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Dive into the research topics where Carolyn Weeks-Levy is active.

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Featured researches published by Carolyn Weeks-Levy.


Vaccine | 2010

Development of a recombinant tetravalent dengue virus vaccine: immunogenicity and efficacy studies in mice and monkeys.

David E. Clements; Beth-Ann Coller; Michael M. Lieberman; Steven A. Ogata; Gordon Wang; Kent E. Harada; J. Robert Putnak; John M. Ivy; Michael McDonell; Gary Bignami; Iain Peters; Julia Leung; Carolyn Weeks-Levy; Eileen Nakano; Tom Humphreys

Truncated recombinant dengue virus envelope protein subunits (80E) are efficiently expressed using the Drosophila Schneider-2 (S2) cell expression system. Binding of conformationally sensitive antibodies as well as X-ray crystal structural studies indicate that the recombinant 80E subunits are properly folded native-like proteins. Combining the 80E subunits from each of the four dengue serotypes with ISCOMATRIX adjuvant, an adjuvant selected from a set of adjuvants tested for maximal and long lasting immune responses, results in high titer virus neutralizing antibody responses. Immunization of mice with a mixture of all four 80E subunits and ISCOMATRIX adjuvant resulted in potent virus neutralizing antibody responses to each of the four serotypes. The responses to the components of the tetravalent mixture were equivalent to the responses to each of the subunits administered individually. In an effort to evaluate the potential protective efficacy of the Drosophila expressed 80E, the dengue serotype 2 (DEN2-80E) subunit was tested in both the mouse and monkey challenge models. In both models protection against viral challenge was achieved with low doses of antigen in the vaccine formulation. In non-human primates, low doses of the tetravalent formulation induced good virus neutralizing antibody titers to all four serotypes and protection against challenge with the two dengue virus serotypes tested. In contrast to previous reports, where subunit vaccine candidates have generally failed to induce potent, protective responses, native-like soluble 80E proteins expressed in the Drosophila S2 cells and administered with appropriate adjuvants are highly immunogenic and capable of eliciting protective responses in both mice and monkeys. These results support the development of a dengue virus tetravalent vaccine based on the four 80E subunits produced in the Drosophila S2 cell expression system.


Clinical and Vaccine Immunology | 2009

Immunogenicity and Protective Efficacy of a Recombinant Subunit West Nile Virus Vaccine in Rhesus Monkeys

Michael M. Lieberman; Vivek R. Nerurkar; Haiyan Luo; Bruce Cropp; Ricardo Carrion; Melissa de la Garza; Beth Ann Coller; D. L. Clements; Steven A. Ogata; Teri Wong; Tim Martyak; Carolyn Weeks-Levy

ABSTRACT The immunogenicity and protective efficacy of a recombinant subunit West Nile virus (WNV) vaccine was evaluated in rhesus macaques (Macaca mulatta). The vaccine consisted of a recombinant envelope (E) protein truncated at the C-terminal end, resulting in a polypeptide containing 80% of the N-terminal amino acids of the native WNV protein (WN-80E), mixed with an adjuvant (GPI-0100). WN-80E was produced in a Drosophila melanogaster expression system with high yield and purified by immunoaffinity chromatography using a monoclonal antibody specific for flavivirus E proteins. Groups of monkeys were vaccinated with formulations containing 1 or 25 μg of WN-80E antigen, and both humoral and cellular immunity were assessed after vaccination. The results demonstrated potent antibody responses to vaccination, as determined by both enzyme-linked immunosorbent assay and virus-neutralizing antibody assays. All vaccinated animals responded favorably, and there was little difference in response between animals immunized with 1 or 25 μg of WN-80E. Cellular immunity was determined by lymphocyte proliferation and cytokine production assays using peripheral blood mononuclear cells from vaccinated animals stimulated in vitro with WN-80E. Cell-mediated immune responses varied from animal to animal within each group. About half of the animals responded with lymphoproliferation, cytokine production, or both. Again, there was little difference in response between animals immunized with a 1- or 25-μg dose of WN-80E in the vaccine formulations. In a separate experiment, groups of monkeys were immunized with the WN-80E/GPI-0100 vaccine or an adjuvant-only control formulation. Animals were then challenged by inoculation of wild-type WNV, and the level of viremia in each animal was monitored daily for 10 days. The results showed that whereas all animals in the control group had detectable viremia for at least 3 days after challenge, all of the vaccinated animals were negative on all days after challenge. Thus, the WN-80E vaccine was 100% efficacious in protecting monkeys against infection with WNV.


Vaccine | 2007

Preparation and immunogenic properties of a recombinant West Nile subunit vaccine

Michael M. Lieberman; David E. Clements; Steven A. Ogata; Gordon Wang; Gloria Corpuz; Teri Wong; Tim Martyak; Lynne Gilson; Beth Ann Coller; Julia Leung; Douglas M. Watts; Robert B. Tesh; Marina Siirin; Amelia Travassos da Rosa; Tom Humphreys; Carolyn Weeks-Levy


Archive | 2006

Influenza recombinant subunit vaccine

Carolyn Weeks-Levy; David E. Clements; Steven A. Ogata


Vaccine | 2007

Efficacy and Durability of a Recombinant Subunit West Nile Vaccine Candidate in Protecting Hamsters from West Nile Encephalitis

Douglas M. Watts; Robert B. Tesh; Marina Siirin; Amelia Travassos da Rosa; Patrick C. Newman; David E. Clements; Steven A. Ogata; Beth Ann Coller; Carolyn Weeks-Levy; Michael M. Lieberman


Vaccine | 2008

Protective efficacy of a recombinant subunit West Nile virus vaccine in domestic geese (Anser anser)

Susan I. Jarvi; Michael M. Lieberman; Erik K. Hofmeister; Vivek R. Nerurkar; Teri Wong; Carolyn Weeks-Levy


American Journal of Tropical Medicine and Hygiene | 2008

Evaluation of the Efficacy of a Recombinant Subunit West Nile Vaccine in Syrian Golden Hamsters

Marina Siirin; Amelia Travassos da Rosa; Patrick C. Newman; Carolyn Weeks-Levy; Beth Ann Coller; Shu Yuan Xiao; Michael M. Lieberman; Douglas M. Watts


Archive | 2010

Recombinant subunit west nile virus vaccine for protections of human subjects

Beth-Ann Coller; Vidya Pai; Carolyn Weeks-Levy; Steven A. Ogata


Archive | 2008

Synthetic expression vectors for insect cells

David E. Clements; Gordon V. L. Wang; Carolyn Weeks-Levy


Archive | 2016

West nile virus vaccine comprising WN-80E recombinant subunit protein

Beth-Ann Coller; Vidya Pai; Carolyn Weeks-Levy; Steven A. Ogata

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Michael M. Lieberman

Fitzsimons Army Medical Center

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Amelia Travassos da Rosa

University of Texas Medical Branch

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Douglas M. Watts

University of Texas at El Paso

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Marina Siirin

University of Texas Medical Branch

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Patrick C. Newman

University of Texas Medical Branch

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