Your search keyword '"Slifka, Mark K"' showing total 4 results

1. Contralateral second dose improves antibody responses to a 2-dose mRNA vaccination regimen

Author

Fazli, Sedigheh, Thomas, Archana, Estrada, Abram E., Ross, Hiro A.P., Lee, David Xthona, Kazmierczak, Steven, Slifka, Mark K., Montefiori, David, Messer, William B., and Curlin, Marcel E.

Subjects

Promega Corp., Vaccination -- Health aspects, Biotechnology industry -- Health aspects, Messenger RNA -- Health aspects, B cells -- Health aspects, Immunoglobulin G -- Health aspects, Health care industry

Abstract

BACKGROUND. Vaccination is typically administered without regard to site of prior vaccination, but this factor may substantially affect downstream immune responses. METHODS. We assessed serological responses to initial COVID-19 vaccination in baseline seronegative adults who received second-dose boosters in the ipsilateral or contralateral arm relative to initial vaccination. We measured serum SARSCoV-2 spike-specific Ig, receptor-binding domain-specific (RBD-specific) IgG, SARS-CoV-2 nucleocapsid-specific IgG, and neutralizing antibody titers against SARS-CoV-2.D614G (early strain) and SARS-CoV-2.B.1.1.529 (Omicron) at approximately 0.6, 8, and 14 months after boosting. RESULTS. In 947 individuals, contralateral boosting was associated with higher spike-specific serum Ig, and this effect increased over time, from a 1.1-fold to a 1.4-fold increase by 14 months (P < 0.001). A similar pattern was seen for RBD-specific IgG. Among 54 pairs matched for age, sex, and relevant time intervals, arm groups had similar antibody levels at study visit 2 (W2), but contralateral boosting resulted in significantly higher binding and neutralizing antibody titers at W3 and W4, with progressive increase over time, ranging from 1.3-fold (total Ig, P = 0.007) to 4.0-fold (pseudovirus neutralization to B.1.1.529, P < 0.001). CONCLUSIONS. In previously unexposed adults receiving an initial vaccine series with the BNT162b2 mRNA COVID-19 vaccine, contralateral boosting substantially increases antibody magnitude and breadth at times beyond 3 weeks after vaccination. This effect should be considered during arm selection in the context of multidose vaccine regimens. FUNDING. M.J. Murdock Charitable Trust, OHSU Foundation, NIH., Introduction In the 227 years since Edward Jenner demonstrated that inoculation with material from cowpox lesions could provide protection from symptomatic illness due to smallpox, vaccine research has advanced to [...]

Published

2024

2. Contralateral second dose improves antibody responses to a two-dose mRNA vaccination regimen

Author

Fazli, Sedigheh, primary, Thomas, Archana, additional, Estrada, Abram E., additional, Ross, Hiro A.P., additional, Xthona Lee, David, additional, Kazmierczak, Steven, additional, Slifka, Mark K., additional, Montefiori, David, additional, Messer, William B., additional, and Curlin, Marcel E., additional

Published

2024

3. Infant diarrheal disease in rhesus macaques impedes microbiome maturation and is linked to uncultured Campylobacter species

Author

Rhoades, Nicholas S., primary, Cinco, Isaac R., additional, Hendrickson, Sara M., additional, Prongay, Kamm, additional, Haertel, Andrew J., additional, Flores, Gilberto E., additional, Slifka, Mark K., additional, and Messaoudi, Ilhem, additional

Published

2024

4. Development of a hydrogen peroxide-inactivated vaccine that protects against viscerotropic yellow fever in a non-human primate model

Author

Amanna, Ian J., Thomas, Archana, Engelmann, Flora, Hammarlund, Erika, Raué, Hans-Peter, Bailey, Adam L., Poore, Elizabeth A., Quintel, Benjamin K., Lewis, Anne D., Axthelm, Michael K., Johnson, Amanda L., Colgin, Lois M.A., Diamond, Michael S., Messaoudi, Ilhem, and Slifka, Mark K.

Abstract

Yellow fever virus (YFV) is endemic in >40 countries and causes viscerotropic disease with up to 20%–60% mortality. Successful live-attenuated yellow fever (YF) vaccines were developed in the mid-1930s, but their use is restricted or formally contraindicated in vulnerable populations including infants, the elderly, and people with compromised immune systems. In these studies, we describe the development of a next-generation hydrogen peroxide-inactivated YF vaccine and determine immune correlates of protection based on log neutralizing index (LNI) and neutralizing titer-50% (NT50) studies. In addition, we compare neutralizing antibody responses and protective efficacy of hydrogen peroxide-inactivated YF vaccine candidates to live-attenuated YFV-17D (YF-VAX) in a rhesus macaque model of viscerotropic YF. Our results indicate that an optimized, inactivated YF vaccine elicits protective antibody responses that prevent viral dissemination and lethal infection in rhesus macaques and may be a suitable alternative for vaccinating vulnerable populations who are not eligible to receive replicating live-attenuated YF vaccines.

Published

2024