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A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults

BACKGROUND: A DNA-prime/human adenovirus serotype 5 (HuAd5) boost vaccine encoding Plasmodium falciparum (Pf) circumsporozoite protein (PfCSP) and Pf apical membrane antigen-1 (PfAMA1), elicited protection in 4/15 (27%) of subjects against controlled human malaria infection (CHMI) that was statistic...

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Autores principales: Sklar, Marvin J., Maiolatesi, Santina, Patterson, Noelle, Sedegah, Martha, Limbach, Keith, Teneza-Mora, Nimfa, Chuang, Ilin, Hollis-Perry, K. Monique, Banania, Jo Glenna, Guzman, Ivelese, Ganeshan, Harini, Reyes, Sharina, Hollingdale, Michael R., Wong, Mimi, Lindstrom, Ashley, Reyes, Anatalio, Alcorta, Yolanda, Garver, Lindsey, Bankard, Kelli, Belmonte, Arnel, Belmonte, Maria, Huang, Jun, Gowda, Kalpana, Inoue, Sandra, Velasco, Rachel, Bergmann-Leitner, Elke, Hutter, Jack, Lee, Tida, Adams, Nehkonti, Chaudhury, Sidhartha, Hunt, Devin, Tamminga, Cindy, Berrie, Eleanor, Bellamy, Duncan, Bittaye, Mustapha, Ewer, Katie, Diggs, Carter, Soisson, Lorraine A., Lawrie, Alison, Hill, Adrian, Richie, Thomas L., Villasante, Eileen, Epstein, Judith E., Duplessis, Christopher A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8425539/
https://www.ncbi.nlm.nih.gov/pubmed/34495988
http://dx.doi.org/10.1371/journal.pone.0256980
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author Sklar, Marvin J.
Maiolatesi, Santina
Patterson, Noelle
Sedegah, Martha
Limbach, Keith
Teneza-Mora, Nimfa
Chuang, Ilin
Hollis-Perry, K. Monique
Banania, Jo Glenna
Guzman, Ivelese
Ganeshan, Harini
Reyes, Sharina
Hollingdale, Michael R.
Wong, Mimi
Lindstrom, Ashley
Reyes, Anatalio
Alcorta, Yolanda
Garver, Lindsey
Bankard, Kelli
Belmonte, Arnel
Belmonte, Maria
Huang, Jun
Gowda, Kalpana
Inoue, Sandra
Velasco, Rachel
Bergmann-Leitner, Elke
Hutter, Jack
Lee, Tida
Adams, Nehkonti
Chaudhury, Sidhartha
Hunt, Devin
Tamminga, Cindy
Berrie, Eleanor
Bellamy, Duncan
Bittaye, Mustapha
Ewer, Katie
Diggs, Carter
Soisson, Lorraine A.
Lawrie, Alison
Hill, Adrian
Richie, Thomas L.
Villasante, Eileen
Epstein, Judith E.
Duplessis, Christopher A.
author_facet Sklar, Marvin J.
Maiolatesi, Santina
Patterson, Noelle
Sedegah, Martha
Limbach, Keith
Teneza-Mora, Nimfa
Chuang, Ilin
Hollis-Perry, K. Monique
Banania, Jo Glenna
Guzman, Ivelese
Ganeshan, Harini
Reyes, Sharina
Hollingdale, Michael R.
Wong, Mimi
Lindstrom, Ashley
Reyes, Anatalio
Alcorta, Yolanda
Garver, Lindsey
Bankard, Kelli
Belmonte, Arnel
Belmonte, Maria
Huang, Jun
Gowda, Kalpana
Inoue, Sandra
Velasco, Rachel
Bergmann-Leitner, Elke
Hutter, Jack
Lee, Tida
Adams, Nehkonti
Chaudhury, Sidhartha
Hunt, Devin
Tamminga, Cindy
Berrie, Eleanor
Bellamy, Duncan
Bittaye, Mustapha
Ewer, Katie
Diggs, Carter
Soisson, Lorraine A.
Lawrie, Alison
Hill, Adrian
Richie, Thomas L.
Villasante, Eileen
Epstein, Judith E.
Duplessis, Christopher A.
author_sort Sklar, Marvin J.
collection PubMed
description BACKGROUND: A DNA-prime/human adenovirus serotype 5 (HuAd5) boost vaccine encoding Plasmodium falciparum (Pf) circumsporozoite protein (PfCSP) and Pf apical membrane antigen-1 (PfAMA1), elicited protection in 4/15 (27%) of subjects against controlled human malaria infection (CHMI) that was statistically associated with CD8+ T cell responses. Subjects with high level pre-existing immunity to HuAd5 were not protected, suggesting an adverse effect on vaccine efficacy (VE). We replaced HuAd5 with chimpanzee adenovirus 63 (ChAd63), and repeated the study, assessing both the two-antigen (CSP, AMA1 = CA) vaccine, and a novel three-antigen (CSP, AMA1, ME-TRAP = CAT) vaccine that included a third pre-erythrocytic stage antigen [malaria multiple epitopes (ME) fused to the Pf thrombospondin-related adhesive protein (TRAP)] to potentially enhance protection. METHODOLOGY: This was an open label, randomized Phase 1 trial, assessing safety, tolerability, and VE against CHMI in healthy, malaria naïve adults. Forty subjects (20 each group) were to receive three monthly CA or CAT DNA priming immunizations, followed by corresponding ChAd63 boost four months later. Four weeks after the boost, immunized subjects and 12 infectivity controls underwent CHMI by mosquito bite using the Pf3D7 strain. VE was assessed by determining the differences in time to parasitemia as detected by thick blood smears up to 28-days post CHMI and utilizing the log rank test, and by calculating the risk ratio of each treatment group and subtracting from 1, with significance calculated by the Cochran-Mantel-Haenszel method. RESULTS: In both groups, systemic adverse events (AEs) were significantly higher after the ChAd63 boost than DNA immunizations. Eleven of 12 infectivity controls developed parasitemia (mean 11.7 days). In the CA group, 15 of 16 (93.8%) immunized subjects developed parasitemia (mean 12.0 days). In the CAT group, 11 of 16 (63.8%) immunized subjects developed parasitemia (mean 13.0 days), indicating significant protection by log rank test compared to infectivity controls (p = 0.0406) and the CA group (p = 0.0229). VE (1 minus the risk ratio) in the CAT group was 25% compared to -2% in the CA group. The CA and CAT vaccines induced robust humoral (ELISA antibodies against CSP, AMA1 and TRAP, and IFA responses against sporozoites and Pf3D7 blood stages), and cellular responses (IFN-γ FluoroSpot responses to CSP, AMA1 and TRAP) that were not associated with protection. CONCLUSIONS: This study demonstrated that the ChAd63 CAT vaccine exhibited significant protective efficacy, and confirmed protection was afforded by adding a third antigen (T) to a two-antigen (CA) formulation to achieve increased VE. Although the ChAd63-CAT vaccine was associated with increased frequencies of systemic AEs compared to the CA vaccine and, historically, compared to the HuAd5 vectored malaria vaccine encoding CSP and AMA1, they were transient and associated with increased vector dosing.
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spelling pubmed-84255392021-09-09 A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults Sklar, Marvin J. Maiolatesi, Santina Patterson, Noelle Sedegah, Martha Limbach, Keith Teneza-Mora, Nimfa Chuang, Ilin Hollis-Perry, K. Monique Banania, Jo Glenna Guzman, Ivelese Ganeshan, Harini Reyes, Sharina Hollingdale, Michael R. Wong, Mimi Lindstrom, Ashley Reyes, Anatalio Alcorta, Yolanda Garver, Lindsey Bankard, Kelli Belmonte, Arnel Belmonte, Maria Huang, Jun Gowda, Kalpana Inoue, Sandra Velasco, Rachel Bergmann-Leitner, Elke Hutter, Jack Lee, Tida Adams, Nehkonti Chaudhury, Sidhartha Hunt, Devin Tamminga, Cindy Berrie, Eleanor Bellamy, Duncan Bittaye, Mustapha Ewer, Katie Diggs, Carter Soisson, Lorraine A. Lawrie, Alison Hill, Adrian Richie, Thomas L. Villasante, Eileen Epstein, Judith E. Duplessis, Christopher A. PLoS One Research Article BACKGROUND: A DNA-prime/human adenovirus serotype 5 (HuAd5) boost vaccine encoding Plasmodium falciparum (Pf) circumsporozoite protein (PfCSP) and Pf apical membrane antigen-1 (PfAMA1), elicited protection in 4/15 (27%) of subjects against controlled human malaria infection (CHMI) that was statistically associated with CD8+ T cell responses. Subjects with high level pre-existing immunity to HuAd5 were not protected, suggesting an adverse effect on vaccine efficacy (VE). We replaced HuAd5 with chimpanzee adenovirus 63 (ChAd63), and repeated the study, assessing both the two-antigen (CSP, AMA1 = CA) vaccine, and a novel three-antigen (CSP, AMA1, ME-TRAP = CAT) vaccine that included a third pre-erythrocytic stage antigen [malaria multiple epitopes (ME) fused to the Pf thrombospondin-related adhesive protein (TRAP)] to potentially enhance protection. METHODOLOGY: This was an open label, randomized Phase 1 trial, assessing safety, tolerability, and VE against CHMI in healthy, malaria naïve adults. Forty subjects (20 each group) were to receive three monthly CA or CAT DNA priming immunizations, followed by corresponding ChAd63 boost four months later. Four weeks after the boost, immunized subjects and 12 infectivity controls underwent CHMI by mosquito bite using the Pf3D7 strain. VE was assessed by determining the differences in time to parasitemia as detected by thick blood smears up to 28-days post CHMI and utilizing the log rank test, and by calculating the risk ratio of each treatment group and subtracting from 1, with significance calculated by the Cochran-Mantel-Haenszel method. RESULTS: In both groups, systemic adverse events (AEs) were significantly higher after the ChAd63 boost than DNA immunizations. Eleven of 12 infectivity controls developed parasitemia (mean 11.7 days). In the CA group, 15 of 16 (93.8%) immunized subjects developed parasitemia (mean 12.0 days). In the CAT group, 11 of 16 (63.8%) immunized subjects developed parasitemia (mean 13.0 days), indicating significant protection by log rank test compared to infectivity controls (p = 0.0406) and the CA group (p = 0.0229). VE (1 minus the risk ratio) in the CAT group was 25% compared to -2% in the CA group. The CA and CAT vaccines induced robust humoral (ELISA antibodies against CSP, AMA1 and TRAP, and IFA responses against sporozoites and Pf3D7 blood stages), and cellular responses (IFN-γ FluoroSpot responses to CSP, AMA1 and TRAP) that were not associated with protection. CONCLUSIONS: This study demonstrated that the ChAd63 CAT vaccine exhibited significant protective efficacy, and confirmed protection was afforded by adding a third antigen (T) to a two-antigen (CA) formulation to achieve increased VE. Although the ChAd63-CAT vaccine was associated with increased frequencies of systemic AEs compared to the CA vaccine and, historically, compared to the HuAd5 vectored malaria vaccine encoding CSP and AMA1, they were transient and associated with increased vector dosing. Public Library of Science 2021-09-08 /pmc/articles/PMC8425539/ /pubmed/34495988 http://dx.doi.org/10.1371/journal.pone.0256980 Text en https://creativecommons.org/publicdomain/zero/1.0/This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Sklar, Marvin J.
Maiolatesi, Santina
Patterson, Noelle
Sedegah, Martha
Limbach, Keith
Teneza-Mora, Nimfa
Chuang, Ilin
Hollis-Perry, K. Monique
Banania, Jo Glenna
Guzman, Ivelese
Ganeshan, Harini
Reyes, Sharina
Hollingdale, Michael R.
Wong, Mimi
Lindstrom, Ashley
Reyes, Anatalio
Alcorta, Yolanda
Garver, Lindsey
Bankard, Kelli
Belmonte, Arnel
Belmonte, Maria
Huang, Jun
Gowda, Kalpana
Inoue, Sandra
Velasco, Rachel
Bergmann-Leitner, Elke
Hutter, Jack
Lee, Tida
Adams, Nehkonti
Chaudhury, Sidhartha
Hunt, Devin
Tamminga, Cindy
Berrie, Eleanor
Bellamy, Duncan
Bittaye, Mustapha
Ewer, Katie
Diggs, Carter
Soisson, Lorraine A.
Lawrie, Alison
Hill, Adrian
Richie, Thomas L.
Villasante, Eileen
Epstein, Judith E.
Duplessis, Christopher A.
A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
title A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
title_full A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
title_fullStr A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
title_full_unstemmed A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
title_short A three-antigen Plasmodium falciparum DNA prime—Adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
title_sort three-antigen plasmodium falciparum dna prime—adenovirus boost malaria vaccine regimen is superior to a two-antigen regimen and protects against controlled human malaria infection in healthy malaria-naïve adults
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8425539/
https://www.ncbi.nlm.nih.gov/pubmed/34495988
http://dx.doi.org/10.1371/journal.pone.0256980
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AT leetida threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT adamsnehkonti threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT chaudhurysidhartha threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT huntdevin threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT tammingacindy threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT berrieeleanor threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT bellamyduncan threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT bittayemustapha threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT ewerkatie threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT diggscarter threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT soissonlorrainea threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT lawriealison threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT hilladrian threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT richiethomasl threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT villasanteeileen threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT epsteinjudithe threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults
AT duplessischristophera threeantigenplasmodiumfalciparumdnaprimeadenovirusboostmalariavaccineregimenissuperiortoatwoantigenregimenandprotectsagainstcontrolledhumanmalariainfectioninhealthymalarianaiveadults