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Dive into the research topics where Robert J. Powell is active.

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Featured researches published by Robert J. Powell.


Journal of Biotechnology | 1996

Optimization of live oral Salmonella-HIV-1 vaccine vectors for the induction of HIV-specific mucosal and systemic immune responses.

David M. Hone; Shaoguang Wu; Robert J. Powell; David W. Pascual; John Van Cott; Jerry R. McGhee; Timothy R. Fouts; Robert G. Tuskan; George K. Lewis

Recent evidence suggests that live oral Salmonella-HIV vaccine vectors have the potential to elicit HIV-specific T cell-mediated immunity in both the mucosal and systemic compartments. We are using the mouse-typhoid model to identify Salmonella::HIV vaccine vector constructs that elicit HIV-specific mucosal and systemic immune responses. Oral immunization of mice with a Salmonella strain that expresses recombinant gp120 (rgp120) in the cytoplasm of the vector elicits a modest gp120-specific T cell proliferation response in the spleen. However, such Salmonella constructs did not stimulate the development of gp120-specific serum IgG or cytotoxic T lymphocytes (CTLs). Interestingly, the majority of cytoplasmically-expressed rgp120 forms inclusion bodies in Salmonella. We believe that in this form rgp120 is highly susceptible to protease degradation by the vector. As such, cytoplasmic rgp120 may not persist in the host after vaccination, resulting in the modest immunogenicity of rgp120 in these constructs. To circumvent this problem we constructed Salmonella strains that express rgp120 on the surface of the vector. Preliminary data suggest that surface-expressed rgp120 is significantly more immunogenic in both the mucosal and systemic compartments than cytoplasmic rgp120. These results, therefore, support the proposal that Salmonella vectors will be a safe and inexpensive means for delivery of HIV antigens to, and the elicitation of HIV-specific T cells in, the mucosal and systemic compartments.


Archive | 2003

Method for introducing and expressing genes in animal cells and live invasive bacterial vectors for use in the same

Robert J. Powell; George K. Lewis; David M. Hone


Infection and Immunity | 1999

Expression of recombinant enterotoxigenic Escherichia coli colonization factor antigen I by Salmonella typhimurium elicits a biphasic T helper cell response

David W. Pascual; David M. Hone; Stacy Hall; Frederik W. van Ginkel; Masafumi Yamamoto; Nancy Walters; Kohataro Fujihashi; Robert J. Powell; Shaoguang Wu; John L. VanCott; Hiroshi Kiyono; Jerry R. McGhee


Archive | 2000

Therapeutic polypeptides and methods for using same

Robert C. Gallo; Joseph Bryant; Yanto Lunardi-Iskandar; Robert J. Powell; Marvin S. Reitz; James S. Foulke; George K. Lewis


Archive | 1996

Method of making non-pyrogenic lipopolysaccharide or A

Robert J. Powell; David M. Hone


Archive | 1996

Novel non-pyrogenic bacterial strains and use of the same

David M. Hone; Robert J. Powell


Archive | 1999

Non-pyrogenic bacterial strains and use of the same

Robert J. Powell; David M. Hone


Archive | 2001

Procede d'introduction et d'expression de genes dans des cellules animales, et vesicules bacteriennes destinees a etre utilisees dans le cadre dudit procede

Robert J. Powell; David M. Hone


Archive | 2000

Polypeptides therapeutiques et leurs methodes d'utilisation

Robert C. Gallo; Joseph Bryant; Yanto Lunardi-Iskandar; Robert J. Powell; Marvin S. Reitz; James S. Foulke; George K. Lewis


The FASEB Journal | 1996

Mode of vaccine expression by salmonella dictates th cell response: Th2 cell precedes TH1 cell antienterotoxigenic e. coli (ETEC) fimbriae responses

David W. Pascual; David M. Hone; Stacy Hall; F. W. Van Ginkel; M. Yamamolo; Keiko Fujihashi; Robert J. Powell; Shaoguang Wu; John L. VanCott; Hiroshi Kiyono; Jerry R. McGhee

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David M. Hone

University of Maryland Biotechnology Institute

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David W. Pascual

University of Mississippi Medical Center

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John L. VanCott

University of Alabama at Birmingham

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