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Dive into the research topics where Shi-Xian Cao is active.

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Featured researches published by Shi-Xian Cao.


Journal of Immunotherapy | 2010

Preclinical qualification of a new multi-antigen candidate vaccine for metastatic melanoma.

Thorsten U. Vogel; Lucian Visan; Belma Ljutic; Beata Gajewska; Judy Caterini; Danielle Salha; Tao Wen; Liwei He; Mark Parrington; Shi-Xian Cao; Bryan McNeil; Devender Sandhu; Nancy Scollard; Linong Zhang; Bill Bradley; Mei Tang; Corey Lovitt; Ray Oomen; Pamela Dunn; Jim Tartaglia; Neil Berinstein

New therapies are urgently required for the treatment of patients with melanoma. Here we describe the generation and preclinical evaluation of 3 new recombinant ALVAC(2) poxviruses vCP2264, vCP2291, and vCP2292 for their ability to induce the desired cellular immune responses against the encoded melanoma-associated antigens. This was done either in HLA-A2/Kb transgenic mice or using in vitro antigen-presentation studies. These studies demonstrated that the vaccine was able to induce HLA-A*0201-restricted T-cell responses against gp100 and NY-ESO-1, detectable directly ex vivo, in HLA-A2/Kb-transgenic mice. The in vitro antigen presentation studies, in the absence of appropriate animal models, demonstrated that target cells infected with the vaccine construct were lysed by MAGE-1, MAGE-3 or MART-1 peptide-specific T cells. These data indicate that ALVAC(2)-encoded melanoma-associated antigens can be properly processed and presented to induce antigen-specific cytotoxic T-cell responses. To enhance the immunogenicity of the melanoma antigens, a TRIad of COstimulatory Molecules (TRICOM) were also cloned into all 3 vectors. Increased in vitro proliferation and IFN-γ production was observed with all ALVAC(2) poxviruses encoding TRICOM, confirming the immune-enhancing effect of the ALVAC-encoded TRICOM. These studies demonstrated that all components of the vaccine were functionally active and provide a rationale for moving this candidate vaccine to the clinic.


Journal of Virology | 1998

Particle size determinants in the human immunodeficiency virus type 1 Gag protein.

Laurence Garnier; Lee Ratner; Benjamin Rovinski; Shi-Xian Cao; John W. Wills


Journal of Virology | 1999

Identification of Retroviral Late Domains as Determinants of Particle Size

Laurence Garnier; Leslie J. Parent; Benjamin Rovinski; Shi-Xian Cao; John W. Wills


Archive | 1999

Vectors for DNA immunization against cervical cancer

Diane M Gajewczyk; Roy Persson; Fei-Long Yao; Shi-Xian Cao; Michel H. Klein; James Tartaglia; Phillipe Moingeon; Benjamin Rovinski


Archive | 1995

Antigenically-marked non-infectious retrovirus-like particles

Benjamin Rovinski; Shi-Xian Cao; Fei-Long Yao; Roy Persson; Michel H. Klein


Archive | 1995

Human immunodeficiency virus type 1 nucleic acids devoid of long terminal repeats capable of encoding for non-infectious, immunogenic, retrovirus-like particles

Benjamin Rovinski; Shi-Xian Cao; Fei-Long Yao; Roy Persson; Michel H. Klein


Archive | 1995

Nucleic acids encoding for non-infectious, replication-defective, self-assembling HIV-1 viral particles containing antigenic markers in the gag coding region

Benjamin Rovinski; Shi-Xian Cao; Fei-Long Yao; Roy Persson; Michel H. Klein


Archive | 1994

Non-infectious, replication-defective, self-assembling HIV-1 viral particles containing antigenic markers in the gag coding region

Benjamin Rovinski; Shi-Xian Cao; Fei-Long Yao; Roy Persson; Michel H. Klein


Archive | 1995

Methods for the detection of HIV-specific immune responses employing non-infectious, non-replicating, IIV retrovirus-like particles containing heterologous antigenic markers

Benjamin Rovinski; Shi-Xian Cao; Fei-Long Yao; Roy Persson; Michel H. Klein


Archive | 2002

Retrovirus-like particles made non-infectious by a plurality of mutations

Benjamin Rovinski; Shi-Xian Cao; Fei-Long Yao; Roy Persson; Michel H. Klein

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