Adenovirus-5-Vectored P. falciparum Vaccine Expressing CSP and AMA1. Part B: Safety, Immunogenicity and Protective Efficacy of the CSP Component

Tamminga, Cindy; Sedegah, Martha; Regis, David; Chuang, Ilin; Epstein, Judith E.; Spring, Michele; Mendoza-Silveiras, Jose; McGrath, Shannon; Maiolatesi, Santina; Reyes, Sharina; Steinbeiss, Victoria; Fedders, Charlotte; Smith, Kathryn; House, Brent; Ganeshan, Harini; Lejano, Jennylynn; Abot, Esteban; Banania, Glenna; Sayo, Renato; Farooq, Fouzia; Belmonte, María; Murphy, Jittawadee; Komisar, Jack; Williams, Jon H Sims; Shi, M.; Brambilla, Donald; Manohar, Nalini; Richie, Nancy; Wood, Chloe; Limbach, Keith; Patterson, Noelle B.; Bruder, Joseph T.; Doolan, Denise L.; King, C. Richter; Diggs, Carter L.; Soisson, Lorraine; Carucci, Daniel J.; Levine, Gail; Dutta, Sandeep; Hollingdale, Michael R.; Ockenhouse, Christian F.; Richie, Thomas L.

doi:10.1371/journal.pone.0025868

Cited by 73 publications

(92 citation statements)

References 83 publications

(94 reference statements)

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“…The results obtained with the mouse model have fueled a number of human trials with plasmid DNA, recombinant viruses, and, more recently, radiation-attenuated sporozoites as vaccine formulations. Unfortunately, in spite of the enthusiasm generated by the mouse model, T cell-based vaccines against preerythrocytic stages of malaria have provided sterile immunity against infection with P. falciparum to only a few vaccinated individuals to date (39)(40)(41)(42)(43)(44). The precise reason for this failure is not clear.…”

Section: Discussionmentioning

confidence: 99%

Immunogenicity of a Prime-Boost Vaccine Containing the Circumsporozoite Proteins of Plasmodium vivax in Rodents

et al. 2014

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g Plasmodium vivax is the most widespread and the second most prevalent malaria-causing species in the world. Current measures used to control the transmission of this disease would benefit from the development of an efficacious vaccine. In the case of the deadly parasite P. falciparum, the recombinant RTS,S vaccine containing the circumsporozoite antigen (CSP) consistently protects 30 to 50% of human volunteers against infection and is undergoing phase III clinical trials in Africa with similar efficacy. These findings encouraged us to develop a P. vivax vaccine containing the three circulating allelic forms of P. vivax CSP. Toward this goal, we generated three recombinant bacterial proteins representing the CSP alleles, as well as a hybrid polypeptide called PvCSP-All-CSP-epitopes. This hybrid contains the conserved N and C termini of P. vivax CSP and the three variant repeat domains in tandem. We also generated simian and human recombinant replication-defective adenovirus vectors expressing PvCSP-All-CSP-epitopes. Mice immunized with the mixture of recombinant proteins in a formulation containing the adjuvant poly(I·C) developed high and long-lasting serum IgG titers comparable to those elicited by proteins emulsified in complete Freund's adjuvant. Antibody titers were similar in mice immunized with homologous (protein-protein) and heterologous (adenovirus-protein) vaccine regimens. The antibodies recognized the three allelic forms of CSP, reacted to the repeated and nonrepeated regions of CSP, and recognized sporozoites expressing the alleles VK210 and VK247. The vaccine formulations described in this work should be useful for the further development of an anti-P. vivax vaccine.

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Section: Discussionmentioning

confidence: 99%

Immunogenicity of a Prime-Boost Vaccine Containing the Circumsporozoite Proteins of Plasmodium vivax in Rodents

et al. 2014

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“…At the end of the 60-min incubation, virus was aspirated from the cells, and the cells were washed with phosphate-buffered saline (PBS), overlaid with 3 ml of prewarmed DMEM plus 10% FBS, and incubated in a 5% CO 2 incubator at either 32°C or 37°C. At various time points postinfection (24,48, and/or 72 h) the infected cells were scraped into 15-ml polypropylene tubes and frozen and thawed three times to lyse infected cells and release vector particles. The number of viral particles was measured by the FFU assay as follows.…”

Section: Methodsmentioning

confidence: 99%

“…Ad5 vectors can be grown to very high yields in bioreactors and can be purified efficiently with reasonable cost-of-goods estimates for vaccines. Adenovirus-based vectors are capable of generating robust and protective T cell and antibody responses in animal models (7)(8)(9)(10)(11)(12)(13)(14)(15)(16)(17), and clinical data conclusively show that Ad5 vectors can induce potent CD8 ϩ and CD4 ϩ T cell and antibody responses in vaccinated volunteers (18)(19)(20)(21)(22)(23)(24)(25). Most encouragingly, the protective capacity of a DNA prime-Ad5 boost regimen expressing two malaria antigens demonstrated sterile protection from malaria in 27% of test subjects (26).…”

mentioning

confidence: 99%

Identification of a Suppressor Mutation That Improves the Yields of Hexon-Modified Adenovirus Vectors

Bruder

Chen

Семенова

et al. 2013

J Virol

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We have generated hexon-modified adenovirus serotype 5 (Ad5) vectors that are not neutralized by Ad5-specific neutralizing antibodies in mice. These vectors are attractive for the advancement of vaccine products because of their potential for inducing robust antigen-specific immune responses in people with prior exposure to Ad5. However, hexon-modified Ad5 vectors displayed an approximate 10-fold growth defect in complementing cells, making potential vaccine costs unacceptably high. Replacing hypervariable regions (HVRs) 1, 2, 4, and 5 with the equivalent HVRs from Ad43 was sufficient to avoid Ad5 preexisting immunity and retain full vaccine potential. However, the resulting vector displayed the same growth defect as the hexon-modified vector carrying all 9 HVRs from Ad43. The growth defect is likely due to a defect in capsid assembly, since DNA replication and late protein accumulation were normal in these vectors. We determined that the hexon-modified vectors have a 32°C cold-sensitive phenotype and selected revertants that restored vector productivity. Genome sequencing identified a single base change resulting in a threonine-to-methionine amino acid substitution at the position equivalent to residue 342 of the wild-type protein. This mutation has a suppressor phenotype (SP), since cloning it into our Ad5 vector containing all nine hypervariable regions from Ad43, Ad5.H(43m-43), increased yields over the version without the SP mutation. This growth improvement was also shown for an Ad5-based hexon-modified vector that carried the hexon hypervariable regions of Ad48, indicating that the SP mutation may have broad applicability for improving the productivity of different hexon-modified vectors.A denovirus vectors are considered a leading viral vector platform for vaccines because of their robust immunogenicity and manufacturing feasibility. The most potent adenovirus vectors for use as vaccines are based on adenovirus serotype 5 (Ad5) (1-6). Ad5 vectors can be grown to very high yields in bioreactors and can be purified efficiently with reasonable cost-of-goods estimates for vaccines. Adenovirus-based vectors are capable of generating robust and protective T cell and antibody responses in animal models (7)(8)(9)(10)(11)(12)(13)(14)(15)(16)(17), and clinical data conclusively show that Ad5 vectors can induce potent CD8 ϩ and CD4 ϩ T cell and antibody responses in vaccinated volunteers (18)(19)(20)(21)(22)(23)(24)(25). Most encouragingly, the protective capacity of a DNA prime-Ad5 boost regimen expressing two malaria antigens demonstrated sterile protection from malaria in 27% of test subjects (26). However, the high prevalence of Ad5-specific neutralizing antibodies (NAb) in human populations, especially in sub-Saharan Africa, has the potential to limit the effectiveness of Ad5-based vaccines (23,(27)(28)(29)(30).Hexon is the most abundant adenoviral structural protein, and studies show that it is the major target for NAb in vivo (23,31,32). These NAbs target the nine hypervariable regions that form the exposed ...

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“…На серонега-тивных и серопозитивных по отношению к Ad5 добровольцах были исследованы различные дозы и схемы введения вакцины. Согласно результа-там эксперимента, вакцина безопасна, хорошо переносится, вызывает иммунный ответ про-должительностью до 12 месяцев (иммунный от-вет был выше в группе с низкой дозой вакцины), как гуморальный, так и клеточный, но не обе-спечивает стерильную защиту [22,30]. В схеме с однократным внутримышечным введением вакцины уровень гуморального иммунного отве-та был низким, хотя клеточный иммунный ответ на антигены малярийного плазмодия наблюдал-ся у 56% испытуемых для CS-антигена и у 100% для АМА1.…”

Section: вакцины на основе ад-векторовunclassified

Development of Vaccines Based on Adenoviral Vectors: A Review of Foreign Clinical Studies (Part 2)

Черенова¹,

Каштиго²,

Саядян³

et al. 2017

Med. immunol.

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Адрес для переписки:Черенова Любовь Викторовна ФГБУ «Федеральный научно-исследовательский центр эпидемиологии и микробиологии им. почетного академика Н.Ф. Гамалеи» Министерства здравоохранения РФ 123098, Россия, г. Москва, ул. Гамалеи, 18. Тел.: 8 (916) 329-92-78. Факс: 8 (499) 193-61-35. E-mail: cherenova@yandex.ru Address for correspondence : Cherenova Liubov V. N. Gamaleya Research Institute of Epidemiology and Microbiology 123098, Russian Federation, Moscow, Gamaleya str., 18. Phone: 7 (916) // Медицинская иммунология, 2017. Т. 19, № 4. С. 329-358. doi: 10.15789/1563-0625-2017-4-329-358 © Черенова Л.В. и соавт., 2017 /Meditsinskaya Immunologiya, 2017, Vol. 19, no. 4, pp. 329-358. doi: 10.15789/1563-0625-2017 Резюме. В настоящее время для многих инфекционных заболеваний человека не разработаны эффективные способы лечения и профилактики. Одним из последних достижений биотехнологии является использование аденовирусных векторов, несущих иммунодоминантные антигены различ-ных патогенов, в качестве генно-инженерных вакцин как профилактических, так и терапевтических. Использование генно-инженерных технологий позволяет не применять при производстве вакцин живые вирусы и бактерии, сокращает время разработки и получения новых вакцинных препаратов. Аденовирусные векторы естественным путем проникают в клетки человека, вызывая довольно дли-тельный и значительный как гуморальный, так и клеточный иммунный ответ. Во второй части об-зора мы планируем привести сведения о проводимых в настоящее время за рубежом клинических испытаниях вакцин на основе аденовирусных векторов против таких инфекционных заболеваний, как грипп, малярия, геморрагическая лихорадка Эбола, туберкулез, гепатит и ряда других. Будут рас-смотрены параметры отбора добровольцев, схемы и дозы, используемые при вакцинации, приведены результаты завершенных экспериментов и предварительные результаты незаконченных на данный момент исследований.

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Adenovirus-5-Vectored P. falciparum Vaccine Expressing CSP and AMA1. Part B: Safety, Immunogenicity and Protective Efficacy of the CSP Component

Cited by 73 publications

References 83 publications

Immunogenicity of a Prime-Boost Vaccine Containing the Circumsporozoite Proteins of Plasmodium vivax in Rodents

Immunogenicity of a Prime-Boost Vaccine Containing the Circumsporozoite Proteins of Plasmodium vivax in Rodents

Identification of a Suppressor Mutation That Improves the Yields of Hexon-Modified Adenovirus Vectors

Development of Vaccines Based on Adenoviral Vectors: A Review of Foreign Clinical Studies (Part 2)

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