Title of article
Characterization of the Cytolytic Trigger Molecules G7/PNK-E as a Molecular Complex on the Surface of Porcine Phagocytes
Author/Authors
Aller، نويسنده , , Steve C. and Cho، نويسنده , , Daeho and Kim، نويسنده , , Yoon B. and Park، نويسنده ,
Issue Information
روزنامه با شماره پیاپی سال 1995
Pages
9
From page
270
To page
278
Abstract
G7 and PNK-E mAbs recognize distinct porcine NK cell and granulocyte function-associated molecules that enhance and induce a significant cytolytic response against tumor cell targets through a mechanism of redirected cytotoxicity. The present study shows that the G7 and PNK-E molecules are present on the surface of porcine neutrophils, monocytes, and pulmonary alveolar maerophages as a physically and functionally associated cytolytic trigger molecular complex. Two-color flow cytometric analysis demonstrates that most, if not all, neutrophils are G7 and PNK-E antigen positive. In contrast, monocytes and PAM contain both G7 and PNK-E positive as well as G7 positive and PNK-E negative subpopulations. mAb binding competition experiments indicate that pretreatment of phagocytes with G7 mAb can block subsequent binding by PNK-E mAb, suggesting that these antigens are physically associated on the surface of porcine phagocytes. Fluorescent co-capping experiments utilizing G7 and PNK-E mAbs clearly demonstrate a physical association between G7 and PNK-E antigens present on the surface of porcine neutrophils. Pretreatment of phagocytes with F(ab′)2 fragments of G7 and PNK-E mAbs shows that F(ab′)2 G7 mAb blocks subsequent induction of phagocyte-mediated tumor cell cytotoxicity by whole PNK-E mAb but pretreatment with F(ab′)2 PNK-E does not block subsequent induction of phagocyte-mediated tumor cell cytotoxicity by whole G7 mAb. In addition, pretreatment of neutrophils and mononuclear phagocytes with F(ab′)2 fragments of G7 mAb blocks subsequent whole PNK-E mAb-dependent activation of a phagocytic cell intracellular oxidative burst response but pretreatment with F(ab′)2 PNK-E does not block subsequent G7 mAb-dependent activation of a phagocytic cell intracellular oxidative burst response. These data reinforce a physical and functional association between the G7 and PNK-E molecules. Recent identification of the G7 antigen as the porcine homolog of FcγRIII indicates that the G7 and PNK-E mAbs recognize a unique and previously uncharacterized FcγR cytolytic trigger molecular complex present on the surface of porcine neutrophils, monocytes, and PAM.
Journal title
Cellular Immunology
Serial Year
1995
Journal title
Cellular Immunology
Record number
1850949
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