M Chen-Woan scite author profile

M Chen-Woan

4Publications

67Citation Statements Received

41Citation Statements Given

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104

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Affiliations

University of Pittsburgh, New York State College of Veterinary Medicine, Cornell University

Publications

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A new protocol for the propagation of dendritic cells from rat bone marrow using recombinant GM-CSF, and their quantification using the mAb OX-62

Chen-Woan

Delaney

Fournier

et al. 1995

Journal of Immunological Methods

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Bone marrow (BM)-derived dendritic cells (DC) are the most potent known antigen (Ag) presenting cell in vivo and in vitro. Detailed analysis of their properties and mechanisms of action requires an ability to produce large numbers of DC. Although DC have been isolated from several rat tissues, including BM, the yield is uniformly low. We describe a simple method for the propagation of large numbers of DC from rat BM and document cell yield with the rat DC marker, OX-62.After depletion of plastic-adherent and Fc + cells by panning on dishes coated with normal serum, residual BM cells were cultured in gelatin coated flasks using murine rGM-CSF supplemented medium. Prior to analysis, non-adherent cells were re-depleted of contaminating Fc + cells. Propagation of DC was monitored by double staining for FACS analysis (major histocompatibility complex (MHC) class II + /OX-62 + , OX-19 − ). Functional assay, morphological analysis and evaluation of homing patterns of cultured cells revealed typical DC characteristics. MHC class II and OX-62 antigen expression increased with time in culture and correlated with allostimulatory ability. DC yield increased until day 7, when 3.3 × 10 6 DC were obtained from an initial 3 × 10 8 unfractionated BM cells. Significant numbers of DC can be generated from rat BM using these simple methods. This should permit analysis and manipulation of rat DC functions in vivo and in vitro.

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In vitro characterization of rat bone marrow-derived dendritic cells and their precursors

Chen-Woan

Delaney

Fournier

et al. 1996

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Although the rat is commonly used for basic immunology and transplantation research, phenotypic and functional characterization of rat dendritic cells (DCs) lags behind similar studies in the human and mouse. Therefore, these features were examined using DCs propagated from cultures of rat bone marrow maintained in a medium supplemented with granulocyte-monocyte colony-stimulating factor. Analysis of cytospin preparations of cultured cells showd that DCs arise from OX7+ myelomonocytic precursors. Typical mature rat DCs were morphologically similar to their mouse and human counterparts and expressed major histocompatibility complex (MHC) class II (common part determinant of Ia), OX62 (integrin molecule), OX7 (CD90), ICAM-1 (CD54), and CTLA4 counterreceptor, but were negative for OX8 (CD8), OX19 (CD5), W3/25 (CD4), and ED2, a rat macrophage marker. Functional analysis of OX62+ sorted DCs showed that they could effectively present the soluble antigen ovalbumin to naive T cells in vitro. A combination of anti-MHC class II monoclonal antibody and CTLA4-immunoglobulin inhibited allostimulatory ability more effectively than either reagent alone. Implications for studying the role of DCs in immune responses in the rat are discussed.

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Evidence That Cyclosporine Treatment Causes the Appearance in Rat Lymph Node of T Cells Having the Antigenic Phenotypes of Cortical Thymocytesnode

Chen-Woan

Goldschneider

1991

TRANSPLANTATION

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The mediators of acquired resistance to Listeria monocytogenes are contained within a population of cytotoxic T cells

Chen-Woan

McGregor

1984

Cellular Immunology

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M Chen-Woan

A new protocol for the propagation of dendritic cells from rat bone marrow using recombinant GM-CSF, and their quantification using the mAb OX-62

In vitro characterization of rat bone marrow-derived dendritic cells and their precursors

Evidence That Cyclosporine Treatment Causes the Appearance in Rat Lymph Node of T Cells Having the Antigenic Phenotypes of Cortical Thymocytesnode

The mediators of acquired resistance to Listeria monocytogenes are contained within a population of cytotoxic T cells

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