David I Bernstein1, Marcela F Pasetti2, Rebecca Brady3, Amanda D Buskirk2, Rezwanul Wahid2, Michelle Dickey3, Mitchell Cohen3, Holly Baughman4, Jill El-Khorazaty4, Nicole Maier5, Marcelo B Sztein2, Shahida Baqar6, A Louis Bourgeois5. 1. Cincinnati Children's Hospital Medical Center, Cincinnati, OH, United States. Electronic address: david.bernstein@cchmc.org. 2. Center for Vaccine Development and Global Health, University of Maryland School of Medicine, Baltimore, MD, United States. 3. Cincinnati Children's Hospital Medical Center, Cincinnati, OH, United States. 4. The Emmes Corporation, Rockville, MD, United States. 5. PATH, Washington, DC, United States. 6. Division of Microbiology and Infectious Diseases, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Bethesda, MD, United States.
Abstract
BACKGROUND: The public health burden of Enterotoxigenic Escherichia coli (ETEC) is high but no vaccine is specifically approved to prevent ETEC infections. METHODS: We performed a Phase 1, dose escalation study (1-50 µg) evaluating the sublingual (SL) delivery of the double mutant heat-labile toxin LTR192G/L211A (dmLT) in 80 healthy adult volunteers. The primary objective was safety and the secondary was the immunogenicity of the dmLT. Subjects received 3 doses of dmLT at days 1, 15, and 29. Subjects receiving the first dose at each dosage level were observed overnight in a research facility. The second and third doses were administered on an outpatient basis. Data from cohorts 1-4 were used to select the cohort 5 dose (25 µg), comparing SL and oral routes. RESULTS: The vaccine appeared safe and well tolerated with only rare development of vomiting or diarrhea. The serum anti-dmLT IgA and IgG and neutralizing antibody responses were modest after any of the SL immunizations. Serum IgA and IgG titers were increased at the higher antigen doses (25 or 50 µg) but the percent with 4-fold increases was at best 38% for both IgA and IgG. The 4-fold increase among subjects receiving all 3 doses was 43% for both IgA and IgG. Antibody titers following oral administration were, in general, significantly higher than after SL. The frequency of IgA- or IgG-ASCs in circulation were somewhat vaccine dose dependent and were detected at a moderate level. However, antibodies in saliva or stool were rarely detected. Post-vaccination increases in T cells or cytokine production were also infrequent. CONCLUSION: The dmLT vaccine formulation evaluated here was safe but only moderately immunogenic at doses up to 50 µg when administered by the SL or oral route. Studies at higher doses with better formulations appear warranted.
BACKGROUND: The public health burden of Enterotoxigenic Escherichia coli (ETEC) is high but no vaccine is specifically approved to prevent ETEC infections. METHODS: We performed a Phase 1, dose escalation study (1-50 µg) evaluating the sublingual (SL) delivery of the double mutant heat-labile toxin LTR192G/L211A (dmLT) in 80 healthy adult volunteers. The primary objective was safety and the secondary was the immunogenicity of the dmLT. Subjects received 3 doses of dmLT at days 1, 15, and 29. Subjects receiving the first dose at each dosage level were observed overnight in a research facility. The second and third doses were administered on an outpatient basis. Data from cohorts 1-4 were used to select the cohort 5 dose (25 µg), comparing SL and oral routes. RESULTS: The vaccine appeared safe and well tolerated with only rare development of vomiting or diarrhea. The serum anti-dmLT IgA and IgG and neutralizing antibody responses were modest after any of the SL immunizations. Serum IgA and IgG titers were increased at the higher antigen doses (25 or 50 µg) but the percent with 4-fold increases was at best 38% for both IgA and IgG. The 4-fold increase among subjects receiving all 3 doses was 43% for both IgA and IgG. Antibody titers following oral administration were, in general, significantly higher than after SL. The frequency of IgA- or IgG-ASCs in circulation were somewhat vaccine dose dependent and were detected at a moderate level. However, antibodies in saliva or stool were rarely detected. Post-vaccination increases in T cells or cytokine production were also infrequent. CONCLUSION: The dmLT vaccine formulation evaluated here was safe but only moderately immunogenic at doses up to 50 µg when administered by the SL or oral route. Studies at higher doses with better formulations appear warranted.
Authors: H Peltola; A Siitonen; H Kyrönseppä; I Simula; L Mattila; P Oksanen; M J Kataja; M Cadoz Journal: Lancet Date: 1991-11-23 Impact factor: 79.321
Authors: Rezwanul Wahid; Marcela F Pasetti; Milton Maciel; Jakub K Simon; Carol O Tacket; Myron M Levine; Marcelo B Sztein Journal: Clin Immunol Date: 2010-12-10 Impact factor: 3.969
Authors: Gregory M Glenn; Christina P Villar; David C Flyer; A Louis Bourgeois; Robin McKenzie; Robert M Lavker; Sarah A Frech Journal: Infect Immun Date: 2007-01-29 Impact factor: 3.441
Authors: Anna Lundgren; Louis Bourgeois; Nils Carlin; John Clements; Björn Gustafsson; Marianne Hartford; Jan Holmgren; Max Petzold; Richard Walker; Ann-Mari Svennerholm Journal: Vaccine Date: 2014-11-05 Impact factor: 3.641
Authors: Zhiming Huo; Sara L Bissett; Raphaela Giemza; Simon Beddows; Clarissa Oeser; David J M Lewis Journal: PLoS One Date: 2012-03-16 Impact factor: 3.240
Authors: Milton Maciel; David Bauer; Robin L Baudier; Jacob Bitoun; John D Clements; Steven T Poole; Mark A Smith; Robert W Kaminski; Stephen J Savarino; Elizabeth B Norton Journal: Infect Immun Date: 2019-10-18 Impact factor: 3.441
Authors: Anusmita Sahoo; Andrew T Jones; Narayanaiah Cheedarla; Sailaja Gangadhara; Vicky Roy; Tiffany M Styles; Ayalnesh Shiferaw; Korey L Walter; LaTonya D Williams; Xiaoying Shen; Gabriel Ozorowski; Wen-Hsin Lee; Samantha Burton; Lasanajak Yi; Xuezheng Song; Zhaohui S Qin; Cynthia A Derdeyn; Andrew B Ward; John D Clements; Raghavan Varadarajan; Georgia D Tomaras; Pamela A Kozlowski; Galit Alter; Rama Rao Amara Journal: Sci Immunol Date: 2022-07-22
Authors: David Poncet; Catherine Hessler; Hong Liang; Sylviane Gautheron; Michelle Sergent; Nicholas D Rintala; Emilie Seydoux; Po-Wei D Huang; David Argilla; Sophie Ruiz; Jon Heinrichs; Milton Maciel; Mark T Orr Journal: NPJ Vaccines Date: 2020-09-11 Impact factor: 7.344
Authors: Addison E Stone; Sarah E Scheuermann; Colin N Haile; Gregory D Cuny; Marcela Lopez Velasquez; Joshua P Linhuber; Anantha L Duddupudi; Jennifer R Vigliaturo; Marco Pravetoni; Therese A Kosten; Thomas R Kosten; Elizabeth B Norton Journal: NPJ Vaccines Date: 2021-05-13 Impact factor: 7.344
Authors: Tida Lee; Ramiro L Gutiérrez; Milton Maciel; Steven Poole; Kayla J Testa; Stefanie Trop; Christopher Duplessis; Alison Lane; Mark S Riddle; Melinda Hamer; Ashley Alcala; Michael Prouty; Nicole Maier; Rahsan Erdem; A Louis Bourgeois; Chad K Porter Journal: Vaccine Date: 2021-08-18 Impact factor: 3.641
Authors: Jessica W Crothers; Elizabeth Ross Colgate; Kelly J Cowan; Dorothy M Dickson; MaryClaire Walsh; Marya Carmolli; Peter F Wright; Elizabeth B Norton; Beth D Kirkpatrick Journal: Vaccine Date: 2022-03-30 Impact factor: 4.169
Authors: Lorena M Coria; Franco L Martinez; Laura A Bruno; Karina A Pasquevich; Juliana Cassataro Journal: Vaccine Date: 2020-06-11 Impact factor: 3.641