessing as an alternative to virus inactivation methods based, e.g., on heat treatment.

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“…Thus, phylogenetic and epidemiological studies, clinical diagnostics, vaccine/antiviral drug development, basic research including virus-vector interaction, transmission, viral immunity, and pathogenesis are still necessary for alphaviral disease prevention. In this special issue of “Chikungunya Virus and (Re-) Emerging Alphaviruses”, we solicit 10 research articles and six review articles covering the development of vaccines and antivirals [1,2,3,4], pathogenesis/immunity [5,6,7,8], viral evolution [9], development of research/diagnostic tools [10,11], vector-virus interaction [12,13], as well as mechanisms of transmission [14].…”

mentioning

confidence: 99%

“…As alphaviruses are blood-borne and could be transmitted by blood transfusion, they pose severe safety concerns for plasma-derived medicinal products (PDMPs) in the epidemic countries. Yue et al have described methods to inactivate/remove the CHIKV and the Mayaro virus (MAYV) from PDMPs [4]. These methods could also be a useful guide for the preparation of inactivated virus vaccines.…”

mentioning

confidence: 99%