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Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA

When introduced in the 1990s, immunization with DNA plasmids was considered potentially revolutionary for vaccine development, particularly for vaccines intended to induce protective CD8 T cell responses against multiple antigens. We conducted, in 1997−1998, the first clinical trial in healthy human...

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Autores principales: Richie, Thomas L., Charoenvit, Yupin, Wang, Ruobing, Epstein, Judith E., Hedstrom, Richard C., Kumar, Sanjai, Luke, Thomas C., Freilich, Daniel A., Aguiar, Joao C., Sacci, Jr., John B., Sedegah, Martha, Nosek, Jr., Ronald A., De La Vega, Patricia, Berzins, Mara P., Majam, Victoria F., Abot, Esteban N., Ganeshan, Harini, Richie, Nancy O., Banania, Jo Glenna, Baraceros, Maria Fe B., Geter, Tanya G., Mere, Robin, Bebris, Lolita, Limbach, Keith, Hickey, Bradley W., Lanar, David E., Ng, Jennifer, Shi, Meng, Hobart, Peter M., Norman, Jon A., Soisson, Lorraine A., Hollingdale, Michael R., Rogers, William O., Doolan, Denise L., Hoffman, Stephen L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Landes Bioscience 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3601132/
https://www.ncbi.nlm.nih.gov/pubmed/23151451
http://dx.doi.org/10.4161/hv.22129
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author Richie, Thomas L.
Charoenvit, Yupin
Wang, Ruobing
Epstein, Judith E.
Hedstrom, Richard C.
Kumar, Sanjai
Luke, Thomas C.
Freilich, Daniel A.
Aguiar, Joao C.
Sacci, Jr., John B.
Sedegah, Martha
Nosek, Jr., Ronald A.
De La Vega, Patricia
Berzins, Mara P.
Majam, Victoria F.
Abot, Esteban N.
Ganeshan, Harini
Richie, Nancy O.
Banania, Jo Glenna
Baraceros, Maria Fe B.
Geter, Tanya G.
Mere, Robin
Bebris, Lolita
Limbach, Keith
Hickey, Bradley W.
Lanar, David E.
Ng, Jennifer
Shi, Meng
Hobart, Peter M.
Norman, Jon A.
Soisson, Lorraine A.
Hollingdale, Michael R.
Rogers, William O.
Doolan, Denise L.
Hoffman, Stephen L.
author_facet Richie, Thomas L.
Charoenvit, Yupin
Wang, Ruobing
Epstein, Judith E.
Hedstrom, Richard C.
Kumar, Sanjai
Luke, Thomas C.
Freilich, Daniel A.
Aguiar, Joao C.
Sacci, Jr., John B.
Sedegah, Martha
Nosek, Jr., Ronald A.
De La Vega, Patricia
Berzins, Mara P.
Majam, Victoria F.
Abot, Esteban N.
Ganeshan, Harini
Richie, Nancy O.
Banania, Jo Glenna
Baraceros, Maria Fe B.
Geter, Tanya G.
Mere, Robin
Bebris, Lolita
Limbach, Keith
Hickey, Bradley W.
Lanar, David E.
Ng, Jennifer
Shi, Meng
Hobart, Peter M.
Norman, Jon A.
Soisson, Lorraine A.
Hollingdale, Michael R.
Rogers, William O.
Doolan, Denise L.
Hoffman, Stephen L.
author_sort Richie, Thomas L.
collection PubMed
description When introduced in the 1990s, immunization with DNA plasmids was considered potentially revolutionary for vaccine development, particularly for vaccines intended to induce protective CD8 T cell responses against multiple antigens. We conducted, in 1997−1998, the first clinical trial in healthy humans of a DNA vaccine, a single plasmid encoding Plasmodium falciparum circumsporozoite protein (PfCSP), as an initial step toward developing a multi-antigen malaria vaccine targeting the liver stages of the parasite. As the next step, we conducted in 2000–2001 a clinical trial of a five-plasmid mixture called MuStDO5 encoding pre-erythrocytic antigens PfCSP, PfSSP2/TRAP, PfEXP1, PfLSA1 and PfLSA3. Thirty-two, malaria-naïve, adult volunteers were enrolled sequentially into four cohorts receiving a mixture of 500 μg of each plasmid plus escalating doses (0, 20, 100 or 500 μg) of a sixth plasmid encoding human granulocyte macrophage-colony stimulating factor (hGM-CSF). Three doses of each formulation were administered intramuscularly by needle-less jet injection at 0, 4 and 8 weeks, and each cohort had controlled human malaria infection administered by five mosquito bites 18 d later. The vaccine was safe and well-tolerated, inducing moderate antigen-specific, MHC-restricted T cell interferon-γ responses but no antibodies. Although no volunteers were protected, T cell responses were boosted post malaria challenge. This trial demonstrated the MuStDO5 DNA and hGM-CSF plasmids to be safe and modestly immunogenic for T cell responses. It also laid the foundation for priming with DNA plasmids and boosting with recombinant viruses, an approach known for nearly 15 y to enhance the immunogenicity and protective efficacy of DNA vaccines.
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spelling pubmed-36011322013-03-22 Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA Richie, Thomas L. Charoenvit, Yupin Wang, Ruobing Epstein, Judith E. Hedstrom, Richard C. Kumar, Sanjai Luke, Thomas C. Freilich, Daniel A. Aguiar, Joao C. Sacci, Jr., John B. Sedegah, Martha Nosek, Jr., Ronald A. De La Vega, Patricia Berzins, Mara P. Majam, Victoria F. Abot, Esteban N. Ganeshan, Harini Richie, Nancy O. Banania, Jo Glenna Baraceros, Maria Fe B. Geter, Tanya G. Mere, Robin Bebris, Lolita Limbach, Keith Hickey, Bradley W. Lanar, David E. Ng, Jennifer Shi, Meng Hobart, Peter M. Norman, Jon A. Soisson, Lorraine A. Hollingdale, Michael R. Rogers, William O. Doolan, Denise L. Hoffman, Stephen L. Hum Vaccin Immunother Research Paper When introduced in the 1990s, immunization with DNA plasmids was considered potentially revolutionary for vaccine development, particularly for vaccines intended to induce protective CD8 T cell responses against multiple antigens. We conducted, in 1997−1998, the first clinical trial in healthy humans of a DNA vaccine, a single plasmid encoding Plasmodium falciparum circumsporozoite protein (PfCSP), as an initial step toward developing a multi-antigen malaria vaccine targeting the liver stages of the parasite. As the next step, we conducted in 2000–2001 a clinical trial of a five-plasmid mixture called MuStDO5 encoding pre-erythrocytic antigens PfCSP, PfSSP2/TRAP, PfEXP1, PfLSA1 and PfLSA3. Thirty-two, malaria-naïve, adult volunteers were enrolled sequentially into four cohorts receiving a mixture of 500 μg of each plasmid plus escalating doses (0, 20, 100 or 500 μg) of a sixth plasmid encoding human granulocyte macrophage-colony stimulating factor (hGM-CSF). Three doses of each formulation were administered intramuscularly by needle-less jet injection at 0, 4 and 8 weeks, and each cohort had controlled human malaria infection administered by five mosquito bites 18 d later. The vaccine was safe and well-tolerated, inducing moderate antigen-specific, MHC-restricted T cell interferon-γ responses but no antibodies. Although no volunteers were protected, T cell responses were boosted post malaria challenge. This trial demonstrated the MuStDO5 DNA and hGM-CSF plasmids to be safe and modestly immunogenic for T cell responses. It also laid the foundation for priming with DNA plasmids and boosting with recombinant viruses, an approach known for nearly 15 y to enhance the immunogenicity and protective efficacy of DNA vaccines. Landes Bioscience 2012-11-01 /pmc/articles/PMC3601132/ /pubmed/23151451 http://dx.doi.org/10.4161/hv.22129 Text en Copyright © 2012 Landes Bioscience http://creativecommons.org/licenses/by-nc/3.0/ This is an open-access article licensed under a Creative Commons Attribution-NonCommercial 3.0 Unported License. The article may be redistributed, reproduced, and reused for non-commercial purposes, provided the original source is properly cited.
spellingShingle Research Paper
Richie, Thomas L.
Charoenvit, Yupin
Wang, Ruobing
Epstein, Judith E.
Hedstrom, Richard C.
Kumar, Sanjai
Luke, Thomas C.
Freilich, Daniel A.
Aguiar, Joao C.
Sacci, Jr., John B.
Sedegah, Martha
Nosek, Jr., Ronald A.
De La Vega, Patricia
Berzins, Mara P.
Majam, Victoria F.
Abot, Esteban N.
Ganeshan, Harini
Richie, Nancy O.
Banania, Jo Glenna
Baraceros, Maria Fe B.
Geter, Tanya G.
Mere, Robin
Bebris, Lolita
Limbach, Keith
Hickey, Bradley W.
Lanar, David E.
Ng, Jennifer
Shi, Meng
Hobart, Peter M.
Norman, Jon A.
Soisson, Lorraine A.
Hollingdale, Michael R.
Rogers, William O.
Doolan, Denise L.
Hoffman, Stephen L.
Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA
title Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA
title_full Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA
title_fullStr Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA
title_full_unstemmed Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA
title_short Clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of MuStDO5, a five-gene, sporozoite/hepatic stage Plasmodium falciparum DNA vaccine combined with escalating dose human GM-CSF DNA
title_sort clinical trial in healthy malaria-naïve adults to evaluate the safety, tolerability, immunogenicity and efficacy of mustdo5, a five-gene, sporozoite/hepatic stage plasmodium falciparum dna vaccine combined with escalating dose human gm-csf dna
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3601132/
https://www.ncbi.nlm.nih.gov/pubmed/23151451
http://dx.doi.org/10.4161/hv.22129
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