Structural and Functional Characterization of Anti-A33 Antibodies Reveal a Potent Cross-Species Orthopoxviruses Neutralizer

Matho, Michael H.; Schlossman, Andrew; Meng, Xiangzhi; Benhnia, Mohammed Rafii‐El‐Idrissi; Kaever, Thomas; Buller, Mark; Doronin, Konstantin; Parker, Scott; Peters, Bjoern; Crotty, Shane; Xiang, Yan; Zajonc, Dirk M.

doi:10.1371/journal.ppat.1005148

Cited by 38 publications

(40 citation statements)

References 71 publications

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“…1). Восемь белков (H3, B5, D8, L1, A17, A27, A28 и A33) к настоящему времени выявлены как антигены, индуцирующие продукцию вируснейтрализующих антител [8,25,[27][28][29]. Участие других вирусных антигенов в развитии протективного иммунного ответа пока недостаточно изучено.…”

Section: антитела синтезируемые в ответ на Vacv вакцинациюunclassified

Genes that control vaccinia virus immunogenicity

Shchelkunov

Shchelkunova

2020

Acta Naturae

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The live smallpox vaccine was a historical first and highly effective vaccine. However, along with high immunogenicity, the vaccinia virus (VACV) caused serious side effects in vaccinees, sometimes with lethal outcomes. Therefore, after global eradication of smallpox, VACV vaccination was stopped. For this reason, most of the human population worldwide lacks specific immunity against not only smallpox, but also other zoonotic orthopoxviruses. Outbreaks of diseases caused by these viruses have increasingly occurred in humans on different continents. However, use of the classical live VACV vaccine for prevention against these diseases is unacceptable because of potential serious side effects, especially in individuals with suppressed immunity or immunodeficiency (e.g., HIV-infected patients). Therefore, highly attenuated VACV variants that preserve their immunogenicity are needed. This review discusses current ideas about the development of a humoral and cellular immune response to orthopoxvirus infection/vaccination and describes genetic engineering approaches that could be utilized to generate safe and highly immunogenic live VACV vaccines.

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Section: антитела синтезируемые в ответ на Vacv вакцинациюunclassified

Genes that control vaccinia virus immunogenicity

Shchelkunov

Shchelkunova

2020

Acta Naturae

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“…В част-ности, для замены VIG разрабатывают противоортопокс-вирусные полноразмерные человеческие или химерные антитела (McCausland et al, 2010;Crickard et al, 2012;Tikunova et al, 2012;Matho et al, 2015). Как правило, для исследования противовирусных свойств получен-ных антител используют экспериментальную наработку антител в системе транзиентной экспрессии при одно-временной трансфекции эукариотических клеток двумя плазмидами, каждая из которых несет ген, кодирующий тяжелую или легкую цепи целевого антитела.…”

Section: результаты и обсуждениеunclassified

Development of a stable eukaryotic strain producing fully human monoclonal antibody on the basis of the human antibody against ectromelia virus

Матвеев¹,

Хлусевич²,

Байков³

et al. 2017

Vestn. VOGiS

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“…The interaction between viruses and their hosts is often determined by interactions between viral glycoproteins and host cell receptors, and thus deletion/mutation of glycoproteins found in the envelope of viruses typically impact host cell entry, host range, and pathogen recognition. As such, viral glycoproteins are a major target of neutralizing antibodies [3][4][5][6][7][8]. This combination of factors, in turn, affects viral pathogenesis [1,2,9].…”

Section: Introductionmentioning

confidence: 99%

An increase in glycoprotein concentration on extracellular virions dramatically alters vaccinia virus infectivity and pathogenesis without impacting immunogenicity

et al. 2021

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The extracellular virion (EV) form of Orthopoxviruses is required for cell-to-cell spread and pathogenesis, and is the target of neutralizing antibodies in the protective immune response. EV have a double envelope that contains several unique proteins that are involved in its intracellular envelopment and/or subsequent infectivity. One of these, F13, is involved in both EV formation and infectivity. Here, we report that replacement of vaccinia virus F13L with the molluscum contagiosum virus homolog, MC021L results in the production of EV particles with significantly increased levels of EV glycoproteins, which correlate with a small plaque phenotype. Using a novel fluorescence-activated virion sorting assay to isolate EV populations based on glycoprotein content we determine that EV containing either higher or lower levels of glycoproteins are less infectious, suggesting that there is an optimal concentration of glycoproteins in the outer envelope that is required for maximal infectivity of EV. This optimal glycoprotein concentration was required for lethality and induction of pathology in a cutaneous model of animal infection, but was not required for induction of a protective immune response. Therefore, our results demonstrate that there is a sensitive balance between glycoprotein incorporation, infectivity, and pathogenesis, and that manipulation of EV glycoprotein levels can produce vaccine vectors in which pathologic side effects are attenuated without a marked diminution in induction of protective immunity.

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Structural and Functional Characterization of Anti-A33 Antibodies Reveal a Potent Cross-Species Orthopoxviruses Neutralizer

Cited by 38 publications

References 71 publications

Genes that control vaccinia virus immunogenicity

Genes that control vaccinia virus immunogenicity

Development of a stable eukaryotic strain producing fully human monoclonal antibody on the basis of the human antibody against ectromelia virus

An increase in glycoprotein concentration on extracellular virions dramatically alters vaccinia virus infectivity and pathogenesis without impacting immunogenicity

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