Your search keyword '"Toth, Kelsey A."' showing total 3 results

1. Central memory CD8+ T lymphocytes mediate lung allograft acceptance.

Author

Krupnick, Alexander Sasha, Lin, Xue, Li, Wenjun, Higashikubo, Ryuiji, Zinselmeyer, Bernd H, Hartzler, Hollyce, Toth, Kelsey, Ritter, Jon H, Berezin, Mikhail Y, Wang, Steven T, Miller, Mark J, Gelman, Andrew E, and Kreisel, Daniel

Subjects

*ANIMAL experimentation, *ANTIGEN presenting cells, *CELL culture, *CELL receptors, *HOMOGRAFTS, *IMMUNITY, *INTERFERONS, *LUNGS, *LUNG surgery, *LUNG transplantation, *RESEARCH methodology, *MICE, *NITRIC oxide, *T cells, *TISSUE culture

Abstract

Memory T lymphocytes are commonly viewed as a major barrier for long-term survival of organ allografts and are thought to accelerate rejection responses due to their rapid infiltration into allografts, low threshold for activation, and ability to produce inflammatory mediators. Because memory T cells are usually associated with rejection, preclinical protocols have been developed to target this population in transplant recipients. Here, using a murine model, we found that costimulatory blockade-mediated lung allograft acceptance depended on the rapid infiltration of the graft by central memory CD8+ T cells (CD44(hi)CD62L(hi)CCR7+). Chemokine receptor signaling and alloantigen recognition were required for trafficking of these memory T cells to lung allografts. Intravital 2-photon imaging revealed that CCR7 expression on CD8+ T cells was critical for formation of stable synapses with antigen-presenting cells, resulting in IFN-γ production, which induced NO and downregulated alloimmune responses. Thus, we describe a critical role for CD8+ central memory T cells in lung allograft acceptance and highlight the need for tailored approaches for tolerance induction in the lung. [ABSTRACT FROM AUTHOR]

Published

2014

2. Central memory CD8+ T lymphocytes mediate lung allograft acceptance.

Author

Krupnick, Alexander Sasha, Xue Lin, Wenjun Li, Ryuiji Higashikubo, Zinselmeyer, Bernd H., Hartzler, Hollyce, Toth, Kelsey, Ritter, Jon H., Berezin, Mikhail Y., Wang, Steven T., Miller, Mark J., Gelman, Andrew E., and Kreisel, Daniel

Subjects

*T cells, *HOMOGRAFTS, *INFLAMMATORY mediators, *SYNAPSES, *ANTIGEN presenting cells

Abstract

Memory T lymphocytes are commonly viewed as a major barrier for long-term survival of organ allografts and are thought to accelerate rejection responses due to their rapid infiltration into allografts, low threshold for activation, and ability to produce inflammatory mediators. Because memory T cells are usually associated with rejection, preclinical protocols have been developed to target this population in transplant recipients. Here, using a murine model, we found that costimulatory blockade--p> CCR7+). Chemokine receptor signaling and alloantigen recognition were required for trafficking of these memory T cells to lung allografts. Intravital 2-photon imaging revealed that CCR7 expression on CD8+ T cells was critical for formation of stable synapses with antigen-presenting cells, resulting in IFN-γ production, which induced NO and downregulated alloimmune responses. Thus, we describe a critical role for CD8+ central memory T cells in lung allograft acceptance and highlight the need for tailored approaches for tolerance induction in the lung. [ABSTRACT FROM AUTHOR]

Published

2014

3. Emergency granulopoiesis promotes neutrophil-dendritic cell encounters that prevent mouse lung allograft acceptance.

Author

Kreisel, Daniel, Sugimoto, Seiichiro, Zhu, Jihong, Nava, Ruben, Li, Wenjun, Okazaki, Mikio, Yamamoto, Sumiharu, Ibrahim, Mohsen, Huang, Howard J., Toth, Kelsey A., Ritte, Jon H. R, Krupnick, Alexander S., Miller, Mark J., and Gelman, Andrew E.

Subjects

*NEUTROPHILS, *DENDRITIC cells, *HOMOGRAFTS, *PHOTONS, *REPERFUSION

Abstract

The mechanisms by which innate immune signals regulate alloimmune responses remain poorly understood. In the present study, we show by intravital 2-photon microscopy direct interactions between graft-infiltrating neutrophils and donor CD11c+ dendritic cells (DCs) within orthotopic lung allografts immediately after reperfusion. Neutrophils isolated from the airways of lung transplantation recipients stimulate donor DCs in a contactdependent fashion to augment their production of IL-12 and expand alloantigenspecific IFN-γ+ T cells. DC IL-12 expression is largely regulated by degranulation and induced by TNF-α associated with the neutrophil plasma membrane. Extended cold ischemic graft storage enhances G-CSF-mediated granulopoiesls and neutrophil graft infiltration, resulting in exacerbation of ischemia-reperfusion iniurv after lung transplantation. lschemia reperfusion injury prevents immunosuppression-mediated acceptance of mouse lung allografts unless G-CSF-ediated granulopoiesis is inhibited. Our findings identify granulopoiesis-mediated augmentation of alloimmunity as a novel link between innate and adaptive immune responses after organ transplantation. [ABSTRACT FROM AUTHOR]

Published

2011