Your search keyword '"Aurélie Ploquin"' showing total 27 results

1. Heterologous cAd3-Ebola and MVA-EbolaZ vaccines are safe and immunogenic in US and Uganda phase 1/1b trials

Author

Myra Happe, Amelia R. Hofstetter, Jing Wang, Galina V. Yamshchikov, LaSonji A. Holman, Laura Novik, Larisa Strom, Francis Kiweewa, Salim Wakabi, Monica Millard, Colleen F. Kelley, Sarah Kabbani, Srilatha Edupuganti, Allison Beck, Florence Kaltovich, Tamar Murray, Susanna Tsukerman, Derick Carr, Carl Ashman, Daphne A. Stanley, Aurélie Ploquin, Robert T. Bailer, Richard Schwartz, Fatim Cham, Allan Tindikahwa, Zonghui Hu, Ingelise J. Gordon, Nadine Rouphael, Katherine V. Houser, Emily E. Coates, Barney S. Graham, Richard A. Koup, John R. Mascola, Nancy J. Sullivan, Merlin L. Robb, Julie A. Ake, Kirsten E. Lyke, Mark J. Mulligan, Julie E. Ledgerwood, Hannah Kibuuka, and the VRC 208 and RV 422 study team

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Ebola virus disease (EVD) is a filoviral infection caused by virus species of the Ebolavirus genus including Zaire ebolavirus (EBOV) and Sudan ebolavirus (SUDV). We investigated the safety and immunogenicity of a heterologous prime-boost regimen involving a chimpanzee adenovirus 3 vectored Ebola vaccine [either monovalent (cAd3-EBOZ) or bivalent (cAd3-EBO)] prime followed by a recombinant modified vaccinia virus Ankara EBOV vaccine (MVA-EbolaZ) boost in two phase 1/1b randomized open-label clinical trials in healthy adults in the United States (US) and Uganda (UG). Trial US (NCT02408913) enrolled 140 participants, including 26 EVD vaccine-naïve and 114 cAd3-Ebola-experienced participants (April-November 2015). Trial UG (NCT02354404) enrolled 90 participants, including 60 EVD vaccine-naïve and 30 DNA Ebola vaccine-experienced participants (February-April 2015). All tested vaccines and regimens were safe and well tolerated with no serious adverse events reported related to study products. Solicited local and systemic reactogenicity was mostly mild to moderate in severity. The heterologous prime-boost regimen was immunogenic, including induction of durable antibody responses which peaked as early as two weeks and persisted up to one year after each vaccination. Different prime-boost intervals impacted the magnitude of humoral and cellular immune responses. The results from these studies demonstrate promising implications for use of these vaccines in both prophylactic and outbreak settings.

Published

2024

2. Definition of herpes simplex virus type 1 helper activities for adeno-associated virus early replication events.

Author

Nathalie Alazard-Dany, Armel Nicolas, Aurélie Ploquin, Regina Strasser, Anna Greco, Alberto L Epstein, Cornel Fraefel, and Anna Salvetti

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The human parvovirus Adeno-Associated Virus (AAV) type 2 can only replicate in cells co-infected with a helper virus, such as Adenovirus or Herpes Simplex Virus type 1 (HSV-1); whereas, in the absence of a helper virus, it establishes a latent infection. Previous studies demonstrated that the ternary HSV-1 helicase/primase (HP) complex (UL5/8/52) and the single-stranded DNA-Binding Protein (ICP8) were sufficient to induce AAV-2 replication in transfected cells. We independently showed that, in the context of a latent AAV-2 infection, the HSV-1 ICP0 protein was able to activate rep gene expression. The present study was conducted to integrate these observations and to further explore the requirement of other HSV-1 proteins during early AAV replication steps, i.e. rep gene expression and AAV DNA replication. Using a cellular model that mimics AAV latency and composite constructs coding for various sets of HSV-1 genes, we first confirmed the role of ICP0 for rep gene expression and demonstrated a synergistic effect of ICP4 and, to a lesser extent, ICP22. Conversely, ICP27 displayed an inhibitory effect. Second, our analyses showed that the effect of ICP0, ICP4, and ICP22 on rep gene expression was essential for the onset of AAV DNA replication in conjunction with the HP complex and ICP8. Third, and most importantly, we demonstrated that the HSV-1 DNA polymerase complex (UL30/UL42) was critical to enhance AAV DNA replication to a significant level in transfected cells and that its catalytic activity was involved in this process. Altogether, this work represents the first comprehensive study recapitulating the series of early events taking place during HSV-1-induced AAV replication.

Published

2009

3. Safety, tolerability, and immunogenicity of the chimpanzee adenovirus type 3-vectored Marburg virus (cAd3-Marburg) vaccine in healthy adults in the USA: a first-in-human, phase 1, open-label, dose-escalation trial

Author

Melinda J Hamer, Katherine V Houser, Amelia R Hofstetter, Ana M Ortega-Villa, Christine Lee, Anne Preston, Brooke Augustine, Charla Andrews, Galina V Yamshchikov, Somia Hickman, Steven Schech, Jack N Hutter, Paul T Scott, Paige E Waterman, Mihret F Amare, Victoria Kioko, Casey Storme, Kayvon Modjarrad, Melanie D McCauley, Merlin L Robb, Martin R Gaudinski, Ingelise J Gordon, LaSonji A Holman, Alicia T Widge, Larisa Strom, Myra Happe, Josephine H Cox, Sandra Vazquez, Daphne A Stanley, Tamar Murray, Caitlyn N M Dulan, Ruth Hunegnaw, Sandeep R Narpala, Phillip A Swanson, Manjula Basappa, Jagada Thillainathan, Marcelino Padilla, Britta Flach, Sarah O’Connell, Olga Trofymenko, Patricia Morgan, Emily E Coates, Jason G Gall, Adrian B McDermott, Richard A Koup, John R Mascola, Aurélie Ploquin, Nancy J Sullivan, Julie A Ake, Julie E Ledgerwood, Rebecca Lampley, Brenda Larkin, Pamela Costner, Hope Wilson, and Mike Read

Subjects

General Medicine

Published

2023

4. A single-shot ChAd3-MARV vaccine confers rapid and durable protection against Marburg virus in nonhuman primates

Author

Ruth Hunegnaw, Anna N. Honko, Lingshu Wang, Derick Carr, Tamar Murray, Wei Shi, Lam Nguyen, Nadia Storm, Caitlyn N. M. Dulan, Kathryn E. Foulds, Krystle N. Agans, Robert W. Cross, Joan B. Geisbert, Cheng Cheng, Aurélie Ploquin, Daphne A. Stanley, Thomas W. Geisbert, Gary J. Nabel, and Nancy J. Sullivan

Subjects

Primates, Marburgvirus, Pan troglodytes, Animals, Humans, Marburg Virus Disease, General Medicine, Ebola Vaccines, Hemorrhagic Fever, Ebola, Ebolavirus, Adenoviridae

Abstract

Marburg virus (MARV) causes a severe hemorrhagic fever disease in primates with mortality rates in humans of up to 90%. MARV has been identified as a category A bioterrorism agent by the Centers for Disease Control and Prevention (CDC) and priority pathogen A by the National Institute of Allergy and Infectious Diseases (NIAID), needing urgent research and development of countermeasures because of the high public health risk it poses. The recent cases of MARV in West Africa underscore the substantial outbreak potential of this virus. The potential for cross-border spread, as had occurred during the 2014–2016 Ebola virus outbreak, illustrates the critical need for MARV vaccines. To support regulatory approval of the chimpanzee adenovirus 3 (ChAd3)–MARV vaccine that has completed phase 1 trials, we showed that the nonreplicating ChAd3 vector, which has a demonstrated safety profile in humans, protected against a uniformly lethal challenge with MARV/Ang. Protective immunity was achieved within 7 days of vaccination and was maintained through 1 year after vaccination. Antigen-specific antibodies were an immune correlate of protection in the acute challenge model, and their concentration was predictive of protection. These results demonstrate that a single-shot ChAd3-MARV vaccine generated a protective immune response that was both rapid and durable with an immune correlate of protection that will support advanced clinical development.

Published

2022

5. Ebola Virus Transmission Initiated by Relapse of Systemic Ebola Virus Disease

Author

Karthik Gangavarapu, Amuri Aziza, Ibrahima Socé Fall, Marceline Akonga, Anne W. Rimion, Yannick Tutu Tshia N’kasar, Moussa Moïse Diagne, Fabrice Mambu, Jean Jacques Muyembe Tamfum, Ali Torkamani, Meris Matondo, Daniel Mukadi, Nancy J. Sullivan, Nella Bisento, Antoine Nkuba-Ndaye, Abdoulaye Yam, Emilia Sana-Paka, Elias Salfati, Kristian G. Andersen, Placide Mbala-Kingebeni, Bibiche Nsunda, Bailey White, Martin Faye, Francois Edidi, John Misasi, Marc A. Suchard, Michael R. Wiley, Boubacar Diallo, Catherine Pratt, Faustin Bile, Aurélie Ploquin, Olivier Tshiani, Matthias Pauthner, Steve Ahuka-Mundeke, Sabue Mulangu, Allison Black, Eddy Kinganda-Lusamaki, Amadou A. Sall, Ousmane Faye, Mbusa Mutafali-Ruffin, Lisa E. Hensley, Trevor Bedford, Marie Roseline Darnycka Belizaire, Victor Epaso, Ian Crozier, Donatien Kazadi, James Hadfield, Andrew Rambaut, Mory Keita, and Junior Bula Bula

Subjects

Male, Fatal outcome, viruses, Disease, 030204 cardiovascular system & hematology, medicine.disease_cause, Medical and Health Sciences, Fatal Outcome, 0302 clinical medicine, Recurrence, Viral, 030212 general & internal medicine, Phylogeny, Genome, biology, Transmission (medicine), General Medicine, Ebolavirus, Infectious Diseases, Vesicular stomatitis virus, Ebola, Democratic Republic of the Congo, Infection, Biotechnology, Adult, Viremia, Vaccine Related, 03 medical and health sciences, Rare Diseases, Biodefense, General & Internal Medicine, medicine, Humans, Ebola Vaccines, Ebola virus, Extramural, business.industry, Prevention, Outbreak, Bayes Theorem, biology.organism_classification, medicine.disease, Virology, Emerging Infectious Diseases, Good Health and Well Being, Mutation, Hemorrhagic Fever, RNA, Immunization, business

Abstract

During the 2018-2020 Ebola virus disease (EVD) outbreak in North Kivu province in the Democratic Republic of Congo, EVD was diagnosed in a patient who had received the recombinant vesicular stomatitis virus-based vaccine expressing a ZEBOV glycoprotein (rVSV-ZEBOV) (Merck). His treatment included an Ebola virus (EBOV)-specific monoclonal antibody (mAb114), and he recovered within 14 days. However, 6 months later, he presented again with severe EVD-like illness and EBOV viremia, and he died. We initiated epidemiologic and genomic investigations that showed that the patient had had a relapse of acute EVD that led to a transmission chain resulting in 91 cases across six health zones over 4 months. (Funded by the Bill and Melinda Gates Foundation and others.).

Published

2021

6. Rapid and Durable Protection Against Marburg Virus with a Single-Shot ChAd3-MARV GP Vaccine

Author

Ruth Hunegnaw, Anna Honko, Lingshu Wang, Derick Carr, Tamar Murray, Wei Shi, Caitlyn N. M. Dulan, Kathryn E. Foulds, Krystle N. Agans, Robert W. Cross, Joan B. Geisbert, Thomas W. Geisbert, Cheng Cheng, Aurélie Ploquin, Daphne A. Stanley, Gary J. Nabel, and Nancy J. Sullivan

Abstract

Marburg virus (MARV) causes a severe hemorrhagic fever disease in primates with mortality rates in humans up to 90%. Since 2018, MARV has been identified as a priority pathogen by the WHO, needing urgent research and development of countermeasures due to the high public health risk it poses. Recently, the first case of MARV in West Africa underscored the significant outbreak potential of this virus. The potential for cross border spread as had occurred during the Ebola 2014-2016 outbreak illustrates the critical need for Marburg vaccines. To support regulatory approval of the ChAd3-Marburg vaccine that has completed Phase I trials, we show that a non-replicating chimpanzee-derived adenovirus vector with a demonstrated safety profile in humans (ChAd3) protected against a uniformly lethal challenge with Marburg-Angola. Protective immunity was achieved within 7 days of vaccination and was maintained through one year post vaccination, antigen-specific antibodies were a significant immune correlate of protection in the acute challenge model (p=0.0003), and predictive for protection with an AUC = 0.88. These results demonstrate that a single-shot ChAd3 MARV vaccine generated a protective immune response that was both rapid and durable with a significant immune correlate of protection that will support advanced clinical development.One Sentence SummaryA single-shot of non-replicating ChAd3-MARV vaccine demonstrated both rapid (within 1 week) and durable (12 months) protection against lethal Marburg virus infection in macaques.

Published

2021

7. Protection from SARS-CoV-2 Delta one year after mRNA-1273 vaccination in rhesus macaques is coincident with anamnestic antibody response in the lung

Author

Alan Dodson, Andrea Carfi, Robert A. Seder, Cynthia G. Lorang, Jesmine Roberts-Torres, Anthony L. Cook, Lauren McCormick, Darin K. Edwards, Anne P. Werner, Danielle A. Wagner, Wei Shi, Mehul S. Suthar, Kevin W. Bock, Bingchun Zhao, Shayne F. Andrew, Juan I. Moliva, Saule T. Nurmukhambetova, Eli Boritz, Laurent Pessaint, Courtney Tucker, Ian N. Moore, Elizabeth McCarthy, Adrienne Goode, Swagata Kar, Bianca M. Nagata, Hanne Leth Andersen, Christopher Cole Honeycutt, Prakriti Mudvari, Mark G. Lewis, Barbara J. Flynn, Daniel C. Douek, Farida Laboune, Seyhan Boyoglu-Barnum, John-Paul Todd, Eun Sung Yang, Mahnaz Minai, Kathryn E. Foulds, I-Ting Teng, Kizzmekia S. Corbett, Lingshu Wang, John R. Mascola, Barney S. Graham, Aurélie Ploquin, Meredith E. Davis-Gardner, Nancy J. Sullivan, Martha Nason, Matthew Gagne, Nicole A. Doria-Rose, and Mario Roederer

Subjects

T cell, T cells, General Biochemistry, Genetics and Molecular Biology, Virus, Article, Immune system, antibody, medicine, anamnestic, B cells, biology, medicine.diagnostic_test, SARS-CoV-2, COVID-19, respiratory system, Vaccine efficacy, respiratory tract diseases, Vaccination, Titer, Bronchoalveolar lavage, medicine.anatomical_structure, mRNA vaccine, Delta, Immunology, biology.protein, mucosal immunity, Antibody

Abstract

mRNA-1273 vaccine efficacy against SARS-CoV-2 Delta wanes over time; however, there are limited data on the impact of durability of immune responses on protection. Here, we immunized rhesus macaques and assessed immune responses over one year in blood, upper and lower airways. Serum neutralizing titers to Delta were 280 and 34 reciprocal ID50 at weeks 6 (peak) and 48 (challenge), respectively. Antibody binding titers also decreased in bronchoalveolar lavage (BAL). Four days after Delta challenge, virus was unculturable in BAL and subgenomic RNA declined by ∼3-log10 compared to control animals. In nasal swabs, sgRNA was reduced by 1-log10 and virus remained culturable. Anamnestic antibodies (590-fold increased titer) but not T cell responses were detected in BAL by day 4 post-challenge. mRNA-1273-mediated protection in the lungs is durable but delayed and potentially dependent on anamnestic antibody responses. Rapid and sustained protection in upper and lower airways may eventually require a boost., A study looking at the immunity against the SARS-CoV-2 delta variant one year after mRNA vaccination founds a durable but delayed anamnestic antibody responses in the lung but limited protection in the upper airway and low neutralizing responses, thus advocating for booster shots for durable upper and lower airway immunity.

Published

2021

8. Protection from SARS-CoV-2 Delta one year after mRNA-1273 vaccination in nonhuman primates is coincident with an anamnestic antibody response in the lower airway

Author

Wei Shi, Daniel C. Douek, Kevin W. Bock, Barbara J. Flynn, Juan I. Moliva, Saule T. Nurmukhambetova, Prakriti Mudvari, Laurent Pessaint, Darin K. Edwards, Elizabeth McCarthy, John R. Mascola, Lauren McCormick, Alan Dodson, Jesmine Roberts-Torres, Ian N. Moore, Mahnaz Minai, John-Paul Todd, Swagata Kar, Hanne Leth Andersen, Danielle A. Wagner, Barney S. Graham, Kathryn E. Foulds, Bianca M. Nagata, Anne P. Werner, Cynthia G. Lorang, Adrienne Goode, Eun Sung Yang, Mehul S. Suthar, Lingshu Wang, Bingchun Zhao, Shayne F. Andrew, Martha Nason, Aurélie Ploquin, Meredith E. Davis-Gardner, Eli Boritz, Andrea Carfi, Robert A. Seder, Anthony L. Cook, Matthew Gagne, Nicole A. Doria-Rose, Mario Roederer, Christopher Cole Honeycutt, Nancy J. Sullivan, Farida Laboune, Kizzmekia S. Corbett, Mark G. Lewis, Courtney Tucker, and Seyhan Boyoglu-Barnum

Subjects

medicine.diagnostic_test, business.industry, T cell, respiratory system, Vaccine efficacy, Virus, Vaccination, Titer, Bronchoalveolar lavage, Immune system, medicine.anatomical_structure, Immunology, medicine, business, Subgenomic mRNA

Abstract

mRNA-1273 vaccine efficacy against SARS-CoV-2 Delta wanes over time; however, there are limited data on the impact of durability of immune responses on protection. We immunized rhesus macaques at weeks 0 and 4 and assessed immune responses over one year in blood, upper and lower airways. Serum neutralizing titers to Delta were 280 and 34 reciprocal ID50 at weeks 6 (peak) and 48 (challenge), respectively. Antibody binding titers also decreased in bronchoalveolar lavage (BAL). Four days after challenge, virus was unculturable in BAL and subgenomic RNA declined ∼3-log10 compared to control animals. In nasal swabs, sgRNA declined 1-log10 and virus remained culturable. Anamnestic antibody responses (590-fold increase) but not T cell responses were detected in BAL by day 4 post-challenge. mRNA-1273-mediated protection in the lungs is durable but delayed and potentially dependent on anamnestic antibody responses. Rapid and sustained protection in upper and lower airways may eventually require a boost.

Published

2021

9. Protection against SARS-CoV-2 Beta Variant in mRNA-1273 Boosted Nonhuman Primates

Author

Daniel C. Douek, Rachel L. Davis, Alex Van Ry, Timothy S. Johnston, Stephen D. Schmidt, Adrian B. McDermott, John R. Mascola, Yi Zhang, Anne P. Werner, Lilin Lai, Evan Lamb, Sarah O’ Connell, Kevin W. Bock, John-Paul Todd, Misook Choe, Amy R. Henry, Wei Shi, Alan Dodson, Danielle A. Wagner, Matthew A. Koch, Barney S. Graham, Aurélie Ploquin, Mehul S. Suthar, Farida Laboune, Chaim A. Schramm, Mitzi M. Donaldson, Samantha J. Provost, John Misasi, Christopher Stringham, Bianca M. Nagata, Hanne Leth Andersen, Ian N. Moore, Kizzmekia S. Corbett, Andrea Carfi, Robert A. Seder, Sandeep Narpala, Seyhan Boyoglu-Barnum, Mark G. Lewis, Josue Marquez, Sijy O'Dell, Nancy J. Sullivan, Lingshu Wang, Juan I. Moliva, Saule T. Nurmukhambetova, Courtney Tucker, Zackery Flinchbaugh, Laurent Pessaint, Shayne F. Andrew, Mahnaz Minai, Eli Boritz, Barbara J. Flynn, Andrew Pekosz, Dillon R. Flebbe, Daniel Valentin, Darin K. Edwards, Matthew Gagne, Angela Choi, Manjari Sriparna, Kathryn E. Foulds, Martha Nason, Anthony L. Cook, Gabriela S. Alvarado, Kai Wu, Nicole A. Doria-Rose, and Mario Roederer

Subjects

2019-20 coronavirus outbreak, COVID-19 Vaccines, Coronavirus disease 2019 (COVID-19), T Follicular Helper Cells, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunization, Secondary, Heterologous, Vaccine Efficacy, Biology, Nose, Antibodies, Viral, Virus Replication, Article, Immune system, Immunogenicity, Vaccine, Memory B Cells, Immunity, Animals, Beta (finance), Neutralizing antibody, Immunity, Mucosal, Messenger RNA, Multidisciplinary, SARS-CoV-2, COVID-19, Th1 Cells, Virology, Antibodies, Neutralizing, Macaca mulatta, Vaccination, Titer, Viral replication, biology.protein, RNA, Viral, Bronchoalveolar Lavage Fluid, 2019-nCoV Vaccine mRNA-1273

Abstract

Neutralizing antibody responses gradually wane after vaccination with mRNA-1273 against several variants of concern (VOC), and additional boost vaccinations may be required to sustain immunity and protection. Here, we evaluated the immune responses in nonhuman primates that received 100 µg of mRNA-1273 vaccine at 0 and 4 weeks and were boosted at week 29 with mRNA-1273 (homologous) or mRNA-1273.β (heterologous), which encompasses the spike sequence of the B.1.351 (beta or β) variant. Reciprocal ID50pseudovirus neutralizing antibody geometric mean titers (GMT) against live SARS-CoV-2 D614G and the β variant, were 4700 and 765, respectively, at week 6, the peak of primary response, and 644 and 553, respectively, at a 5-month post-vaccination memory time point. Two weeks following homologous or heterologous boost β-specific reciprocal ID50GMT were 5000 and 3000, respectively. At week 38, animals were challenged in the upper and lower airway with the β variant. Two days post-challenge, viral replication was low to undetectable in both BAL and nasal swabs in most of the boosted animals. These data show that boosting with the homologous mRNA-1273 vaccine six months after primary immunization provides up to a 20-fold increase in neutralizing antibody responses across all VOC, which may be required to sustain high-level protection against severe disease, especially for at-risk populations.One-sentence summarymRNA-1273 boosted nonhuman primates have increased immune responses and are protected against SARS-CoV-2 beta infection.

Published

2021

10. Les vecteurs AAV pour le transfert de gène in vivo ou comment un petit virus devient grand

Author

Rachel, Millet, Axel, Rossi, Aurélie, Ploquin, Alberto L, Epstein, Anna, Greco, and Anna, Salvetti

Abstract

Among the variety of viral vectors, those derived from the human parvovirus Adeno-Associated Virus (AAV) have emerged as a very efficient tool for in vivo gene transfer into a variety of tissues and animal species during the two last decades. The relative simplicity of the organization of the AAV genome and the non-pathogenic property of the parental AAV has greatly contributed to the use of this viral vector among the gene transfer community. However, the limited knowledge of the wild type (wt) virus compared to other viral vectors has required considerable efforts to gain insight into wt AAV biology in order to improve the AAV vector system for therapy. This review will summarize the most important features of both wt and recombinant AAV to show how the increased understanding of the biology of the virus has enabled AAV vectors to lead the in vivo gene transfer field.

Published

2020

11. Functional Interrogation and Mining of Natively-Paired Human VH:VL Antibody Repertoires

Author

M. Anthony Moody, Aaron G. Schmidt, John Misasi, Wing Pui Kong, Bo Wang, Farida Laboune, John R. Mascola, George Georgiou, Chang W. Choi, Alberto Cagigi, Eun Sung Yang, Nancy J. Sullivan, Morgan R. Timm, Kwanyee Leung, Daniel C. Douek, Rui Kong, Julie E. Ledgerwood, Ahmed S. Fahad, Barney S. Graham, David R. Ambrozak, Jonathan R. McDaniel, Elise G. Viox, Erica Normandin, Brandon J. DeKosky, Jiwon Lee, Thomas Niezold, George Delidakis, Amy R. Henry, Aurélie Ploquin, Mark Connors, Leigh Kendra Elizabeth, Andrew D. Ellington, and William N. Voss

Subjects

0301 basic medicine, Biomedical Engineering, Hemagglutinin (influenza), Bioengineering, HIV Infections, Yeast display, HIV Antibodies, medicine.disease_cause, Applied Microbiology and Biotechnology, Article, 03 medical and health sciences, 0302 clinical medicine, Peptide Library, medicine, Humans, Amino Acid Sequence, Peptide library, chemistry.chemical_classification, B-Lymphocytes, Ebola virus, biology, virus diseases, Antibodies, Monoclonal, High-Throughput Nucleotide Sequencing, Amplicon, Virology, Antibodies, Neutralizing, 3. Good health, 030104 developmental biology, chemistry, 030220 oncology & carcinogenesis, biology.protein, HIV-1, Molecular Medicine, Surface expression, Antibody, Glycoprotein, Biotechnology

Abstract

We present a technology to screen millions of B cells for natively paired human antibody repertoires. Libraries of natively paired, variable region heavy and light (VH:VL) amplicons are expressed in a yeast display platform that is optimized for human Fab surface expression. Using our method we identify HIV-1 broadly neutralizing antibodies (bNAbs) from an HIV-1 slow progressor and high-affinity neutralizing antibodies against Ebola virus glycoprotein and influenza hemagglutinin.

Published

2018

12. Chimpanzee Adenovirus Vector Ebola Vaccine

Author

Julie E, Ledgerwood, Adam D, DeZure, Daphne A, Stanley, Emily E, Coates, Laura, Novik, Mary E, Enama, Nina M, Berkowitz, Zonghui, Hu, Gyan, Joshi, Aurélie, Ploquin, Sandra, Sitar, Ingelise J, Gordon, Sarah A, Plummer, LaSonji A, Holman, Cynthia S, Hendel, Galina, Yamshchikov, Francois, Roman, Alfredo, Nicosia, Stefano, Colloca, Riccardo, Cortese, Robert T, Bailer, Richard M, Schwartz, Mario, Roederer, John R, Mascola, Richard A, Koup, Nancy J, Sullivan, Barney S, Graham, and Sarah, Romano

Subjects

Adult, Male, 0301 basic medicine, Fever, Pan troglodytes, T-Lymphocytes, Genetic Vectors, Simian, Antibodies, Viral, medicine.disease_cause, 03 medical and health sciences, Animals, Humans, Medicine, Vector (molecular biology), Ebola Vaccines, Glycoproteins, Ebolavirus, Ebola virus, Ebola vaccine, biology, business.industry, Immunogenicity, General Medicine, Hemorrhagic Fever, Ebola, Middle Aged, biology.organism_classification, Antibodies, Neutralizing, Virology, Vaccination, Clinical trial, 030104 developmental biology, Immunology, Adenoviruses, Simian, business

Abstract

BackgroundThe unprecedented 2014 epidemic of Ebola virus disease (EVD) prompted an international response to accelerate the availability of a preventive vaccine. A replication-defective recombinant chimpanzee adenovirus type 3–vectored ebolavirus vaccine (cAd3-EBO), encoding the glycoprotein from Zaire and Sudan species, that offers protection in the nonhuman primate model, was rapidly advanced into phase 1 clinical evaluation. MethodsWe conducted a phase 1, dose-escalation, open-label trial of cAd3-EBO. Twenty healthy adults, in sequentially enrolled groups of 10 each, received vaccination intramuscularly in doses of 2×1010 particle units or 2×1011 particle units. Primary and secondary end points related to safety and immunogenicity were assessed throughout the first 8 weeks after vaccination; in addition, longer-term vaccine durability was assessed at 48 weeks after vaccination. ResultsIn this small study, no safety concerns were identified; however, transient fever developed within 1 day after vaccinat...

Published

2017

13. ADENO-ASSOCIATED VIRUS (AAV) VECTORS

Author

Anna Salvetti, Aurélie Ploquin, and Hildegard Büning

Subjects

medicine, Biology, medicine.disease_cause, Virology, Adeno-associated virus

Published

2019

14. Protective monotherapy against lethal Ebola virus infection by a potently neutralizing antibody

Author

Masaru Kanekiyo, Ryan P. Staupe, Julie E. Ledgerwood, Elisabetta Cameroni, Chiara Silacci, Aurélie Ploquin, Jean-jacques Muyembe-Tamfun, John C. Trefry, Davide Corti, John Misasi, Gloria Agatic, Wei Shi, John R. Mascola, Laurent Perez, Sabue Mulangu, Neville K. Kisalu, Antonio Lanzavecchia, Ingelise J. Gordon, Emily A. Thompson, Barney S. Graham, Suzanne E. Wollen, Blanca Fernandez-Rodriguez, Federica Sallusto, Fabrizia Vanzetta, Nicole A. Doria-Rose, Misook Choe, Michael Bailey, Alberto Cagigi, Nancy J. Sullivan, Daphne A. Stanley, and Hadar Marcus

Subjects

Adult, Male, 0301 basic medicine, medicine.drug_class, viruses, Molecular Sequence Data, 030106 microbiology, Disease, Biology, ZMapp, Antibodies, Viral, medicine.disease_cause, Monoclonal antibody, Virus, Disease Outbreaks, 03 medical and health sciences, medicine, Animals, Humans, Survivors, Neutralizing antibody, Clinical Trials as Topic, Multidisciplinary, Ebola virus, Antibodies, Monoclonal, Outbreak, Hemorrhagic Fever, Ebola, Ebolavirus, Antibodies, Neutralizing, Virology, 030104 developmental biology, Immunology, biology.protein, Macaca, Female, Antibody, medicine.drug

Abstract

Antibodies block Ebola virus entry The recent Ebola virus outbreak in West Africa illustrates the need for both an effective vaccine and therapies to treat infected individuals. Corti et al. isolated two monoclonal antibodies from a survivor of the 1995 Kikwit outbreak and demonstrated their therapeutic efficacy in Ebola virus–infected macaques. In fact, one antibody protected macaques when it was given up to 5 days after infection. Misasi et al. solved the crystal structures of fragments of the two antibodies bound to the Ebola virus glycoprotein (GP), which mediates viral cell entry. The two antibodies targeted different regions of GP, but in both cases blocked steps required for viral entry. Science , this issue pp. 1339 & 1343

Published

2016

15. Vaccine-Mediated Induction of an Ebolavirus Cross-Species Antibody Binding to Conserved Epitopes on the Glycoprotein Heptad Repeat 2/Membrane-Proximal External Junction

Author

Thomas Niezold, Nancy J. Sullivan, Yan Zhou, Aurélie Ploquin, John Misasi, Yaroslav Tsybovsky, and Alberto Cagigi

Subjects

0301 basic medicine, Immunogen, Supplement Articles, Cross Reactions, medicine.disease_cause, Antibodies, Viral, Epitope, 03 medical and health sciences, Epitopes, 0302 clinical medicine, medicine, Immunology and Allergy, Animals, Ebola Vaccines, Receptor, chemistry.chemical_classification, Ebolavirus, Ebola virus, Membrane Glycoproteins, biology, Chemistry, Vaccination, Virology, Heptad repeat, Macaca fascicularis, 030104 developmental biology, Infectious Diseases, biology.protein, Antibody, Glycoprotein, 030217 neurology & neurosurgery

Abstract

The membrane-proximal external regions (MPER) of the human immunodeficiency virus envelope glycoprotein (GP) generate broadly reactive antibody responses and are the focus of vaccine development efforts. The conservation of amino acids within filovirus GP heptad repeat region (HR)2/MPER suggests that it may also represent a target for a pan-filovirus vaccine. We immunized a cynomolgus macaque against Ebola virus (EBOV) using a deoxyribonucleic acid/adenovirus 5 prime/boost strategy, sequenced memory B-cell receptors, and tested the antibodies for functional activity against EBOV GP. Antibody ma-C10 bound to GP with an affinity of 48 nM and was capable of inducing antibody-dependent cellular cytotoxicity. Three-dimensional reconstruction of single-particle, negative-stained, electron microscopy showed that ma-C10 bound to the HR2/MPER, and enzyme-linked immunosorbent assay reveals it binds to residues 621-631. More importantly, ma-C10 was found to bind to the GP of the 3 most clinically relevant Ebolavirus species, suggesting that a cross-species immunogen strategy targeting the residues in this region may be a feasible approach for producing a pan-filovirus vaccine.

Published

2018

16. Vaccine Generation of Protective Ebola Antibodies and Identification of Conserved B-Cell Signatures

Author

Alberto Cagigi, Mario Roederer, David R. Ambrozak, John Misasi, Yaroslav Tsybovsky, Daphne A. Stanley, Nancy J. Sullivan, Rosemarie D. Mason, and Aurélie Ploquin

Subjects

0301 basic medicine, Zaire ebolavirus, medicine.drug_class, Supplement Articles, Biology, medicine.disease_cause, Monoclonal antibody, Antibodies, Viral, Macaque, 03 medical and health sciences, 0302 clinical medicine, Antigen, Viral Envelope Proteins, biology.animal, medicine, Immunology and Allergy, Animals, Humans, Ebola Vaccines, B-Lymphocytes, Ebola virus, Vaccination, Antibodies, Monoclonal, Hydrogen-Ion Concentration, Ebolavirus, Virology, Antibodies, Neutralizing, Macaca fascicularis, 030104 developmental biology, Infectious Diseases, Immunization, 030220 oncology & carcinogenesis, biology.protein, Antibody

Abstract

We recently identified a single potently neutralizing monoclonal antibody (mAb), mAb114, isolated from a human survivor of natural Zaire ebolavirus (EBOV) infection, which fully protects nonhuman primates (NHPs) against lethal EBOV challenge. To evaluate the ability of vaccination to generate mAbs such as mAb114, we cloned antibodies from NHPs vaccinated with vectors encoding the EBOV glycoprotein (GP). We identified 14 unique mAbs with potent binding to GP, 4 of which were neutralized and had the functional characteristics of mAb114. These vaccine-induced macaque mAbs share many sequence similarities with mAb114 and use the same mAb114 VH gene (ie, IGHV3-13) when classified using the macaque IMGT database. The antigen-specific VH-gene repertoire present after each immunization indicated that IGHV3-13 mAbs populate an EBOV-specific B-cell repertoire that appears to become more prominent with subsequent boosting. These findings will support structure-based vaccine design aimed at enhanced induction of antibodies such as mAb114.

Published

2018

17. Ebola Vaccines

Author

Nancy J. Sullivan, Kendra E. Leigh, and Aurélie Ploquin

Subjects

Ebola vaccine, Biology, Virology

Published

2018

18. Contributors

Author

Sergio Abrignani, S. Sohail Ahmed, Ian J. Amanna, Teresa A. Anderson, Peter R. Arlett, William L. Atkinson, Francisco M. Averhoff, R. Bruce Aylward, Martin F. Bachmann, Carol J. Baker, Henry H. Balfour, W. Ripley Ballou, Ralph S. Baric, Alan D.T. Barrett, Elizabeth D. Barnett, Lahouari Belgharbi, Elliot M. Berinstein, Neil L. Berinstein, Jeffrey M. Bethony, Hugues Bogaerts, Adrian Bot, Philip S. Brachman, Joseph S. Bresee, Alireza Khadem Broojerdi, Arthur L. Caplan, Marco Cavaleri, Thomas Cherian, Pele Choi-Sing, John D. Clemens, Stephen L. Cochi, Amanda Cohn, Capt. Margaret M. Cortese, Nancy J. Cox, Felicity Cutts, Ron Dagan, Harry R. Dalton, Robert S. Daum, Andrea Sudell Davey, Raffaele De Francesco, Kari Debbink, Michael D. Decker, Sachin N. Desai, Frank DeStefano, R. Gordon Douglas, Katrin Dubischar, W. John Edmunds, Kathryn M. Edwards, William Egan, Rudolf Eggers, Falk Ehmann, Ronald W. Ellis, Aadil El-Turabi, Dean D. Erdman, Hildegund Ertl, Paul E.M. Fine, Theresa M. Finn, Allison Fisher, Martin Friede, Arthur M. Friedlander, Alicia M. Fry, Nathalie Garçon, Paul A. Gastañaduy, Mark D. Gershman, Anne A. Gershon, Bradford D. Gessner, Peter Gilbert, Ann M. Ginsberg, Marc P. Girard, Phillip L. Gomez, James L. Goodson, Robert R. Goodwin, Lance K. Gordon, John D. Grabenstein, Barney S. Graham, Rachel L. Graham, Dan M. Granoff, Gregory C. Gray, Marion F. Gruber, Scott B. Halstead, Willem Hanekom, Lee H. Harrison, Thomas R. Hawn, C. Mary Healy, Donald A. Henderson, Allan Hildesheim, Susan L. Hills, Jan Holmgren, Joachim Hombach, Peter J. Hotez, Michael Houghton, Avril Melissa Houston, Barbara J. Howe, Jacques Izopet, Denise J. Jamieson, Courtney Jarrahian, Kari Johansen, Ruth A. Karron, Richard B. Kennedy, Olen M. Kew, Yury Khudyakov, Michel Klein, Keith P. Klugman, Jacob F. Kocher, Wayne C. Koff, Herwig Kollaritsch, Karen L. Kotloff, Phyllis E. Kozarsky, Andrew T. Kroger, Xavier Kurz, Seema S. Lakdawala, J. Michael Lane, Kendra Leigh, Myron J. Levin, Emily Marcus Levine, Myron M. Levine, Lisa C. Lindesmith, Per Ljungman, Douglas R. Lowy, Catherine J. Luke, Anna Lundgren, Patrick Lydon, Richard Malley, Mona Marin, Lauri E. Markowitz, Lieut. Valerie B. Marshall, Mark A. Miller, Thomas P. Monath, William J. Moss, Kim Mulholland, Daniel M. Musher, Gary J. Nabel, Thirumeni Nagarajan, GB Nair, Srinivas Acharya Nanduri, Petra Neddermann, Noele P. Nelson, Paul A. Offit, Jean-Marie Okwo-Bele, Saad B. Omer, Walter A. Orenstein, Petra C.F. Oyston, Mark J. Papania, Umesh D. Parashar, Dina Pfeifer, Larry K. Pickering, Phillip R. Pittman, Aurélie Ploquin, Stanley A. Plotkin, Susan L. Plotkin, Gregory A. Poland, Andrew J. Pollard, Firdausi Qadri, Mary R. Quirk, Raman D.S.V. Rao, Rino Rappuoli, Susan E. Reef, Alison D. Ridpath, James M. Robinson, Lance E. Rodewald, Carmen A. Rodriguez-Hernandez, Martha H. Roper, Steven A. Rubin, Charles E. Rupprecht, William A. Rutala, David Salisbury, Vijay B. Samant, Suryaprakash Sambhara, Mathuram Santosham, John T. Schiller, Mark R. Schleiss, Anne Schuchat, Jason L. Schwartz, Heather M. Scobie, J. Anthony Scott, Jane F. Seward, Daniel Shouval, Claire-Anne Siegrist, Mark K. Slifka, Samir V. Sodha, Lawrence R. Stanberry, J. Erin Staples, Allen C. Steere, Robert Steffen, Peter M. Strebel, Kanta Subbarao, Nancy J. Sullivan, Catherine G. Sutcliffe, Andrea R. Sutherland, Roland W. Sutter, Stephen J. Thomas, Tejpratap S.P Tiwari, Theodore F. Tsai, Pierre Van Damme, Johan Vekemans, Emmanuel Vidor, John W. Ward, Steven G.F. Wassilak, David J. Weber, David B. Weiner, Deborah L. Wexler, Melinda Wharton, Cynthia G. Whitney, E. Diane Williamson, David J. Wood, Ningshao Xia, Zhi Yi Xu, Alessandro Zanetti, and Darin Zehrung

Published

2018

19. Dissociation of skeletal muscle for flow cytometric characterization of immune cells in macaques

Author

Aurélie Ploquin, Karin Loré, Gustaf Lindgren, José DelaO Hernández, Daphne A. Stanley, Hugues Fausther-Bovendo, Frank Liang, Richard A. Koup, Aiala Salvador Martinez, Nancy J. Sullivan, and Jason M. Brenchley

Subjects

Muscle tissue, Neutrophils, Immunology, Cell, Biology, Article, Monocytes, Flow cytometry, Immune system, In vivo, medicine, Animals, Immunology and Allergy, Myocyte, Lymphocytes, Muscle, Skeletal, Vaccines, medicine.diagnostic_test, Macrophages, Skeletal muscle, Dendritic Cells, Dendritic cell, Flow Cytometry, medicine.anatomical_structure, Macaca

Abstract

The majority of vaccines and several treatments are administered by intramuscular injection. The aim is to engage and activate immune cells, although they are rare in normal skeletal muscle. The phenotype and function of resident as well as infiltrating immune cells in the muscle after injection are largely unknown. While methods for obtaining and characterizing murine muscle cell suspensions have been reported, protocols for nonhuman primates (NHPs) have not been well defined. NHPs comprise important in vivo models for studies of immune cell function due to their high degree of resemblance with humans. In this study, we developed and systematically compared methods to collect vaccine-injected muscle tissue to be processed into single cell suspensions for flow cytometric characterization of immune cells. We found that muscle tissue processed by mechanical disruption alone resulted in significantly lower immune cell yields compared to enzymatic digestion using Liberase. Dendritic cell subsets, monocytes, macrophages, neutrophils, B cells, T cells and NK cells were readily detected in the muscle by the classical human markers. The methods for obtaining skeletal muscle cell suspension established here offer opportunities to increase the understanding of immune responses in the muscle, and provides a basis for defining immediate post-injection vaccine responses in primates.

Published

2015

20. Ebola Immunity: Gaining a Winning Position in Lightning Chess

Author

Nancy J. Sullivan, Aurélie Ploquin, and Yan Zhou

Subjects

0301 basic medicine, Zaire ebolavirus, Transmission (medicine), Immunology, Disease, Biology, Hemorrhagic Fever, Ebola, medicine.disease_cause, Pathogenicity, Antibodies, Viral, Ebolavirus, Virology, Genus Ebolavirus, West africa, 03 medical and health sciences, 030104 developmental biology, Immune system, Immunity, Host-Pathogen Interactions, medicine, Immunology and Allergy, Animals, Humans

Abstract

Zaire ebolavirus (EBOV), one of five species in the genus Ebolavirus, is the causative agent of the hemorrhagic fever disease epidemic that claimed more than 11,000 lives from 2014 to 2016 in West Africa. The combination of EBOV’s ability to disseminate broadly and rapidly within the host and its high pathogenicity pose unique challenges to the human immune system postinfection. Potential transmission from apparently healthy EBOV survivors reported in the recent epidemic raises questions about EBOV persistence and immune surveillance mechanisms. Clinical, virological, and immunological data collected since the West Africa epidemic have greatly enhanced our knowledge of host–virus interactions. However, critical knowledge gaps remain in our understanding of what is necessary for an effective host immune response for protection against, or for clearance of, EBOV infection. This review provides an overview of immune responses against EBOV and discusses those associated with the success or failure to control EBOV infection.

Published

2017

21. Functional Interrogation and Mining of Natively-Paired Human VH:VL Antibody Repertoires

Author

Brandon J. DeKosky, Bo Wang, Morgan Timm, Jiwon Lee, Erica Normandin, John Misasi, Rui Kong, Jonathan R. McDaniel, George Delidakis, Kendra E. Leigh, Thomas Niezold, Aurélie Ploquin, Elise G. Viox, Ahmed Fahad, Alberto Cagigi, Kwanyee Leung, Eun Sung Yang, Wing-Pui Kong, William Voss, Aaron G. Schmidt, M. Anthony Moody, David Ambrozak, Amy R. Henry, Farida Laboune, Julie E. Ledgerwood, Barney S. Graham, Mark Connors, Daniel C. Douek, Nancy Sullivan, Andrew D. Ellington, and George Georgiou

Subjects

Immunology, Immunology and Allergy

Abstract

Next-Generation sequencing has become an essential tool in the analysis of antibody responses in the settings of health, vaccination, and disease. However, immune receptors comprise two chains encoded by separate mRNA strands, and conventional NextGen sequencing fails to identify the native pairings encoded by individual lymphocytes. To overcome this limitation we have applied recent technical advances in high-throughput sequencing and functional analysis of complete antibodies (i.e., paired heavy and light chain sequencing) to generate a comprehensive understanding of the antibody response to vaccination and natural infection. Here we present a new technology to screen natively-paired human antibody repertoires from millions of B cells. Libraries of natively-paired variable region heavy and light (VH:VL) amplicons were expressed in a yeast display platform that was optimized for human Fab surface expression, and the resulting libraries were interrogated for binding to viral vaccine antigens via FACS paired with next generation sequencing. Using our method we identified HIV-1 broadly neutralizing antibodies (bNAbs) from an HIV-1 slow progressor and high-affinity neutralizing antibodies responding to an Ebola virus glycoprotein vaccination. These next-generation approaches are providing detailed molecular feedback on immune receptor responses and are informing the design and discovery of new vaccines and therapeutics.

Published

2018

22. Safety and immunogenicity of a chimpanzee adenovirus-vectored Ebola vaccine in healthy adults: a randomised, double-blind, placebo-controlled, dose-finding, phase 1/2a study

Author

Olivier Tshiani Mbaya, Camille Cochet, Grégoire Wuerzner, Olga De Santis, Nancy J. Sullivan, Robert T. Bailer, Marie Paule Kieny, Iris De Ryck, Régine Audran, Barney S. Graham, Loane Warpelin-Decrausaz, Laure Vallotton, Carole Mayor, Aurélie Ploquin, Vasee S. Moorthy, W. Ripley Ballou, Anne Christine Thierry, Viviane Steiner-Monard, Emilie Pothin, François Spertini, François Roman, Blaise Genton, Yan Zhou, Daniel Estoppey, and Sophie Lonchampt

Subjects

0301 basic medicine, Adult, Male, medicine.medical_specialty, Fever, Dose-Response Relationship, Immunologic, Placebo, Antibodies, Viral, law.invention, Adenoviridae, 03 medical and health sciences, Young Adult, Randomized controlled trial, law, Internal medicine, medicine, Vaccines, DNA, Humans, Seroconversion, Ebola Vaccines, Adverse effect, Intention-to-treat analysis, Ebola vaccine, business.industry, Hemorrhagic Fever, Ebola, Middle Aged, Ebolavirus, 3. Good health, Surgery, Vaccination, Clinical trial, 030104 developmental biology, Infectious Diseases, Military Personnel, Immunoglobulin G, Female, business

Abstract

Summary Background The ongoing Ebola outbreak led to accelerated efforts to test vaccine candidates. On the basis of a request by WHO, we aimed to assess the safety and immunogenicity of the monovalent, recombinant, chimpanzee adenovirus type-3 vector-based Ebola Zaire vaccine (ChAd3-EBO-Z). Methods We did this randomised, double-blind, placebo-controlled, dose-finding, phase 1/2a trial at the Centre Hospitalier Universitaire Vaudois, Lausanne, Switzerland. Participants (aged 18–65 years) were randomly assigned (2:2:1), via two computer-generated randomisation lists for individuals potentially deployed in endemic areas and those not deployed, to receive a single intramuscular dose of high-dose vaccine (5 × 10 10 viral particles), low-dose vaccine (2·5 × 10 10 viral particles), or placebo. Deployed participants were allocated to only the vaccine groups. Group allocation was concealed from non-deployed participants, investigators, and outcome assessors. The safety evaluation was not masked for potentially deployed participants, who were therefore not included in the safety analysis for comparison between the vaccine doses and placebo, but were pooled with the non-deployed group to compare immunogenicity. The main objectives were safety and immunogenicity of ChAd3-EBO-Z. We did analysis by intention to treat. This trial is registered with ClinicalTrials.gov, number NCT02289027. Findings Between Oct 24, 2014, and June 22, 2015, we randomly assigned 120 participants, of whom 18 (15%) were potentially deployed and 102 (85%) were non-deployed, to receive high-dose vaccine (n=49), low-dose vaccine (n=51), or placebo (n=20). Participants were followed up for 6 months. No vaccine-related serious adverse events were reported. We recorded local adverse events in 30 (75%) of 40 participants in the high-dose group, 33 (79%) of 42 participants in the low-dose group, and five (25%) of 20 participants in the placebo group. Fatigue or malaise was the most common systemic adverse event, reported in 25 (62%) participants in the high-dose group, 25 (60%) participants in the low-dose group, and five (25%) participants in the placebo group, followed by headache, reported in 23 (57%), 25 (60%), and three (15%) participants, respectively. Fever occurred 24 h after injection in 12 (30%) participants in the high-dose group and 11 (26%) participants in the low-dose group versus one (5%) participant in the placebo group. Geometric mean concentrations of IgG antibodies against Ebola glycoprotein peaked on day 28 at 51 μg/mL (95% CI 41·1–63·3) in the high-dose group, 44·9 μg/mL (25·8–56·3) in the low-dose group, and 5·2 μg/mL (3·5–7·6) in the placebo group, with respective response rates of 96% (95% CI 85·7–99·5), 96% (86·5–99·5), and 5% (0·1–24·9). Geometric mean concentrations decreased by day 180 to 25·5 μg/mL (95% CI 20·6–31·5) in the high-dose group, 22·1 μg/mL (19·3–28·6) in the low-dose group, and 3·2 μg/mL (2·4–4·9) in the placebo group. 28 (57%) participants given high-dose vaccine and 31 (61%) participants given low-dose vaccine developed glycoprotein-specific CD4 cell responses, and 33 (67%) and 35 (69%), respectively, developed CD8 responses. Interpretation ChAd3-EBO-Z was safe and well tolerated, although mild to moderate systemic adverse events were common. A single dose was immunogenic in almost all vaccine recipients. Antibody responses were still significantly present at 6 months. There was no significant difference between doses for safety and immunogenicity outcomes. This acceptable safety profile provides a reliable basis to proceed with phase 2 and phase 3 efficacy trials in Africa. Funding Swiss State Secretariat for Education, Research and Innovation (SERI), through the EU Horizon 2020 Research and Innovation Programme.

Published

2015

23. Chimpanzee Adenovirus Vector Ebola Vaccine--Preliminary Report

Author

Riccardo Cortese, Adam DeZure, Nancy J. Sullivan, Sarah A. Plummer, Zonghui Hu, John R. Mascola, Abstr Act, Mario Roederer, Daphne A. Stanley, Mary E. Enama, Barney S. Graham, Cynthia S. Hendel, Alfredo Nicosia, Sandra Sitar, Ingelise J. Gordon, Richard M. Schwartz, Aurélie Ploquin, Richard A. Koup, Julie E. Ledgerwood, Robert T. Bailer, Gyan Joshi, François Roman, Stefano Colloca, Nina M. Berkowitz, Galina Yamshchikov, LaSonji A. Holman, and Laura Novik

Subjects

Ebolavirus, medicine.medical_specialty, Ebola virus, Reactogenicity, Ebola vaccine, Pan troglodytes, business.industry, Immunogenicity, Genetic Vectors, General Medicine, Hemorrhagic Fever, Ebola, medicine.disease_cause, Adenoviridae, Vaccination, Clinical trial, Titer, Internal medicine, medicine, Adenoviruses, Simian, Animals, Humans, Ebola Vaccines, business

Abstract

Background The unprecedented 2014 epidemic of Ebola virus disease (EVD) has prompted an international response to accelerate the availability of a preventive vaccine. A replicationdefective recombinant chimpanzee adenovirus type 3–vectored ebolavirus vaccine (cAd3-EBO), encoding the glycoprotein from Zaire and Sudan species that offers protection in the nonhuman primate model, was rapidly advanced into phase 1 clinical evaluation. Methods We conducted a phase 1, dose-escalation, open-label trial of cAd3-EBO. Twenty healthy adults, in sequentially enrolled groups of 10 each, received vaccination intramuscularly in doses of 2×10 10 particle units or 2×10 11 particle units. Primary and secondary end points related to safety and immunogenicity were assessed throughout the first 4 weeks after vaccination. Results In this small study, no safety concerns were identified; however, transient fever developed within 1 day after vaccination in two participants who had received the 2×10 11 particle-unit dose. Glycoprotein-specific antibodies were induced in all 20 participants; the titers were of greater magnitude in the group that received the 2×10 11 particle-unit dose than in the group that received the 2×10 10 particle-unit dose (geometric mean titer against the Zaire antigen, 2037 vs. 331; P = 0.001). Glycoproteinspecific T-cell responses were more frequent among those who received the 2x10 11 particle-unit dose than among those who received the 2×10 10 particle-unit dose, with a CD4 response in 10 of 10 participants versus 3 of 10 participants (P = 0.004) and a CD8 response in 7 of 10 participants versus 2 of 10 participants (P = 0.07). Conclusions Reactogenicity and immune responses to cAd3-EBO vaccine were dose-dependent. At the 2×10 11 particle-unit dose, glycoprotein Zaire–specific antibody responses were in the range reported to be associated with vaccine-induced protective immunity in challenge studies involving nonhuman primates. Clinical trials assessing cAd3-EBO are ongoing. (Funded by the Intramural Research Program of the National Institutes of Health; VRC 207 ClinicalTrials.gov number, NCT02231866.)

Published

2015

24. 10: ADENO-ASSOCIATED VIRUS (AAV) VECTORS

Author

Hildegard Büning, Aurélie Ploquin, and Anna Salvetti

Subjects

Self-complementary adeno-associated virus (scAAV), medicine, Biology, medicine.disease_cause, Virology, Adeno-associated virus

Published

2014

25. Protection against henipavirus infection by use of recombinant adeno-associated virus-vector vaccines

Author

Véronique Barateau, Kum Thong Wong, François-Loïc Cosset, Cyrille Mathieu, Judith Szécsi, Aurélie Ploquin, Branka Horvat, Anna Salvetti, Kien Chai Ong, Vanessa Guillaume, Virologie humaine, École normale supérieure - Lyon (ENS Lyon)-IFR128-Institut National de la Santé et de la Recherche Médicale (INSERM), and École normale supérieure de Lyon (ENS de Lyon)-IFR128-Institut National de la Santé et de la Recherche Médicale (INSERM)

Subjects

Male, viruses, [SDV]Life Sciences [q-bio], MESH: Cricetinae, MESH: Henipavirus Infections, MESH: Dependovirus, Antibodies, Viral, medicine.disease_cause, Recombinant virus, MESH: Antibodies, Neutralizing, Mice, Hepatitis E virus, MESH: Genetic Vectors, Cricetinae, Immunology and Allergy, MESH: Animals, Vector (molecular biology), MESH: Immunity, Humoral, Adeno-associated virus, Henipavirus Infections, MESH: Immunoglobulin G, Vaccines, Synthetic, 0303 health sciences, Dependovirus, 3. Good health, Vaccination, Infectious Diseases, Viruses, Henipavirus, MESH: Cell Line, Tumor, MESH: Vaccines, Synthetic, Genetic Vectors, Biology, Virus, AAV vectors, Major Articles and Brief Reports, 03 medical and health sciences, MESH: Viral Vaccines, Cell Line, Tumor, medicine, Animals, Humans, Hendra Virus, MESH: Mice, 030304 developmental biology, MESH: Humans, 030306 microbiology, Viral Vaccines, biology.organism_classification, Antibodies, Neutralizing, Virology, MESH: Male, Immunity, Humoral, Disease Models, Animal, Immunoglobulin G, Humoral Immunity, Immunology, MESH: Disease Models, Animal, Vaccine, MESH: Antibodies, Viral

Abstract

International audience; Nipah virus (NiV) and Hendra virus (HeV) are closely related, recently emerged paramyxoviruses that are capable of causing considerable morbidity and mortality in several mammalian species, including humans. Henipavirus-specific vaccines are still commercially unavailable, and development of novel antiviral strategies to prevent lethal infections due to henipaviruses is highly desirable. Here we describe the development of adeno-associated virus (AAV) vaccines expressing the NiV G protein. Characterization of these vaccines in mice demonstrated that a single intramuscular AAV injection was sufficient to induce a potent and long-lasting antibody response. Translational studies in hamsters further demonstrated that all vaccinated animals were protected against lethal challenge with NiV. In addition, this vaccine induced a cross-protective immune response that was able to protect 50% of the animals against a challenge by HeV. This study presents a new efficient vaccination strategy against henipaviruses and opens novel perspectives on the use of AAV vectors as vaccines against emergent diseases.

Published

2013

26. Definition of herpes simplex virus type 1 helper activities for adeno-associated virus early replication events

Author

Alberto L. Epstein, Cornel Fraefel, Nathalie Alazard-Dany, Aurélie Ploquin, Anna Salvetti, Armel Nicolas, Anna Greco, Regina Strasser, University of Zurich, Salvetti, A, Centre de Recherches Pétrographiques et Géochimiques (CRPG), Institut national des sciences de l'Univers (INSU - CNRS)-Université de Lorraine (UL)-Centre National de la Recherche Scientifique (CNRS), Centre de génétique et de physiologie moléculaire et cellulaire (CGPhiMC), Centre National de la Recherche Scientifique (CNRS)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon, Vecteurs viraux et transfert des gènes in vivo, and Institut National de la Santé et de la Recherche Médicale (INSERM)

Subjects

ICP8, viruses, MESH: Exodeoxyribonucleases, 2405 Parasitology, Fluorescent Antibody Technique, MESH: DNA Replication, MESH: Dependovirus, DNA-Directed DNA Polymerase, Herpesvirus 1, Human, medicine.disease_cause, Virus Replication, Polymerase Chain Reaction, MESH: Gene Expression Regulation, Viral, MESH: DNA-Directed DNA Polymerase, Chlorocebus aethiops, MESH: Blotting, Southern, MESH: Animals, MESH: In Situ Hybridization, Fluorescence, MESH: Fluorescent Antibody Technique, Adeno-associated virus, lcsh:QH301-705.5, In Situ Hybridization, Fluorescence, 0303 health sciences, 030302 biochemistry & molecular biology, 2404 Microbiology, Dependovirus, 3. Good health, DNA-Binding Proteins, MESH: Herpesvirus 1, Human, Blotting, Southern, Virology/Viral Replication and Gene Regulation, Helper virus, MESH: Helper Viruses, Primase, Helper Viruses, Research Article, Plasmids, 10244 Institute of Virology, DNA Replication, Gene Expression Regulation, Viral, lcsh:Immunologic diseases. Allergy, Ubiquitin-Protein Ligases, Immunology, MESH: Vero Cells, Biology, Microbiology, Immediate-Early Proteins, 03 medical and health sciences, Viral Proteins, Replication factor C, 1311 Genetics, MESH: Plasmids, Virology, Genetics, medicine, 1312 Molecular Biology, Animals, Humans, Molecular Biology, Vero Cells, 030304 developmental biology, 2403 Immunology, MESH: Humans, MESH: Virus Replication, Virology/Persistence and Latency, DNA replication, MESH: Immediate-Early Proteins, MESH: Polymerase Chain Reaction, [SDV.BBM.BM]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Molecular biology, biochemical phenomena, metabolism, and nutrition, MESH: Ubiquitin-Protein Ligases, MESH: Cercopithecus aethiops, MESH: Viral Proteins, MESH: Hela Cells, Herpes simplex virus, Exodeoxyribonucleases, Viral replication, lcsh:Biology (General), 2406 Virology, 570 Life sciences, biology, Parasitology, lcsh:RC581-607, MESH: DNA-Binding Proteins, HeLa Cells

Abstract

The human parvovirus Adeno-Associated Virus (AAV) type 2 can only replicate in cells co-infected with a helper virus, such as Adenovirus or Herpes Simplex Virus type 1 (HSV-1); whereas, in the absence of a helper virus, it establishes a latent infection. Previous studies demonstrated that the ternary HSV-1 helicase/primase (HP) complex (UL5/8/52) and the single-stranded DNA-Binding Protein (ICP8) were sufficient to induce AAV-2 replication in transfected cells. We independently showed that, in the context of a latent AAV-2 infection, the HSV-1 ICP0 protein was able to activate rep gene expression. The present study was conducted to integrate these observations and to further explore the requirement of other HSV-1 proteins during early AAV replication steps, i.e. rep gene expression and AAV DNA replication. Using a cellular model that mimics AAV latency and composite constructs coding for various sets of HSV-1 genes, we first confirmed the role of ICP0 for rep gene expression and demonstrated a synergistic effect of ICP4 and, to a lesser extent, ICP22. Conversely, ICP27 displayed an inhibitory effect. Second, our analyses showed that the effect of ICP0, ICP4, and ICP22 on rep gene expression was essential for the onset of AAV DNA replication in conjunction with the HP complex and ICP8. Third, and most importantly, we demonstrated that the HSV-1 DNA polymerase complex (UL30/UL42) was critical to enhance AAV DNA replication to a significant level in transfected cells and that its catalytic activity was involved in this process. Altogether, this work represents the first comprehensive study recapitulating the series of early events taking place during HSV-1–induced AAV replication., Author Summary The Adeno-Associated Virus (AAV) is a human parvovirus that is widely used as a recombinant vector for gene transfer in animal studies and clinical trials designed to treat acquired or inherited genetic diseases. Wild type AAV is defined as a defective virus because it requires the presence of a helper virus to efficiently replicate. Although many viruses can provide helper functions to AAV, only those of Adenovirus were extensively studied, leading to the generation of molecular tools for recombinant AAV vector production. This study focuses on the helper activities of another virus, the Herpes Simplex Virus type-1 (HSV-1). We demonstrate that nine HSV-1 proteins are able to fully and efficiently support the early steps of AAV replication. As such, this study provides new information critical for the understanding of AAV replication and also opens the way for new biotechnological developments in the field of recombinant AAV vectors.

Published

2009

27. Use of ChAd3-EBO-Z Ebola virus vaccine in Malian and US adults, and boosting of Malian adults with MVA-BN-Filo: a phase 1, single-blind, randomised trial, a phase 1b, open-label and double-blind, dose-escalation trial, and a nested, randomised, double-blind, placebo-controlled trial

Author

Milagritos D, Tapia, Samba O, Sow, Kirsten E, Lyke, Fadima Cheick, Haidara, Fatoumata, Diallo, Moussa, Doumbia, Awa, Traore, Flanon, Coulibaly, Mamoudou, Kodio, Uma, Onwuchekwa, Marcelo B, Sztein, Rezwanul, Wahid, James D, Campbell, Marie-Paule, Kieny, Vasee, Moorthy, Egeruan B, Imoukhuede, Tommy, Rampling, Francois, Roman, Iris, De Ryck, Abbie R, Bellamy, Len, Dally, Olivier Tshiani, Mbaya, Aurélie, Ploquin, Yan, Zhou, Daphne A, Stanley, Robert, Bailer, Richard A, Koup, Mario, Roederer, Julie, Ledgerwood, Adrian V S, Hill, W Ripley, Ballou, Nancy, Sullivan, Barney, Graham, and Myron M, Levine

Subjects

Adult, Male, Adolescent, Dose-Response Relationship, Immunologic, Immunization, Secondary, Hemorrhagic Fever, Ebola, Middle Aged, Mali, United States, Young Adult, Infectious Diseases, Double-Blind Method, Animals, Humans, Female, Single-Blind Method, Ebola Vaccines, Antigens, Viral, Aged, Glycoproteins

Abstract

SummaryBackgroundThe 2014 west African Zaire Ebola virus epidemic prompted worldwide partners to accelerate clinical development of replication-defective chimpanzee adenovirus 3 vector vaccine expressing Zaire Ebola virus glycoprotein (ChAd3-EBO-Z). We aimed to investigate the safety, tolerability, and immunogenicity of ChAd3-EBO-Z in Malian and US adults, and assess the effect of boosting of Malians with modified vaccinia Ankara expressing Zaire Ebola virus glycoprotein and other filovirus antigens (MVA-BN-Filo).MethodsIn the phase 1, single-blind, randomised trial of ChAd3-EBO-Z in the USA, we recruited adults aged 18–65 years from the University of Maryland medical community and the Baltimore community. In the phase 1b, open-label and double-blind, dose-escalation trial of ChAd3-EBO-Z in Mali, we recruited adults 18–50 years of age from six hospitals and health centres in Bamako (Mali), some of whom were also eligible for a nested, randomised, double-blind, placebo-controlled trial of MVA-BN-Filo. For randomised segments of the Malian trial and for the US trial, we randomly allocated participants (1:1; block size of six [Malian] or four [US]; ARB produced computer-generated randomisation lists; clinical staff did randomisation) to different single doses of intramuscular immunisation with ChAd3-EBO-Z: Malians received 1 × 1010 viral particle units (pu), 2·5 × 1010 pu, 5 × 1010 pu, or 1 × 1011 pu; US participants received 1 × 1010 pu or 1 × 1011 pu. We randomly allocated Malians in the nested trial (1:1) to receive a single dose of 2 × 108 plaque-forming units of MVA-BN-Filo or saline placebo. In the double-blind segments of the Malian trial, investigators, clinical staff, participants, and immunology laboratory staff were masked, but the study pharmacist (MK), vaccine administrator, and study statistician (ARB) were unmasked. In the US trial, investigators were not masked, but participants were. Analyses were per protocol. The primary outcome was safety, measured with occurrence of adverse events for 7 days after vaccination. Both trials are registered with ClinicalTrials.gov, numbers NCT02231866 (US) and NCT02267109 (Malian).FindingsBetween Oct 8, 2014, and Feb 16, 2015, we randomly allocated 91 participants in Mali (ten [11%] to 1 × 1010 pu, 35 [38%] to 2·5 × 1010 pu, 35 [38%] to 5 × 1010 pu, and 11 [12%] to 1 × 1011 pu) and 20 in the USA (ten [50%] to 1 × 1010 pu and ten [50%] to 1 × 1011 pu), and boosted 52 Malians with MVA-BN-Filo (27 [52%]) or saline (25 [48%]). We identified no safety concerns with either vaccine: seven (8%) of 91 participants in Mali (five [5%] received 5 × 1010 and two [2%] received 1 × 1011 pu) and four (20%) of 20 in the USA (all received 1 × 1011 pu) given ChAd3-EBO-Z had fever lasting for less than 24 h, and 15 (56%) of 27 Malians boosted with MVA-BN-Filo had injection-site pain or tenderness.Interpretation1 × 1011 pu single-dose ChAd3-EBO-Z could suffice for phase 3 efficacy trials of ring-vaccination containment needing short-term, high-level protection to interrupt transmission. MVA-BN-Filo boosting, although a complex regimen, could confer long-lived protection if needed (eg, for health-care workers).FundingWellcome Trust, Medical Research Council UK, Department for International Development UK, National Cancer Institute, Frederick National Laboratory for Cancer Research, Federal Funds from National Institute of Allergy and Infectious Diseases.